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1
Zampagni, Maria Luisa <1966>. "Studio cinematico dell'articolazione del gomito e valutazione del carrying angle durante l'esercizio fisico." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/136/1/MariaLuisaZampagniDottoratoXIXCicloScienzeMotorie.pdf.
Full textAbstract:
Questo progetto di ricerca, è stato sviluppato per studiare le caratteristiche anatomofunzionali che definiscono l’articolazione del gomito, ed in modo articolare la presenza dell’angolazione valga che origina dalla diversa orientazione degli assi meccanici dell’avambraccio e del braccio e, denominata in letteratura come carrying angle.
L’obiettivo principale di questo lavoro - meglio espresso nei diversi capitoli - è stato, quello di identificare un nuovo approccio di misura per la stima di questo angolo,
utilizzabile sia per gli studi di biomeccanica articolare, che per gli studi di analisi del movimento per l’arto superiore.
Il primo obiettivo è stato quello di scegliere un algoritmo di calcolo che rispettasse le caratteristiche dell’articolazione, ed in modo particolare abile a minimizzare gli errori introdotti sia nella fase di acquisizione dei punti di repere anatomici, che in quella legata alla predizione del movimento di flesso-estensione, con un modello matematico.
Per questo motivo abbiamo dovuto realizzare una serie di misure in un primo tempo su due cadaveri di arto superiore, poi, seguendo le regole classiche per la validazione dell’approccio metodologico adottato, si sono realizzate misure in-vivo, prima in massima estensione e poi durante il movimento.
Inizialmente abbiamo pensato di comparare le misure lineari relative alle ampiezze del braccio (ampiezza tra l’epicondilo laterale e mediale) e dell’avambraccio (ampiezza tra lo stiloide ulnare e radiale) con quelle ottenute mediante un antropometro; successivamente
dopo aver verificato la ripetibilità tra i diversi operatori nell’ acquisizione dei punti di repere anatomici con il digitalizzatore Faro Arm, abbiamo comparato le
misure ottenute relative al carrying angle con quelle di un goniometro standard, classicamente utilizzato nella pratica clinica per la definizione dei range di movimento
dell’arto superiore.
Infine, considerando la bontà delle misure ottenute, abbiamo riproposto tale metodologia con stumenti stereofotogrammetrici per l’analisi del movimento (VICON System), ottenendo la stessa stabilit`a nell’andamento del carrying angle in funzione della flessione, sia come riportato dagli studi in letteratura, sia come riscontrato nel nostro studio in-vitro.
In conclusione, questo lavoro di ricerca ha evidenziato (sia per i risultati ottenuti, che per la elevata numerosità dei soggetti testati), come gli esseri umani presentino una grande variabilità individuale nel valore di questo angolo, e di come questo possa aiutare per la corretta definizione di un modello 3-D dell’arto superiore.
Pertanto, gli studi futuri sulla biomeccanica dell’arto superiore dovrebbero includere sempre la valutazione di questa misura.
2
Zampagni, Maria Luisa <1966>. "Studio cinematico dell'articolazione del gomito e valutazione del carrying angle durante l'esercizio fisico." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/136/.
Full textAbstract:
Questo progetto di ricerca, è stato sviluppato per studiare le caratteristiche anatomofunzionali che definiscono l’articolazione del gomito, ed in modo articolare la presenza dell’angolazione valga che origina dalla diversa orientazione degli assi meccanici dell’avambraccio e del braccio e, denominata in letteratura come carrying angle.
L’obiettivo principale di questo lavoro - meglio espresso nei diversi capitoli - è stato, quello di identificare un nuovo approccio di misura per la stima di questo angolo,
utilizzabile sia per gli studi di biomeccanica articolare, che per gli studi di analisi del movimento per l’arto superiore.
Il primo obiettivo è stato quello di scegliere un algoritmo di calcolo che rispettasse le caratteristiche dell’articolazione, ed in modo particolare abile a minimizzare gli errori introdotti sia nella fase di acquisizione dei punti di repere anatomici, che in quella legata alla predizione del movimento di flesso-estensione, con un modello matematico.
Per questo motivo abbiamo dovuto realizzare una serie di misure in un primo tempo su due cadaveri di arto superiore, poi, seguendo le regole classiche per la validazione dell’approccio metodologico adottato, si sono realizzate misure in-vivo, prima in massima estensione e poi durante il movimento.
Inizialmente abbiamo pensato di comparare le misure lineari relative alle ampiezze del braccio (ampiezza tra l’epicondilo laterale e mediale) e dell’avambraccio (ampiezza tra lo stiloide ulnare e radiale) con quelle ottenute mediante un antropometro; successivamente
dopo aver verificato la ripetibilità tra i diversi operatori nell’ acquisizione dei punti di repere anatomici con il digitalizzatore Faro Arm, abbiamo comparato le
misure ottenute relative al carrying angle con quelle di un goniometro standard, classicamente utilizzato nella pratica clinica per la definizione dei range di movimento
dell’arto superiore.
Infine, considerando la bontà delle misure ottenute, abbiamo riproposto tale metodologia con stumenti stereofotogrammetrici per l’analisi del movimento (VICON System), ottenendo la stessa stabilit`a nell’andamento del carrying angle in funzione della flessione, sia come riportato dagli studi in letteratura, sia come riscontrato nel nostro studio in-vitro.
In conclusione, questo lavoro di ricerca ha evidenziato (sia per i risultati ottenuti, che per la elevata numerosità dei soggetti testati), come gli esseri umani presentino una grande variabilità individuale nel valore di questo angolo, e di come questo possa aiutare per la corretta definizione di un modello 3-D dell’arto superiore.
Pertanto, gli studi futuri sulla biomeccanica dell’arto superiore dovrebbero includere sempre la valutazione di questa misura.
3
Dentico, Daniela <1975>. "Mappe funzionali nervose delle modificazioni del ciclo veglia-sonno indotte da esposizione a bassa temperatura ambientale." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/250/1/Tesi_dottorato_daniela_dentico_BIO09.pdf.
Full text
4
Dentico, Daniela <1975>. "Mappe funzionali nervose delle modificazioni del ciclo veglia-sonno indotte da esposizione a bassa temperatura ambientale." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/250/.
Full text
5
Peña, Altamira Luis Emiliano <1979>. "Neurochemical analysis and identification of potentially involved proteins in a mouse model of Amyotrophic Lateral Sclerosis." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/416/1/phdemiliano.pdf.
Full text
6
Peña, Altamira Luis Emiliano <1979>. "Neurochemical analysis and identification of potentially involved proteins in a mouse model of Amyotrophic Lateral Sclerosis." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/416/.
Full text
7
Porro, Antonio <1979>. "Transcription regulation of ABC drug transporters by MYC oncoproteins." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/417/1/Tesi_Antonio_Porro.pdf.
Full text
8
Porro, Antonio <1979>. "Transcription regulation of ABC drug transporters by MYC oncoproteins." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/417/.
Full text
9
Burattini, Costanza <1977>. "Role of the endogenous opioid system in addiction to alcohol and cocaine." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/444/1/Tesi__Burattini.pdf.
Full text
10
Burattini, Costanza <1977>. "Role of the endogenous opioid system in addiction to alcohol and cocaine." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/444/.
Full text
11
Contestabile, Andrea <1971>. "Regulation of transcription factor Lot1 expression during proliferation/differentiation of neuronal cells." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/445/1/Tesi_AndreaContestabile.pdf.
Full text
12
Contestabile, Andrea <1971>. "Regulation of transcription factor Lot1 expression during proliferation/differentiation of neuronal cells." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/445/.
Full text
13
Berteotti, Chiara <1979>. "Central autonomic control in spontaneously hypertensive rats: a study on phasic phenomena during rapid-eye-movement sleep." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/495/1/TesiChiaraBerteotti-1.pdf.
Full textAbstract:
The cardiovascular regulation undergoes wide changes in the different states of sleepwake cycle. In particular, the relationship between spontaneous fluctuations in heart period and arterial pressure clearly shows differences between the two sleep states. In non rapid-eye-movement sleep, heart rhythm is under prevalent baroreflex control,
whereas in rapid-eye-movement sleep central autonomic commands prevail (Zoccoli et al., 2001). Moreover, during rapid-eye-movement sleep the cardiovascular variables show wide fluctuations around their mean value. In particular, during rapid-eyemovement sleep, the arterial pressure shows phasic hypertensive events which are superimposed upon the tonic level of arterial pressure. These phasic increases in arterial pressure are accompanied by an increase in heart rate (Sei & Morita, 1996; Silvani et al., 2005). Thus, rapid-eye-movement sleep may represent an “autonomic stress test” for the cardiovascular system, able to unmask pathological patterns of cardiovascular regulation (Verrier et al. 2005), but this hypothesis has never been tested
experimentally. The aim of this study was to investigate whether rapid-eye-movement sleep may reveal derangements in central autonomic cardiovascular control in an experimental
model of essential hypertension. The study was performed in Spontaneously Hypertensive Rats, which represent the most widely used model of essential hypertension, and allow full control of genetic and environmental confounding factors.
In particular, we analyzed the cardiovascular, electroencephalogram, and electromyogram changes associated with phasic hypertensive events during rapid-eyemovement sleep in Spontaneously Hypertensive Rats and in their genetic Wistar Kyoto control strain. Moreover, we studied also a group of Spontaneously Hypertensive Rats made phenotypically normotensive by means of a chronic treatment with an angiotensin converting enzyme inhibitor, the Enalapril maleate, from the age of four weeks to the end of the experiment. All rats were implanted with electrodes for
electroencephalographic and electromyographic recordings and with an arterial catheter for arterial pressure measurement. After six days for postoperative recovery, the rats were studied for five days, at an age of ten weeks.The study indicated that the peak of mean arterial pressure increase during the phasic hypertensive events in rapid-eye-movement sleep did not differ significantly between Spontaneously Hypertensive Rats and Wistar Kyoto rats, while on the other hand Spontaneously Hypertensive Rats showed a reduced increase in the frequency of theta rhythm and a reduced tachicardia with respect to Wistar Kyoto rats. The same pattern of changes in mean arterial pressure, heart period, and theta frequency was observed between Spontaneously Hypertensive Rats and Spontaneously Hypertensive Rats
treated with Enalapril maleate. Spontaneously Hypertensive Rats do not differ from Wistar Kyoto rats only in terms of arterial hypertension, but also due to multiple unknown genetic differences. Spontaneously Hypertensive Rats were developed by selective breeding of Wistar Kyoto rats based only on the level of arterial pressure. However, in this process, multiple genes possibly unrelated to hypertension may have been selected together with the genetic determinants of hypertension (Carley et al., 2000). This study indicated that Spontaneously Hypertensive Rats differ from Wistar Kyoto rats, but not from Spontaneously Hypertensive Rats treated with Enalapril maleate, in terms of arterial pH and theta frequency. This feature may be due to genetic determinants unrelated to hypertension. In sharp contrast, the persistence of differences in the peak of heart period decrease and the peak of theta frequency increase during phasic hypertensive events between Spontaneously Hypertensive Rats and Spontaneously Hypertensive Rats treated with Enalapril maleate demonstrates that the observed reduction in central autonomic control of the cardiovascular system in Spontaneously Hypertensive Rats is not an irreversible consequence of inherited genetic determinants. Rather, the comparison between Spontaneously Hypertensive Rats and
Spontaneously Hypertensive Rats treated with Enalapril maleate indicates that the observed differences in central autonomic control are the result of the hypertension per se. This work supports the view that the study of cardiovascular regulation in sleep provides fundamental insight on the pathophysiology of hypertension, and may thus contribute to the understanding of this disease, which is a major health problem in European countries (Wolf-Maier et al., 2003) with its burden of cardiac, vascular, and renal complications.
14
Berteotti, Chiara <1979>. "Central autonomic control in spontaneously hypertensive rats: a study on phasic phenomena during rapid-eye-movement sleep." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/495/.
Full textAbstract:
The cardiovascular regulation undergoes wide changes in the different states of sleepwake cycle. In particular, the relationship between spontaneous fluctuations in heart period and arterial pressure clearly shows differences between the two sleep states. In non rapid-eye-movement sleep, heart rhythm is under prevalent baroreflex control,
whereas in rapid-eye-movement sleep central autonomic commands prevail (Zoccoli et al., 2001). Moreover, during rapid-eye-movement sleep the cardiovascular variables show wide fluctuations around their mean value. In particular, during rapid-eyemovement sleep, the arterial pressure shows phasic hypertensive events which are superimposed upon the tonic level of arterial pressure. These phasic increases in arterial pressure are accompanied by an increase in heart rate (Sei & Morita, 1996; Silvani et al., 2005). Thus, rapid-eye-movement sleep may represent an “autonomic stress test” for the cardiovascular system, able to unmask pathological patterns of cardiovascular regulation (Verrier et al. 2005), but this hypothesis has never been tested
experimentally. The aim of this study was to investigate whether rapid-eye-movement sleep may reveal derangements in central autonomic cardiovascular control in an experimental
model of essential hypertension. The study was performed in Spontaneously Hypertensive Rats, which represent the most widely used model of essential hypertension, and allow full control of genetic and environmental confounding factors.
In particular, we analyzed the cardiovascular, electroencephalogram, and electromyogram changes associated with phasic hypertensive events during rapid-eyemovement sleep in Spontaneously Hypertensive Rats and in their genetic Wistar Kyoto control strain. Moreover, we studied also a group of Spontaneously Hypertensive Rats made phenotypically normotensive by means of a chronic treatment with an angiotensin converting enzyme inhibitor, the Enalapril maleate, from the age of four weeks to the end of the experiment. All rats were implanted with electrodes for
electroencephalographic and electromyographic recordings and with an arterial catheter for arterial pressure measurement. After six days for postoperative recovery, the rats were studied for five days, at an age of ten weeks.The study indicated that the peak of mean arterial pressure increase during the phasic hypertensive events in rapid-eye-movement sleep did not differ significantly between Spontaneously Hypertensive Rats and Wistar Kyoto rats, while on the other hand Spontaneously Hypertensive Rats showed a reduced increase in the frequency of theta rhythm and a reduced tachicardia with respect to Wistar Kyoto rats. The same pattern of changes in mean arterial pressure, heart period, and theta frequency was observed between Spontaneously Hypertensive Rats and Spontaneously Hypertensive Rats
treated with Enalapril maleate. Spontaneously Hypertensive Rats do not differ from Wistar Kyoto rats only in terms of arterial hypertension, but also due to multiple unknown genetic differences. Spontaneously Hypertensive Rats were developed by selective breeding of Wistar Kyoto rats based only on the level of arterial pressure. However, in this process, multiple genes possibly unrelated to hypertension may have been selected together with the genetic determinants of hypertension (Carley et al., 2000). This study indicated that Spontaneously Hypertensive Rats differ from Wistar Kyoto rats, but not from Spontaneously Hypertensive Rats treated with Enalapril maleate, in terms of arterial pH and theta frequency. This feature may be due to genetic determinants unrelated to hypertension. In sharp contrast, the persistence of differences in the peak of heart period decrease and the peak of theta frequency increase during phasic hypertensive events between Spontaneously Hypertensive Rats and Spontaneously Hypertensive Rats treated with Enalapril maleate demonstrates that the observed reduction in central autonomic control of the cardiovascular system in Spontaneously Hypertensive Rats is not an irreversible consequence of inherited genetic determinants. Rather, the comparison between Spontaneously Hypertensive Rats and
Spontaneously Hypertensive Rats treated with Enalapril maleate indicates that the observed differences in central autonomic control are the result of the hypertension per se. This work supports the view that the study of cardiovascular regulation in sleep provides fundamental insight on the pathophysiology of hypertension, and may thus contribute to the understanding of this disease, which is a major health problem in European countries (Wolf-Maier et al., 2003) with its burden of cardiac, vascular, and renal complications.
15
Passarelli, Lauretta <1976>. "Studio anatomo-funzionale della parete posteriore del solco parieto-occipitale nel cervello di Macaco." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/624/1/Passarelli_Lauretta_tesi.pdf.
Full text
16
Passarelli, Lauretta <1976>. "Studio anatomo-funzionale della parete posteriore del solco parieto-occipitale nel cervello di Macaco." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2007. http://amsdottorato.unibo.it/624/.
Full text
17
Strillacci, Antonio <1979>. "RNA Interference and cyclooxygenase-2 (COX-2) regulation in colon cancer cells." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/680/1/Tesi_Strillacci_Antonio.pdf.
Full textAbstract:
Despite new methods and combined strategies, conventional cancer chemotherapy still lacks
specificity and induces drug resistance. Gene therapy can offer the potential to obtain the success in
the clinical treatment of cancer and this can be achieved by replacing mutated tumour suppressor
genes, inhibiting gene transcription, introducing new genes encoding for therapeutic products, or
specifically silencing any given target gene. Concerning gene silencing, attention has recently
shifted onto the RNA interference (RNAi) phenomenon. Gene silencing mediated by RNAi
machinery is based on short RNA molecules, small interfering RNAs (siRNAs) and microRNAs
(miRNAs), that are fully o partially homologous to the mRNA of the genes being silenced,
respectively. On one hand, synthetic siRNAs appear as an important research tool to understand the
function of a gene and the prospect of using siRNAs as potent and specific inhibitors of any target
gene provides a new therapeutical approach for many untreatable diseases, particularly cancer. On
the other hand, the discovery of the gene regulatory pathways mediated by miRNAs, offered to the
research community new important perspectives for the comprehension of the physiological and,
above all, the pathological mechanisms underlying the gene regulation. Indeed, changes in miRNAs
expression have been identified in several types of neoplasia and it has also been proposed that the
overexpression of genes in cancer cells may be due to the disruption of a control network in which
relevant miRNA are implicated. For these reasons, I focused my research on a possible link
between RNAi and the enzyme cyclooxygenase-2 (COX-2) in the field of colorectal cancer (CRC),
since it has been established that the transition adenoma-adenocarcinoma and the progression of
CRC depend on aberrant constitutive expression of COX-2 gene. In fact, overexpressed COX-2 is
involved in the block of apoptosis, the stimulation of tumor-angiogenesis and promotes cell
invasion, tumour growth and metastatization.
On the basis of data reported in the literature, the first aim of my research was to develop an
innovative and effective tool, based on the RNAi mechanism, able to silence strongly and
specifically COX-2 expression in human colorectal cancer cell lines. In this study, I firstly show
that an siRNA sequence directed against COX-2 mRNA (siCOX-2), potently downregulated COX-2
gene expression in human umbilical vein endothelial cells (HUVEC) and inhibited PMA-induced
angiogenesis in vitro in a specific, non-toxic manner. Moreover, I found that the insertion of a
specific cassette carrying anti-COX-2 shRNA sequence (shCOX-2, the precursor of siCOX-2
previously tested) into a viral vector (pSUPER.retro) greatly increased silencing potency in a colon
cancer cell line (HT-29) without activating any interferon response. Phenotypically, COX-2
deficient HT-29 cells showed a significant impairment of their in vitro malignant behaviour. Thus,
results reported here indicate an easy-to-use, powerful and high selective virus-based method to
knockdown COX-2 gene in a stable and long-lasting manner, in colon cancer cells. Furthermore,
they open up the possibility of an in vivo application of this anti-COX-2 retroviral vector, as
therapeutic agent for human cancers overexpressing COX-2.
In order to improve the tumour selectivity, pSUPER.retro vector was modified for the shCOX-2
expression cassette. The aim was to obtain a strong, specific transcription of shCOX-2 followed by
COX-2 silencing mediated by siCOX-2 only in cancer cells. For this reason, H1 promoter in basic
pSUPER.retro vector [pS(H1)] was substituted with the human Cox-2 promoter [pS(COX2)] and
with a promoter containing repeated copies of the TCF binding element (TBE) [pS(TBE)]. These
promoters were choosen because they are partculary activated in colon cancer cells. COX-2 was
effectively silenced in HT-29 and HCA-7 colon cancer cells by using enhanced pS(COX2) and
pS(TBE) vectors. In particular, an higher siCOX-2 production followed by a stronger inhibition of
Cox-2 gene were achieved by using pS(TBE) vector, that represents not only the most effective, but
also the most specific system to downregulate COX-2 in colon cancer cells.
Because of the many limits that a retroviral therapy could have in a possible in vivo treatment of
CRC, the next goal was to render the enhanced RNAi-mediate COX-2 silencing more suitable for
this kind of application. Xiang and et al. (2006) demonstrated that it is possible to induce RNAi in
mammalian cells after infection with engineered E. Coli strains expressing Inv and HlyA genes,
which encode for two bacterial factors needed for successful transfer of shRNA in mammalian
cells. This system, called “trans-kingdom” RNAi (tkRNAi) could represent an optimal approach for
the treatment of colorectal cancer, since E. Coli in normally resident in human intestinal flora and
could easily vehicled to the tumor tissue. For this reason, I tested the improved COX-2 silencing
mediated by pS(COX2) and pS(TBE) vectors by using tkRNAi system. Results obtained in HT-29
and HCA-7 cell lines were in high agreement with data previously collected after the transfection of
pS(COX2) and pS(TBE) vectors in the same cell lines. These findings suggest that tkRNAi system
for COX-2 silencing, in particular mediated by pS(TBE) vector, could represent a promising tool
for the treatment of colorectal cancer.
Flanking the studies addressed to the setting-up of a RNAi-mediated therapeutical strategy, I
proposed to get ahead with the comprehension of new molecular basis of human colorectal cancer.
In particular, it is known that components of the miRNA/RNAi pathway may be altered during the
progressive development of colorectal cancer (CRC), and it has been already demonstrated that
some miRNAs work as tumor suppressors or oncomiRs in colon cancer. Thus, my hypothesis was
that overexpressed COX-2 protein in colon cancer could be the result of decreased levels of one or
more tumor suppressor miRNAs.
In this thesis, I clearly show an inverse correlation between COX-2 expression and the human miR-
101(1) levels in colon cancer cell lines, tissues and metastases. I also demonstrate that the in vitro
modulating of miR-101(1) expression in colon cancer cell lines leads to significant variations in
COX-2 expression, and this phenomenon is based on a direct interaction between miR-101(1) and
COX-2 mRNA. Moreover, I started to investigate miR-101(1) regulation in the hypoxic
environment since adaptation to hypoxia is critical for tumor cell growth and survival and it is
known that COX-2 can be induced directly by hypoxia-inducible factor 1 (HIF-1). Surprisingly, I
observed that COX-2 overexpression induced by hypoxia is always coupled to a significant
decrease of miR-101(1) levels in colon cancer cell lines, suggesting that miR-101(1) regulation
could be involved in the adaption of cancer cells to the hypoxic environment that strongly
characterize CRC tissues.
18
Strillacci, Antonio <1979>. "RNA Interference and cyclooxygenase-2 (COX-2) regulation in colon cancer cells." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/680/.
Full textAbstract:
Despite new methods and combined strategies, conventional cancer chemotherapy still lacks
specificity and induces drug resistance. Gene therapy can offer the potential to obtain the success in
the clinical treatment of cancer and this can be achieved by replacing mutated tumour suppressor
genes, inhibiting gene transcription, introducing new genes encoding for therapeutic products, or
specifically silencing any given target gene. Concerning gene silencing, attention has recently
shifted onto the RNA interference (RNAi) phenomenon. Gene silencing mediated by RNAi
machinery is based on short RNA molecules, small interfering RNAs (siRNAs) and microRNAs
(miRNAs), that are fully o partially homologous to the mRNA of the genes being silenced,
respectively. On one hand, synthetic siRNAs appear as an important research tool to understand the
function of a gene and the prospect of using siRNAs as potent and specific inhibitors of any target
gene provides a new therapeutical approach for many untreatable diseases, particularly cancer. On
the other hand, the discovery of the gene regulatory pathways mediated by miRNAs, offered to the
research community new important perspectives for the comprehension of the physiological and,
above all, the pathological mechanisms underlying the gene regulation. Indeed, changes in miRNAs
expression have been identified in several types of neoplasia and it has also been proposed that the
overexpression of genes in cancer cells may be due to the disruption of a control network in which
relevant miRNA are implicated. For these reasons, I focused my research on a possible link
between RNAi and the enzyme cyclooxygenase-2 (COX-2) in the field of colorectal cancer (CRC),
since it has been established that the transition adenoma-adenocarcinoma and the progression of
CRC depend on aberrant constitutive expression of COX-2 gene. In fact, overexpressed COX-2 is
involved in the block of apoptosis, the stimulation of tumor-angiogenesis and promotes cell
invasion, tumour growth and metastatization.
On the basis of data reported in the literature, the first aim of my research was to develop an
innovative and effective tool, based on the RNAi mechanism, able to silence strongly and
specifically COX-2 expression in human colorectal cancer cell lines. In this study, I firstly show
that an siRNA sequence directed against COX-2 mRNA (siCOX-2), potently downregulated COX-2
gene expression in human umbilical vein endothelial cells (HUVEC) and inhibited PMA-induced
angiogenesis in vitro in a specific, non-toxic manner. Moreover, I found that the insertion of a
specific cassette carrying anti-COX-2 shRNA sequence (shCOX-2, the precursor of siCOX-2
previously tested) into a viral vector (pSUPER.retro) greatly increased silencing potency in a colon
cancer cell line (HT-29) without activating any interferon response. Phenotypically, COX-2
deficient HT-29 cells showed a significant impairment of their in vitro malignant behaviour. Thus,
results reported here indicate an easy-to-use, powerful and high selective virus-based method to
knockdown COX-2 gene in a stable and long-lasting manner, in colon cancer cells. Furthermore,
they open up the possibility of an in vivo application of this anti-COX-2 retroviral vector, as
therapeutic agent for human cancers overexpressing COX-2.
In order to improve the tumour selectivity, pSUPER.retro vector was modified for the shCOX-2
expression cassette. The aim was to obtain a strong, specific transcription of shCOX-2 followed by
COX-2 silencing mediated by siCOX-2 only in cancer cells. For this reason, H1 promoter in basic
pSUPER.retro vector [pS(H1)] was substituted with the human Cox-2 promoter [pS(COX2)] and
with a promoter containing repeated copies of the TCF binding element (TBE) [pS(TBE)]. These
promoters were choosen because they are partculary activated in colon cancer cells. COX-2 was
effectively silenced in HT-29 and HCA-7 colon cancer cells by using enhanced pS(COX2) and
pS(TBE) vectors. In particular, an higher siCOX-2 production followed by a stronger inhibition of
Cox-2 gene were achieved by using pS(TBE) vector, that represents not only the most effective, but
also the most specific system to downregulate COX-2 in colon cancer cells.
Because of the many limits that a retroviral therapy could have in a possible in vivo treatment of
CRC, the next goal was to render the enhanced RNAi-mediate COX-2 silencing more suitable for
this kind of application. Xiang and et al. (2006) demonstrated that it is possible to induce RNAi in
mammalian cells after infection with engineered E. Coli strains expressing Inv and HlyA genes,
which encode for two bacterial factors needed for successful transfer of shRNA in mammalian
cells. This system, called “trans-kingdom” RNAi (tkRNAi) could represent an optimal approach for
the treatment of colorectal cancer, since E. Coli in normally resident in human intestinal flora and
could easily vehicled to the tumor tissue. For this reason, I tested the improved COX-2 silencing
mediated by pS(COX2) and pS(TBE) vectors by using tkRNAi system. Results obtained in HT-29
and HCA-7 cell lines were in high agreement with data previously collected after the transfection of
pS(COX2) and pS(TBE) vectors in the same cell lines. These findings suggest that tkRNAi system
for COX-2 silencing, in particular mediated by pS(TBE) vector, could represent a promising tool
for the treatment of colorectal cancer.
Flanking the studies addressed to the setting-up of a RNAi-mediated therapeutical strategy, I
proposed to get ahead with the comprehension of new molecular basis of human colorectal cancer.
In particular, it is known that components of the miRNA/RNAi pathway may be altered during the
progressive development of colorectal cancer (CRC), and it has been already demonstrated that
some miRNAs work as tumor suppressors or oncomiRs in colon cancer. Thus, my hypothesis was
that overexpressed COX-2 protein in colon cancer could be the result of decreased levels of one or
more tumor suppressor miRNAs.
In this thesis, I clearly show an inverse correlation between COX-2 expression and the human miR-
101(1) levels in colon cancer cell lines, tissues and metastases. I also demonstrate that the in vitro
modulating of miR-101(1) expression in colon cancer cell lines leads to significant variations in
COX-2 expression, and this phenomenon is based on a direct interaction between miR-101(1) and
COX-2 mRNA. Moreover, I started to investigate miR-101(1) regulation in the hypoxic
environment since adaptation to hypoxia is critical for tumor cell growth and survival and it is
known that COX-2 can be induced directly by hypoxia-inducible factor 1 (HIF-1). Surprisingly, I
observed that COX-2 overexpression induced by hypoxia is always coupled to a significant
decrease of miR-101(1) levels in colon cancer cell lines, suggesting that miR-101(1) regulation
could be involved in the adaption of cancer cells to the hypoxic environment that strongly
characterize CRC tissues.
19
Rizzi, Simona <1971>. "Effects of environmental complexity on neurogenesis in the hippocampal dentate gyrus." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/988/1/Tesi_Rizzi_Simona.pdf.
Full textAbstract:
Introduction. Postnatal neurogenesis in the hippocampal dentate gyrus, can be modulated by numerous determinants, such as hormones, transmitters and stress. Among the factors positively interfering with neurogenesis, the complexity of the environment appears to play a particularly striking role. Adult mice reared in an enriched environment produce more neurons and exhibit better performance in hippocampus-specific learning tasks. While the effects of complex environments on hippocampal neurogenesis are well documented, there is a lack of information on the effects of living under socio-sensory deprivation conditions. Due to the immaturity of rats and mice at birth, studies dealing with the effects of environmental enrichment on hippocampal neurogenesis were carried out in adult animals, i.e. during a period of relatively low rate of neurogenesis. The impact of environment is likely to be more dramatic during the first postnatal weeks, because at this time granule cell production is remarkably higher than at later phases of development.
The aim of the present research was to clarify whether and to what extent isolated or enriched rearing conditions affect hippocampal neurogenesis during the early postnatal period, a time window characterized by a high rate of precursor proliferation and to elucidate the mechanisms underlying these effects. The experimental model chosen for this research was the guinea pig, a precocious rodent, which, at 4-5 days of age can be independent from maternal care.
Experimental design. Animals were assigned to a standard (control), an isolated, or an enriched environment a few days after birth (P5-P6). On P14-P17 animals received one daily bromodeoxyuridine (BrdU) injection, to label dividing cells, and were sacrificed either on P18, to evaluate cell proliferation or on P45, to evaluate cell survival and differentiation.
Methods. Brain sections were processed for BrdU immunhistochemistry, to quantify the new born and surviving cells. The phenotype of the surviving cells was examined by means of confocal microscopy and immunofluorescent double-labeling for BrdU and either a marker of neurons (NeuN) or a marker of astrocytes (GFAP). Apoptotic cell death was examined with the TUNEL method. Serial sections were processed for immunohistochemistry for i) vimentin, a marker of radial glial cells, ii) BDNF (brain-derived neurotrofic factor), a neurotrophin involved in neuron proliferation/survival, iii) PSA-NCAM (the polysialylated form of the neural cell adhesion molecule), a molecule associated with neuronal migration. Total granule cell number in the dentate gyrus was evaluated by stereological methods, in Nissl-stained sections.
Results. Effects of isolation. In P18 isolated animals we found a reduced cell proliferation (-35%) compared to controls and a lower expression of BDNF. Though in absolute terms P45 isolated
animals had less surviving cells than controls, they showed no differences in survival rate and phenotype percent distribution compared to controls. Evaluation of the absolute number of surviving cells of each phenotype showed that isolated animals had a reduced number of cells with neuronal phenotype than controls. Looking at the location of the new neurons, we found that while in control animals 76% of them had migrated to the granule cell layer, in isolated animals only 55% of the new neurons had reached this layer. Examination of radial glia cells of P18 and P45 animals by vimentin immunohistochemistry showed that in isolated animals radial glia cells were reduced in density and had less and shorter processes. Granule cell count revealed that isolated animals had less granule cells than controls (-32% at P18 and -42% at P45). Effects of enrichment. In P18 enriched animals there was an increase in cell proliferation (+26%) compared to controls and a higher expression of BDNF. Though in both groups there was a decline in the number of BrdU-positive cells by P45, enriched animals had more surviving cells (+63) and a higher survival rate than controls. No differences were found between control and enriched animals in phenotype percent distribution. Evaluation of the absolute number of cells of each phenotype showed that enriched animals had a larger number of cells of each phenotype than controls. Looking at the location of cells of each phenotype we found that enriched animals had more new neurons in the granule cell layer and more astrocytes and cells with undetermined phenotype in the hilus. Enriched animals had a higher expression of PSA-NCAM in the granule cell layer and hilus Vimentin immunohistochemistry showed that in enriched animals radial glia cells were more numerous and had more processes.. Granule cell count revealed that enriched animals had more granule cells than controls (+37% at P18 and +31% at P45).
Discussion. Results show that isolation rearing reduces hippocampal cell proliferation but does not affect cell survival, while enriched rearing increases both cell proliferation and cell survival. Changes in the expression of BDNF are likely to contribute to he effects of environment on precursor cell proliferation. The reduction and increase in final number of granule neurons in isolated and enriched animals, respectively, are attributable to the effects of environment on cell proliferation and survival and not to changes in the differentiation program. As radial glia cells play a pivotal role in neuron guidance to the granule cell layer, the reduced number of radial glia cells in isolated animals and the increased number in enriched animals suggests that the size of radial glia population may change dynamically, in order to match changes in neuron production. The high PSA-NCAM expression in enriched animals may concur to favor the survival of the new neurons by facilitating their migration to the granule cell layer.
Conclusions. By using a precocious rodent we could demonstrate that isolated/enriched rearing conditions, at a time window during which intense granule cell proliferation takes place, lead to a
notable decrease/increase of total granule cell number. The time-course and magnitude of postnatal granule cell production in guinea pigs are more similar to the human and non-human primate condition than in rats and mice. Translation of current data to humans would imply that exposure of children to environments poor/rich of stimuli may have a notably large impact on dentate neurogenesis and, very likely, on hippocampus dependent memory functions.
20
Rizzi, Simona <1971>. "Effects of environmental complexity on neurogenesis in the hippocampal dentate gyrus." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/988/.
Full textAbstract:
Introduction. Postnatal neurogenesis in the hippocampal dentate gyrus, can be modulated by numerous determinants, such as hormones, transmitters and stress. Among the factors positively interfering with neurogenesis, the complexity of the environment appears to play a particularly striking role. Adult mice reared in an enriched environment produce more neurons and exhibit better performance in hippocampus-specific learning tasks. While the effects of complex environments on hippocampal neurogenesis are well documented, there is a lack of information on the effects of living under socio-sensory deprivation conditions. Due to the immaturity of rats and mice at birth, studies dealing with the effects of environmental enrichment on hippocampal neurogenesis were carried out in adult animals, i.e. during a period of relatively low rate of neurogenesis. The impact of environment is likely to be more dramatic during the first postnatal weeks, because at this time granule cell production is remarkably higher than at later phases of development.
The aim of the present research was to clarify whether and to what extent isolated or enriched rearing conditions affect hippocampal neurogenesis during the early postnatal period, a time window characterized by a high rate of precursor proliferation and to elucidate the mechanisms underlying these effects. The experimental model chosen for this research was the guinea pig, a precocious rodent, which, at 4-5 days of age can be independent from maternal care.
Experimental design. Animals were assigned to a standard (control), an isolated, or an enriched environment a few days after birth (P5-P6). On P14-P17 animals received one daily bromodeoxyuridine (BrdU) injection, to label dividing cells, and were sacrificed either on P18, to evaluate cell proliferation or on P45, to evaluate cell survival and differentiation.
Methods. Brain sections were processed for BrdU immunhistochemistry, to quantify the new born and surviving cells. The phenotype of the surviving cells was examined by means of confocal microscopy and immunofluorescent double-labeling for BrdU and either a marker of neurons (NeuN) or a marker of astrocytes (GFAP). Apoptotic cell death was examined with the TUNEL method. Serial sections were processed for immunohistochemistry for i) vimentin, a marker of radial glial cells, ii) BDNF (brain-derived neurotrofic factor), a neurotrophin involved in neuron proliferation/survival, iii) PSA-NCAM (the polysialylated form of the neural cell adhesion molecule), a molecule associated with neuronal migration. Total granule cell number in the dentate gyrus was evaluated by stereological methods, in Nissl-stained sections.
Results. Effects of isolation. In P18 isolated animals we found a reduced cell proliferation (-35%) compared to controls and a lower expression of BDNF. Though in absolute terms P45 isolated
animals had less surviving cells than controls, they showed no differences in survival rate and phenotype percent distribution compared to controls. Evaluation of the absolute number of surviving cells of each phenotype showed that isolated animals had a reduced number of cells with neuronal phenotype than controls. Looking at the location of the new neurons, we found that while in control animals 76% of them had migrated to the granule cell layer, in isolated animals only 55% of the new neurons had reached this layer. Examination of radial glia cells of P18 and P45 animals by vimentin immunohistochemistry showed that in isolated animals radial glia cells were reduced in density and had less and shorter processes. Granule cell count revealed that isolated animals had less granule cells than controls (-32% at P18 and -42% at P45). Effects of enrichment. In P18 enriched animals there was an increase in cell proliferation (+26%) compared to controls and a higher expression of BDNF. Though in both groups there was a decline in the number of BrdU-positive cells by P45, enriched animals had more surviving cells (+63) and a higher survival rate than controls. No differences were found between control and enriched animals in phenotype percent distribution. Evaluation of the absolute number of cells of each phenotype showed that enriched animals had a larger number of cells of each phenotype than controls. Looking at the location of cells of each phenotype we found that enriched animals had more new neurons in the granule cell layer and more astrocytes and cells with undetermined phenotype in the hilus. Enriched animals had a higher expression of PSA-NCAM in the granule cell layer and hilus Vimentin immunohistochemistry showed that in enriched animals radial glia cells were more numerous and had more processes.. Granule cell count revealed that enriched animals had more granule cells than controls (+37% at P18 and +31% at P45).
Discussion. Results show that isolation rearing reduces hippocampal cell proliferation but does not affect cell survival, while enriched rearing increases both cell proliferation and cell survival. Changes in the expression of BDNF are likely to contribute to he effects of environment on precursor cell proliferation. The reduction and increase in final number of granule neurons in isolated and enriched animals, respectively, are attributable to the effects of environment on cell proliferation and survival and not to changes in the differentiation program. As radial glia cells play a pivotal role in neuron guidance to the granule cell layer, the reduced number of radial glia cells in isolated animals and the increased number in enriched animals suggests that the size of radial glia population may change dynamically, in order to match changes in neuron production. The high PSA-NCAM expression in enriched animals may concur to favor the survival of the new neurons by facilitating their migration to the granule cell layer.
Conclusions. By using a precocious rodent we could demonstrate that isolated/enriched rearing conditions, at a time window during which intense granule cell proliferation takes place, lead to a
notable decrease/increase of total granule cell number. The time-course and magnitude of postnatal granule cell production in guinea pigs are more similar to the human and non-human primate condition than in rats and mice. Translation of current data to humans would imply that exposure of children to environments poor/rich of stimuli may have a notably large impact on dentate neurogenesis and, very likely, on hippocampus dependent memory functions.
21
Del, Sindaco Elide <1980>. "Studio dei meccanismi di regolazione a lungo termine della comparsa del sonno REM nel ratto." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/989/1/Tesi_Del_Sindaco_Elide.pdf.
Full text
22
Del, Sindaco Elide <1980>. "Studio dei meccanismi di regolazione a lungo termine della comparsa del sonno REM nel ratto." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/989/.
Full text
23
Fila, Tatiana <1978>. "Neurogenesis impairment and cell cycle alterations in Down Syndrome." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/990/1/Tesi_Fila_Tatiana.pdf.
Full text
24
Fila, Tatiana <1978>. "Neurogenesis impairment and cell cycle alterations in Down Syndrome." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/990/.
Full text
25
Donnini, Filippo <1975>. "Strategie di monitoraggio mediante biomarker e organismi sentinella applicate a zone umide e costiere." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/1032/1/Tesi_Donnini_Filippo.pdf.
Full text
26
Donnini, Filippo <1975>. "Strategie di monitoraggio mediante biomarker e organismi sentinella applicate a zone umide e costiere." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2008. http://amsdottorato.unibo.it/1032/.
Full text
27
Balietti, Marta <1974>. "Morphological and functional study of cerebral aging in rat." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1418/1/Balietti_Marta_Tesi.pdf.
Full textAbstract:
Aging is a physiological process characterized by a progressive decline of the “cellular homeostatic reserve”, refereed as the capability to respond suitably to exogenous and endogenous stressful stimuli. Due to their high energetic requests and post-mitotic nature, neurons are peculiarly susceptible to this phenomenon. However, the aged brain maintains a certain level of adaptive capacities and if properly stimulated may warrant a considerable functional recovery.
Aim of the present research was to verify the plastic potentialities of the aging brain of rats subjected to two kind of exogenous stimuli: A) the replacement of the standard diet with a ketogenic regimen (the change forces the brain to use ketone bodies (KB) in alternative to glucose to satisfy the energetic needs) and B) a behavioural task able to induce the formation of inhibitory avoidance memory.
A) Fifteen male Wistar rats of 19 months of age were divided into three groups (average body weight pair-matched), and fed for 8 weeks with different dietary regimens: i) diet containing 10% medium chain triglycerides (MCT); ii) diet containing 20% MCT; iii) standard commercial chow. Five young (5 months of age) and five old (26-27 months of age) animals fed with the standard diet were used as further controls. The following morphological parameters reflecting synaptic plasticity were evaluated in the stratum moleculare of the hippocampal CA1 region (SM CA1), in the outer molecular layer of the hippocampal dentate gyrus (OML DG), and in the granule cell layer of the cerebellar cortex (GCL-CCx): average area (S), numeric density (Nvs), and surface density (Sv) of synapses, and average volume (V), numeric density (Nvm), and volume density (Vv) of synaptic mitochondria. Moreover, succinic dehydrogenase (SDH) activity was cytochemically determined in Purkinje cells (PC) and V, Nvm, Vv, and cytochemical precipitate area/mitochondrial area (R) of SDH-positive mitochondria were evaluated.
In SM CA1, MCT-KDs induced the early appearance of the morphological patterns typical of old animals: higher S and V, and lower Nvs and Nvm. On the contrary, in OML DG, Sv and Vv of MCT-KDs-fed rats were higher (as a result of higher Nvs and Nvm) vs. controls; these modifications are known to improve synaptic function and metabolic supply. The opposite effects of MCT-KDs might reflect the different susceptibility of these brain regions to the aging processes: OML DG is less vulnerable than SM CA1, and the reactivation of ketone bodies uptake and catabolism might occur more efficiently in this region, allowing the exploitation of their peculiar metabolic properties. In GCL-CCx, the results described a new scenario in comparison to that found in the hippocampal formation: 10%MCT-KD induced the early appearance of senescent patterns (decreased Nvs and Nvm; increased V), whereas 20%MCT-KD caused no changes. Since GCL-CCx is more vulnerable to age than DG, and less than CA1, these data further support the hypothesis that MCT-KDs effects in the aging brain critically depend on neuronal vulnerability to age, besides MCT percentage. Regarding PC, it was decided to evaluate only the metabolic effect of the dietetic regimen (20%MCT-KD) characterized by less side effects. KD counteracted age-related decrease in numeric density of SDH-positive mitochondria, and enhanced their energetic efficiency (R was significantly higher in MCT-KD-fed rats vs. all the controls). Since it is well known that Purkinje and dentate gyrus cells are less vulnerable to aging than CA1 neurons, these results corroborate our previous hypothesis.
In conclusion, the A) experimental line provides the first evidence that morphological and functional parameters reflecting synaptic plasticity and mitochondrial metabolic competence may be modulated by MCT-KDs in the pre-senescent central nervous system, and that the effects may be heterogeneous in different brain regions. MCT-KDs seem to supply high energy metabolic intermediates and to be beneficial (“anti-aging”) for those neurons that maintain the capability to exploit them. This implies risks but also promising potentialities for the therapeutic use of these diets during aging
B) Morphological parameters of synapses and synaptic mitochondria in SM CA1 were investigated in old (26-27 month-old) female Wistar rats following a single trial inhibitory avoidance task. In this memory protocol animals learn to avoid a dark compartment in which they received a mild, inescapable foot-shock. Rats were tested 3 and 6 or 9 hours after the training, divided into good and bad responders according to their performance (retention times above or below 100 s, respectively) and immediately sacrificed. Nvs, S, Sv, Nvm, V, and Vv were evaluated. In the good responder group, the numeric density of synapses and mitochondria was significantly higher and the average mitochondrial volume was significantly smaller 9 hours vs. 6 hours after the training. No significant differences were observed among bad responders. Thus, better performances in passive avoidance memory task are correlated with more efficient plastic remodeling of synaptic contacts and mitochondria in hippocampal CA1. These findings indicate that maintenance of synaptic plastic reactivity during aging is a critical requirement for preserving long-term memory consolidation.
28
Balietti, Marta <1974>. "Morphological and functional study of cerebral aging in rat." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1418/.
Full textAbstract:
Aging is a physiological process characterized by a progressive decline of the “cellular homeostatic reserve”, refereed as the capability to respond suitably to exogenous and endogenous stressful stimuli. Due to their high energetic requests and post-mitotic nature, neurons are peculiarly susceptible to this phenomenon. However, the aged brain maintains a certain level of adaptive capacities and if properly stimulated may warrant a considerable functional recovery.
Aim of the present research was to verify the plastic potentialities of the aging brain of rats subjected to two kind of exogenous stimuli: A) the replacement of the standard diet with a ketogenic regimen (the change forces the brain to use ketone bodies (KB) in alternative to glucose to satisfy the energetic needs) and B) a behavioural task able to induce the formation of inhibitory avoidance memory.
A) Fifteen male Wistar rats of 19 months of age were divided into three groups (average body weight pair-matched), and fed for 8 weeks with different dietary regimens: i) diet containing 10% medium chain triglycerides (MCT); ii) diet containing 20% MCT; iii) standard commercial chow. Five young (5 months of age) and five old (26-27 months of age) animals fed with the standard diet were used as further controls. The following morphological parameters reflecting synaptic plasticity were evaluated in the stratum moleculare of the hippocampal CA1 region (SM CA1), in the outer molecular layer of the hippocampal dentate gyrus (OML DG), and in the granule cell layer of the cerebellar cortex (GCL-CCx): average area (S), numeric density (Nvs), and surface density (Sv) of synapses, and average volume (V), numeric density (Nvm), and volume density (Vv) of synaptic mitochondria. Moreover, succinic dehydrogenase (SDH) activity was cytochemically determined in Purkinje cells (PC) and V, Nvm, Vv, and cytochemical precipitate area/mitochondrial area (R) of SDH-positive mitochondria were evaluated.
In SM CA1, MCT-KDs induced the early appearance of the morphological patterns typical of old animals: higher S and V, and lower Nvs and Nvm. On the contrary, in OML DG, Sv and Vv of MCT-KDs-fed rats were higher (as a result of higher Nvs and Nvm) vs. controls; these modifications are known to improve synaptic function and metabolic supply. The opposite effects of MCT-KDs might reflect the different susceptibility of these brain regions to the aging processes: OML DG is less vulnerable than SM CA1, and the reactivation of ketone bodies uptake and catabolism might occur more efficiently in this region, allowing the exploitation of their peculiar metabolic properties. In GCL-CCx, the results described a new scenario in comparison to that found in the hippocampal formation: 10%MCT-KD induced the early appearance of senescent patterns (decreased Nvs and Nvm; increased V), whereas 20%MCT-KD caused no changes. Since GCL-CCx is more vulnerable to age than DG, and less than CA1, these data further support the hypothesis that MCT-KDs effects in the aging brain critically depend on neuronal vulnerability to age, besides MCT percentage. Regarding PC, it was decided to evaluate only the metabolic effect of the dietetic regimen (20%MCT-KD) characterized by less side effects. KD counteracted age-related decrease in numeric density of SDH-positive mitochondria, and enhanced their energetic efficiency (R was significantly higher in MCT-KD-fed rats vs. all the controls). Since it is well known that Purkinje and dentate gyrus cells are less vulnerable to aging than CA1 neurons, these results corroborate our previous hypothesis.
In conclusion, the A) experimental line provides the first evidence that morphological and functional parameters reflecting synaptic plasticity and mitochondrial metabolic competence may be modulated by MCT-KDs in the pre-senescent central nervous system, and that the effects may be heterogeneous in different brain regions. MCT-KDs seem to supply high energy metabolic intermediates and to be beneficial (“anti-aging”) for those neurons that maintain the capability to exploit them. This implies risks but also promising potentialities for the therapeutic use of these diets during aging
B) Morphological parameters of synapses and synaptic mitochondria in SM CA1 were investigated in old (26-27 month-old) female Wistar rats following a single trial inhibitory avoidance task. In this memory protocol animals learn to avoid a dark compartment in which they received a mild, inescapable foot-shock. Rats were tested 3 and 6 or 9 hours after the training, divided into good and bad responders according to their performance (retention times above or below 100 s, respectively) and immediately sacrificed. Nvs, S, Sv, Nvm, V, and Vv were evaluated. In the good responder group, the numeric density of synapses and mitochondria was significantly higher and the average mitochondrial volume was significantly smaller 9 hours vs. 6 hours after the training. No significant differences were observed among bad responders. Thus, better performances in passive avoidance memory task are correlated with more efficient plastic remodeling of synaptic contacts and mitochondria in hippocampal CA1. These findings indicate that maintenance of synaptic plastic reactivity during aging is a critical requirement for preserving long-term memory consolidation.
29
Monaco, Simona <1978>. "Contribution of Vision and Proprioception to the Precision of Reaching Movements." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1540/1/Monaco_Simona_tesi.pdf.
Full textAbstract:
Ren and colleagues (2006) found that saccades to visual targets became less accurate when somatosensory information about hand location was added, suggesting that saccades rely mainly on vision. We conducted two kinematic experiments to examine whether or not reaching movements would also show such strong reliance on vision. In Experiment 1, subjects used their dominant right hand to perform reaches, with or without a delay, to an external visual target or to their own left fingertip positioned either by the experimenter or by the participant. Unlike saccades, reaches became more accurate and precise when proprioceptive information was available. In Experiment 2, subjects reached toward external or bodily targets with differing amounts of visual information. Proprioception improved performance only when vision was limited. Our results indicate that reaching movements, unlike saccades, are improved rather than impaired by the addition of somatosensory information.
30
Monaco, Simona <1978>. "Contribution of Vision and Proprioception to the Precision of Reaching Movements." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1540/.
Full textAbstract:
Ren and colleagues (2006) found that saccades to visual targets became less accurate when somatosensory information about hand location was added, suggesting that saccades rely mainly on vision. We conducted two kinematic experiments to examine whether or not reaching movements would also show such strong reliance on vision. In Experiment 1, subjects used their dominant right hand to perform reaches, with or without a delay, to an external visual target or to their own left fingertip positioned either by the experimenter or by the participant. Unlike saccades, reaches became more accurate and precise when proprioceptive information was available. In Experiment 2, subjects reached toward external or bodily targets with differing amounts of visual information. Proprioception improved performance only when vision was limited. Our results indicate that reaching movements, unlike saccades, are improved rather than impaired by the addition of somatosensory information.
31
Filippini, Daniela <1978>. "Controllo dell'atto di prensione: coinvolgimento dell'area V6A nell'orientamento del polso." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1649/1/Filippini_Daniela_tesi.pdf.
Full textAbstract:
Prehension in an act of coordinated reaching and grasping. The reaching component is concerned with bringing the hand to object to be grasped (transport phase); the grasping component refers to the shaping of the hand according to the object features (grasping phase) (Jeannerod, 1981). Reaching and grasping involve different muscles, proximal and distal muscles respectively, and are controlled by different parietofrontal circuit (Jeannerod et al., 1995): a medial circuit, involving area of superior parietal lobule and dorsal premotor area 6 (PMd) (dorsomedial visual stream), is mainly concerned with reaching; a lateral circuit, involving the inferior parietal lobule and ventral premotor area 6 (PMv) (dorsolateral visual stream), with grasping. Area V6A is located in the caudalmost part of the superior parietal lobule, so it belongs to the dorsomedial visual stream; it contains neurons sensitive to visual stimuli (Galletti et al. 1993, 1996, 1999) as well as cells sensitive to the direction of gaze (Galletti et al. 1995) and cells showing saccade-related activity (Nakamura et al. 1999; Kutz et al. 2003). Area V6A contains also arm-reaching neurons likely involved in the control of the direction of the arm during movements towards objects in the peripersonal space (Galletti et al. 1997; Fattori et al. 2001). The present results confirm this finding and demonstrate that during the reach-to-grasp the V6A neurons are also modulated by the orientation of the wrist.
Experiments were approved by the Bioethical Committee of the University of Bologna and were performed in accordance with National laws on care and use of laboratory animals and with the European Communities Council Directive of 24th November 1986 (86/609/EEC), recently revised by the Council of Europe guidelines (Appendix A of Convention ETS 123).
Experiments were performed in two awake Macaca fascicularis. Each monkey was trained to sit in a primate chair with the head restrained to perform reaching and grasping arm movements in complete darkness while gazing a small fixation point. The object to be grasped was a handle that could have different orientation. We recorded neural activity from 163 neurons of the anterior parietal sulcus; 116/163 (71%) neurons were modulated by the reach-to-grasp task during the execution of the forward movements toward the target (epoch MOV), 111/163 (68%) during the pulling of the handle (epoch HOLD) and 102/163 during the execution of backward movements (epoch M2) (t_test, p ≤ 0.05). About the 45% of the tested cells turned out to be sensitive to the orientation of the handle (one way ANOVA, p ≤ 0.05).
To study how the distal components of the movement, such as the hand preshaping during the reaching of the handle, could influence the neuronal discharge, we compared the neuronal activity during the reaching movements towards the same spatial location in reach-to-point and reach-to-grasp tasks. Both tasks required proximal arm movements; only the reach-to-grasp task required distal movements to orient the wrist and to shape the hand to grasp the handle. The 56% of V6A cells showed significant differences in the neural discharge (one way ANOVA, p ≤ 0.05) between the reach-to-point and the reach-to-grasp tasks during MOV, 54% during HOLD and 52% during M2. These data show that reaching and grasping are processed by the same population of neurons, providing evidence that the coordination of reaching and grasping takes place much earlier than previously thought, i.e., in the parieto-occipital cortex. The data here reported are in agreement with results of lesions to the medial posterior parietal cortex in both monkeys and humans, and with recent imaging data in humans, all of them indicating a functional coupling in the control of reaching and grasping by the medial parietofrontal circuit.
32
Filippini, Daniela <1978>. "Controllo dell'atto di prensione: coinvolgimento dell'area V6A nell'orientamento del polso." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1649/.
Full textAbstract:
Prehension in an act of coordinated reaching and grasping. The reaching component is concerned with bringing the hand to object to be grasped (transport phase); the grasping component refers to the shaping of the hand according to the object features (grasping phase) (Jeannerod, 1981). Reaching and grasping involve different muscles, proximal and distal muscles respectively, and are controlled by different parietofrontal circuit (Jeannerod et al., 1995): a medial circuit, involving area of superior parietal lobule and dorsal premotor area 6 (PMd) (dorsomedial visual stream), is mainly concerned with reaching; a lateral circuit, involving the inferior parietal lobule and ventral premotor area 6 (PMv) (dorsolateral visual stream), with grasping. Area V6A is located in the caudalmost part of the superior parietal lobule, so it belongs to the dorsomedial visual stream; it contains neurons sensitive to visual stimuli (Galletti et al. 1993, 1996, 1999) as well as cells sensitive to the direction of gaze (Galletti et al. 1995) and cells showing saccade-related activity (Nakamura et al. 1999; Kutz et al. 2003). Area V6A contains also arm-reaching neurons likely involved in the control of the direction of the arm during movements towards objects in the peripersonal space (Galletti et al. 1997; Fattori et al. 2001). The present results confirm this finding and demonstrate that during the reach-to-grasp the V6A neurons are also modulated by the orientation of the wrist.
Experiments were approved by the Bioethical Committee of the University of Bologna and were performed in accordance with National laws on care and use of laboratory animals and with the European Communities Council Directive of 24th November 1986 (86/609/EEC), recently revised by the Council of Europe guidelines (Appendix A of Convention ETS 123).
Experiments were performed in two awake Macaca fascicularis. Each monkey was trained to sit in a primate chair with the head restrained to perform reaching and grasping arm movements in complete darkness while gazing a small fixation point. The object to be grasped was a handle that could have different orientation. We recorded neural activity from 163 neurons of the anterior parietal sulcus; 116/163 (71%) neurons were modulated by the reach-to-grasp task during the execution of the forward movements toward the target (epoch MOV), 111/163 (68%) during the pulling of the handle (epoch HOLD) and 102/163 during the execution of backward movements (epoch M2) (t_test, p ≤ 0.05). About the 45% of the tested cells turned out to be sensitive to the orientation of the handle (one way ANOVA, p ≤ 0.05).
To study how the distal components of the movement, such as the hand preshaping during the reaching of the handle, could influence the neuronal discharge, we compared the neuronal activity during the reaching movements towards the same spatial location in reach-to-point and reach-to-grasp tasks. Both tasks required proximal arm movements; only the reach-to-grasp task required distal movements to orient the wrist and to shape the hand to grasp the handle. The 56% of V6A cells showed significant differences in the neural discharge (one way ANOVA, p ≤ 0.05) between the reach-to-point and the reach-to-grasp tasks during MOV, 54% during HOLD and 52% during M2. These data show that reaching and grasping are processed by the same population of neurons, providing evidence that the coordination of reaching and grasping takes place much earlier than previously thought, i.e., in the parieto-occipital cortex. The data here reported are in agreement with results of lesions to the medial posterior parietal cortex in both monkeys and humans, and with recent imaging data in humans, all of them indicating a functional coupling in the control of reaching and grasping by the medial parietofrontal circuit.
33
Bergami, Matteo <1981>. "Role of BDNF secretion and signaling in the activity-dependent refinement of synaptic connections." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1757/1/Matteo_Bergami_tesi.pdf.
Full textAbstract:
Neuronal networks exhibit diverse types of plasticity, including the activity-dependent regulation of synaptic functions and refinement of synaptic connections. In addition, continuous generation of new neurons in the “adult” brain (adult neurogenesis) represents a powerful form of structural plasticity establishing new connections and possibly implementing pre-existing neuronal circuits (Kempermann et al, 2000; Ming and Song, 2005). Neurotrophins, a family of neuronal growth factors, are crucially involved in the modulation of activity-dependent neuronal plasticity. The first evidence for the physiological importance of this role evolved from the observations that the local administration of neurotrophins has dramatic effects on the activity-dependent refinement of synaptic connections in the visual cortex (McAllister et al, 1999; Berardi et al, 2000; Thoenen, 1995). Moreover, the local availability of critical amounts of neurotrophins appears to be relevant for the ability of hippocampal neurons to undergo long-term potentiation (LTP) of the synaptic transmission (Lu, 2004; Aicardi et al, 2004). To achieve a comprehensive understanding of the modulatory role of neurotrophins in integrated neuronal systems, informations on the mechanisms about local neurotrophins synthesis and secretion as well as ditribution of their cognate receptors are of crucial importance.
In the first part of this doctoral thesis I have used electrophysiological approaches and real-time imaging tecniques to investigate additional features about the regulation of neurotrophins secretion, namely the capability of the neurotrophin brain-derived neurotrophic factor (BDNF) to undergo synaptic recycling. In cortical and hippocampal slices as well as in dissociated cell cultures, neuronal activity rapidly enhances the neuronal expression and secretion of BDNF which is subsequently taken up by neurons themselves but also by
perineuronal astrocytes, through the selective activation of BDNF receptors. Moreover, internalized BDNF becomes part of the releasable source of the neurotrophin, which is promptly recruited for activity-dependent recycling. Thus, we described for the first time that neurons and astrocytes contain an endocytic compartment competent for BDNF recycling, suggesting a specialized form of bidirectional communication between neurons and glia. The mechanism of BDNF recycling is reminiscent of that for neurotransmitters and identifies BDNF as a new modulator implicated in neuro- and glio-transmission.
In the second part of this doctoral thesis I addressed the role of BDNF signaling in adult hippocampal neurogenesis. I have generated a transgenic mouse model to specifically investigate the influence of BDNF signaling on the generation, differentiation, survival and connectivity of newborn neurons into the adult hippocampal network. I demonstrated that the survival of newborn neurons critically depends on the activation of the BDNF receptor TrkB. The TrkB-dependent decision regarding life or death in these newborn neurons takes place right at the transition point of their morphological and functional maturation Before newborn neurons start to die, they exhibit a drastic reduction in dendritic complexity and spine density compared to wild-type newborn neurons, indicating that this receptor is required for the connectivity of newborn neurons. Both the failure to become integrated and subsequent dying lead to impaired LTP. Finally, mice lacking a functional TrkB in the restricted population of newborn neurons show behavioral deficits, namely increased anxiety-like behavior. These data suggest that the integration and establishment of proper connections by newly generated neurons into the pre-existing network are relevant features for regulating the emotional state of the animal.
34
Bergami, Matteo <1981>. "Role of BDNF secretion and signaling in the activity-dependent refinement of synaptic connections." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1757/.
Full textAbstract:
Neuronal networks exhibit diverse types of plasticity, including the activity-dependent regulation of synaptic functions and refinement of synaptic connections. In addition, continuous generation of new neurons in the “adult” brain (adult neurogenesis) represents a powerful form of structural plasticity establishing new connections and possibly implementing pre-existing neuronal circuits (Kempermann et al, 2000; Ming and Song, 2005). Neurotrophins, a family of neuronal growth factors, are crucially involved in the modulation of activity-dependent neuronal plasticity. The first evidence for the physiological importance of this role evolved from the observations that the local administration of neurotrophins has dramatic effects on the activity-dependent refinement of synaptic connections in the visual cortex (McAllister et al, 1999; Berardi et al, 2000; Thoenen, 1995). Moreover, the local availability of critical amounts of neurotrophins appears to be relevant for the ability of hippocampal neurons to undergo long-term potentiation (LTP) of the synaptic transmission (Lu, 2004; Aicardi et al, 2004). To achieve a comprehensive understanding of the modulatory role of neurotrophins in integrated neuronal systems, informations on the mechanisms about local neurotrophins synthesis and secretion as well as ditribution of their cognate receptors are of crucial importance.
In the first part of this doctoral thesis I have used electrophysiological approaches and real-time imaging tecniques to investigate additional features about the regulation of neurotrophins secretion, namely the capability of the neurotrophin brain-derived neurotrophic factor (BDNF) to undergo synaptic recycling. In cortical and hippocampal slices as well as in dissociated cell cultures, neuronal activity rapidly enhances the neuronal expression and secretion of BDNF which is subsequently taken up by neurons themselves but also by
perineuronal astrocytes, through the selective activation of BDNF receptors. Moreover, internalized BDNF becomes part of the releasable source of the neurotrophin, which is promptly recruited for activity-dependent recycling. Thus, we described for the first time that neurons and astrocytes contain an endocytic compartment competent for BDNF recycling, suggesting a specialized form of bidirectional communication between neurons and glia. The mechanism of BDNF recycling is reminiscent of that for neurotransmitters and identifies BDNF as a new modulator implicated in neuro- and glio-transmission.
In the second part of this doctoral thesis I addressed the role of BDNF signaling in adult hippocampal neurogenesis. I have generated a transgenic mouse model to specifically investigate the influence of BDNF signaling on the generation, differentiation, survival and connectivity of newborn neurons into the adult hippocampal network. I demonstrated that the survival of newborn neurons critically depends on the activation of the BDNF receptor TrkB. The TrkB-dependent decision regarding life or death in these newborn neurons takes place right at the transition point of their morphological and functional maturation Before newborn neurons start to die, they exhibit a drastic reduction in dendritic complexity and spine density compared to wild-type newborn neurons, indicating that this receptor is required for the connectivity of newborn neurons. Both the failure to become integrated and subsequent dying lead to impaired LTP. Finally, mice lacking a functional TrkB in the restricted population of newborn neurons show behavioral deficits, namely increased anxiety-like behavior. These data suggest that the integration and establishment of proper connections by newly generated neurons into the pre-existing network are relevant features for regulating the emotional state of the animal.
35
Martelli, Davide <1976>. "Influenza dell'Omeostasi Idrico-Elettrolitica sul Ciclo Veglia-Sonno." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1816/1/Martelli_Davide_tesi.pdf.
Full textAbstract:
During the wake sleep (W-S) cycle in mammals, the alternation of the different states, wake, NREM sleep (NREMS) and REM sleep (REMS), is associated not only with electroencephalographic or behavioural changes, but also with modifications in the physiological regulations of the organism. The most evident change is the existence of a suspension of the somatic and autonomic thermoregulatory responses during REMS. Since thermoregulation is prevalently controlled by the Preoptic Area-Anterior Hypothalamus (PO-AH), its suspension during REM sleep has been taken as a sign of an impairment of the hypothalamic integrative activity that could explain the modifications in physiological regulation observed in this sleep stage.
The recent finding from our laboratory that the secretion of the antidiuretic hormone arginine-vasopressin (AVP) in response to a central osmotic stimulation is quantitatively the same throughout the different stages of the W-S cycle, has shown that hypothalamic osmoregulation is not suspended during REMS.
In order to clarify the extent of the hypothalamic involvement in the regulation of the W-S cycle, we have studied the effects of three days of water deprivation and of two days of recovery during which animals were allowed a free access to water, on the architecture of the W-S cycle. The condition of water deprivation represents a severe challenge involving neuroendocrine and autonomic hypothalamic regulations.
In contradiction with thermoregulatory studies, in which it has been clearly demonstrated that a thermal challenge selectively reduces REMS occurrence, the results of this study show that REMS occurrence is mildly reduced only in the third day of water deprivation. The most striking effects produced by water deprivation appear to concern NREMS, which shows a selective and significant reduction in its slow EEG activity (delta-power) but not in its duration. The recovery period is mainly characterized by a disruption of the normal circadian rhythm of REMS occurrence and by a rebound of the delta power in NREMS.
Thus, an autonomic challenge different from those related to thermoregulation and an endocrine challenge as the continuous secretion of AVP show to exert different effects on the stages of the wake-sleep cycle. Also, this study demonstrates that the impairment of the hypothalamic integrative activity thought to characterize the occurrence of REMS only involves thermoregulatory structures.
36
Martelli, Davide <1976>. "Influenza dell'Omeostasi Idrico-Elettrolitica sul Ciclo Veglia-Sonno." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/1816/.
Full textAbstract:
During the wake sleep (W-S) cycle in mammals, the alternation of the different states, wake, NREM sleep (NREMS) and REM sleep (REMS), is associated not only with electroencephalographic or behavioural changes, but also with modifications in the physiological regulations of the organism. The most evident change is the existence of a suspension of the somatic and autonomic thermoregulatory responses during REMS. Since thermoregulation is prevalently controlled by the Preoptic Area-Anterior Hypothalamus (PO-AH), its suspension during REM sleep has been taken as a sign of an impairment of the hypothalamic integrative activity that could explain the modifications in physiological regulation observed in this sleep stage.
The recent finding from our laboratory that the secretion of the antidiuretic hormone arginine-vasopressin (AVP) in response to a central osmotic stimulation is quantitatively the same throughout the different stages of the W-S cycle, has shown that hypothalamic osmoregulation is not suspended during REMS.
In order to clarify the extent of the hypothalamic involvement in the regulation of the W-S cycle, we have studied the effects of three days of water deprivation and of two days of recovery during which animals were allowed a free access to water, on the architecture of the W-S cycle. The condition of water deprivation represents a severe challenge involving neuroendocrine and autonomic hypothalamic regulations.
In contradiction with thermoregulatory studies, in which it has been clearly demonstrated that a thermal challenge selectively reduces REMS occurrence, the results of this study show that REMS occurrence is mildly reduced only in the third day of water deprivation. The most striking effects produced by water deprivation appear to concern NREMS, which shows a selective and significant reduction in its slow EEG activity (delta-power) but not in its duration. The recovery period is mainly characterized by a disruption of the normal circadian rhythm of REMS occurrence and by a rebound of the delta power in NREMS.
Thus, an autonomic challenge different from those related to thermoregulation and an endocrine challenge as the continuous secretion of AVP show to exert different effects on the stages of the wake-sleep cycle. Also, this study demonstrates that the impairment of the hypothalamic integrative activity thought to characterize the occurrence of REMS only involves thermoregulatory structures.
37
Tradori, Iosto <1980>. "Differenze emodinamiche dopo test da sforzo rettangolari di diversa intensità e durata." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/2071/1/tradori_iosto_tesi.pdf.
Full textAbstract:
La risposta emodinamica all'esercizio dinamico è stata oggetto di numerosi studi scientifici. Poca attenzione è stata invece rivolta agli aggiustamenti cardiovascolari che si verificano quando si interrompe uno sforzo dinamico. Al cessare dell' esercizio, la frequenza cardiaca e la contrattilità miocardica subiscono un decremento repentino e vengono rilasciati in quantità i prodotti finali del
metabolismo muscolare, come lattato, ioni idrogeno, adenosina, sostanze in grado di indurre vasodilatazione nei gruppi muscolari precedentemente attivati determinando una riduzione del precarico, post-carico cardiaco, contrattilità miocardica e una dilatazione delle arteriole periferiche, così da mantenere le resistenze vascolari periferiche a un basso livello. Inoltre, si verificano
alterazioni della concentrazione ematica di elettroliti, diminuzione delle catecolamine circolanti e si verifica un ipertono vagale : tutti questi fenomeni possono avere un effetto significativo sullo stato emodinamico. In questo studio si voleva valutare in che misura l’eventuale effetto ipotensivo dovuto all’esercizio fosse legato all’intensità del carico lavorativo applicato ed alla sua durata. Il
campione esaminato comprendeva 20 soggetti maschi attivi. I soggetti venivano sottoposti a quattro test in giornate diverse. La prova da sforzo preliminare consisteva in una prova da sforzo triangolare massimale eseguita al cicloergometro con un protocollo incrementale di 30 Watt al
minuto. Il test si articolava in una prima fase della durata di 3 minuti nei quali venivano registrati i dati basali, in una seconda fase della durata di tre minuti in cui il soggetto compiva un riscaldamento al cicloergometro, che precedeva l’inizio dello sforzo, ad un carico di 20 W. Al termine della prova venivano calcolati il massimo carico lavorativo raggiunto (Wmax) ed il valore di soglia anaerobica (SA). Dopo la prova da sforzo preliminare il soggetto effettuava 3 esercizi rettangolari di diversa intensità in maniera randomizzata così strutturati: test 70% SA; test 130% SA, 130% Wmax : prove da sforzo rettangolari ad un carico lavorativo pari alla percentuale
indicatain relazione ai valori di SA e Wmax ottenuti nella prova da sforzo preliminare. Tali test duravano dieci minuti o fino all'esaurimento del soggetto. Le prova erano precedute da tre minuti di riposo e da tre minuti di riscaldamento. Il recupero aveva una durata di 30 minuti. La PA veniva misurata ogni 5 minuti durante lo sforzo, ogni minuto nei primi 5 minuti di recupero e successivamente ogni 5 minuti fino alla conclusione del recupero. Dai risultati emerge come l'effetto ipotensivo sia stato più marcato nel recupero dall'intensità di carico lavorativo meno elevata, cioè dopo il test 70%SA. C'è da considerare che la più bassa intensità di sforzo permetteva di praticare un esercizio significativamente più lungo rispetto ai test 130%SA e 130%Wmax. È quindi verosimile che anche la durata dell'esercizio e non solo la sua intensità abbia avuto un ruolo fondamentale nel determinare l'ipotensione nel recupero evidenziata in questo studio. L’effetto ipotensivo più evidente si è manifestato nelle prove a più bassa intensità ma con carico lavorativo totale più elevato. I dati supportano la tendenza a considerare non tanto l’intensità e la durata dell’esercizio in modo isolato, quanto piuttosto il carico lavorativo totale
(intensità x durata). L'effetto ipotensivo registrato nello studio è da ascriversi soprattutto ad una persistente vasodilatazione susseguente allo sforzo. Infatti, nel recupero dal test 70%SA, le RVP si mantenevano basse rispetto ai valori di riposo. Tale dato potrebbe avere un grande valore clinico nella prescrizione dell'attività fisica più idonea nei soggetti ipertesi,che potrebbero beneficiare di un eventuale effetto ipotensivo successivo all'attività praticata. Pertanto in futuro bisognerà estendere lo studio ai soggetti ipertesi. La conferma di tale risultato in questi soggetti permetterebbe di scegliere correttamente l'intensità e la durata del carico lavorativo, in modo da calibrare lo sforzo al grado di patologia del soggetto.
38
Tradori, Iosto <1980>. "Differenze emodinamiche dopo test da sforzo rettangolari di diversa intensità e durata." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2009. http://amsdottorato.unibo.it/2071/.
Full textAbstract:
La risposta emodinamica all'esercizio dinamico è stata oggetto di numerosi studi scientifici. Poca attenzione è stata invece rivolta agli aggiustamenti cardiovascolari che si verificano quando si interrompe uno sforzo dinamico. Al cessare dell' esercizio, la frequenza cardiaca e la contrattilità miocardica subiscono un decremento repentino e vengono rilasciati in quantità i prodotti finali del
metabolismo muscolare, come lattato, ioni idrogeno, adenosina, sostanze in grado di indurre vasodilatazione nei gruppi muscolari precedentemente attivati determinando una riduzione del precarico, post-carico cardiaco, contrattilità miocardica e una dilatazione delle arteriole periferiche, così da mantenere le resistenze vascolari periferiche a un basso livello. Inoltre, si verificano
alterazioni della concentrazione ematica di elettroliti, diminuzione delle catecolamine circolanti e si verifica un ipertono vagale : tutti questi fenomeni possono avere un effetto significativo sullo stato emodinamico. In questo studio si voleva valutare in che misura l’eventuale effetto ipotensivo dovuto all’esercizio fosse legato all’intensità del carico lavorativo applicato ed alla sua durata. Il
campione esaminato comprendeva 20 soggetti maschi attivi. I soggetti venivano sottoposti a quattro test in giornate diverse. La prova da sforzo preliminare consisteva in una prova da sforzo triangolare massimale eseguita al cicloergometro con un protocollo incrementale di 30 Watt al
minuto. Il test si articolava in una prima fase della durata di 3 minuti nei quali venivano registrati i dati basali, in una seconda fase della durata di tre minuti in cui il soggetto compiva un riscaldamento al cicloergometro, che precedeva l’inizio dello sforzo, ad un carico di 20 W. Al termine della prova venivano calcolati il massimo carico lavorativo raggiunto (Wmax) ed il valore di soglia anaerobica (SA). Dopo la prova da sforzo preliminare il soggetto effettuava 3 esercizi rettangolari di diversa intensità in maniera randomizzata così strutturati: test 70% SA; test 130% SA, 130% Wmax : prove da sforzo rettangolari ad un carico lavorativo pari alla percentuale
indicatain relazione ai valori di SA e Wmax ottenuti nella prova da sforzo preliminare. Tali test duravano dieci minuti o fino all'esaurimento del soggetto. Le prova erano precedute da tre minuti di riposo e da tre minuti di riscaldamento. Il recupero aveva una durata di 30 minuti. La PA veniva misurata ogni 5 minuti durante lo sforzo, ogni minuto nei primi 5 minuti di recupero e successivamente ogni 5 minuti fino alla conclusione del recupero. Dai risultati emerge come l'effetto ipotensivo sia stato più marcato nel recupero dall'intensità di carico lavorativo meno elevata, cioè dopo il test 70%SA. C'è da considerare che la più bassa intensità di sforzo permetteva di praticare un esercizio significativamente più lungo rispetto ai test 130%SA e 130%Wmax. È quindi verosimile che anche la durata dell'esercizio e non solo la sua intensità abbia avuto un ruolo fondamentale nel determinare l'ipotensione nel recupero evidenziata in questo studio. L’effetto ipotensivo più evidente si è manifestato nelle prove a più bassa intensità ma con carico lavorativo totale più elevato. I dati supportano la tendenza a considerare non tanto l’intensità e la durata dell’esercizio in modo isolato, quanto piuttosto il carico lavorativo totale
(intensità x durata). L'effetto ipotensivo registrato nello studio è da ascriversi soprattutto ad una persistente vasodilatazione susseguente allo sforzo. Infatti, nel recupero dal test 70%SA, le RVP si mantenevano basse rispetto ai valori di riposo. Tale dato potrebbe avere un grande valore clinico nella prescrizione dell'attività fisica più idonea nei soggetti ipertesi,che potrebbero beneficiare di un eventuale effetto ipotensivo successivo all'attività praticata. Pertanto in futuro bisognerà estendere lo studio ai soggetti ipertesi. La conferma di tale risultato in questi soggetti permetterebbe di scegliere correttamente l'intensità e la durata del carico lavorativo, in modo da calibrare lo sforzo al grado di patologia del soggetto.
39
Gambi, Naimj <1980>. "Experimental Studies on Electromagnetic Fields Effects on Biological Targets: Simulation and Dosimetry." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/2472/1/Gambi_Naimj_Tesi.pdf.
Full text
40
Gambi, Naimj <1980>. "Experimental Studies on Electromagnetic Fields Effects on Biological Targets: Simulation and Dosimetry." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/2472/.
Full text
41
Paterini, Paola <1973>. "Infiammazione e cancro: l'interazione COX-2/CA-IX promuove il potenziale invasivo e la sopravvivenza in ipossia delle cellule del cancro colon-rettale." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/2579/1/paterini_paola_tesi.pdf.
Full textAbstract:
Cyclooxygenase-2/Carbonic anhydrase-IX up-regulation promotes invasive potential and hypoxia survival in colorectal cancer cells
Purpose: Cyclooxygenase-2 (COX-2) is a major mediator of inflammation, playing a pivotal role in colorectal carcinogenesis. Hypoxia is an universal hallmark of solid tumour in vivo. This investigation was prompted by the observation that in colorectal cancer cells the expression of COX-2 protein is positively correlated with that of the hypoxia survival gene Carbonic Anhydrase-IX (CA-IX).
Experimental Design: Since COX-2 gene expression and activity is increased in hypoxia, and that CA-IX is expressed also in normoxia in colorectal cancer cells, we tested the hypothesis that COX-2 activity in normoxia, as well as in hypoxia may be functionally linked to that of CA-IX gene. We investigated the role of COX-2 and CA-IX in colorectal cancer cell lines. In this regard, we performed RNA interference to knockdown COX-2 gene in vitro and immunohistochemistry to evaluate the protein expression of COX-2 and CA-IX in human colon cancer tissue specimens ex vivo.
Results: We found that COX-2, by PGE2 production, controls CA-IX gene expression in an ERK dependent manner. In line with this finding, we also showed that the COX-2 inhibition by a specific short harpin COX-2 RNA (shCOX-2) or by a specific drug (SC-236), down-regulated CA-IX expression in colon cancer cells. We then exposed colon cancer cells to hypoxia stimuli and found that COX-2/CA-IX interplay promoted hypoxia survival. Moreover, we also report that COX-2/CA-IX interplay triggers Matrix Metalloproteinase 2/9 (MMP-2/9) activation and enhances the invasiveness of colorectal cancer cells. Thus given our above observations, we found that CA-IX and COX-2 protein expressions correlate with more aggressive stage colorectal cancer tissues ex vivo.
Conclusions: Taken together these data indicate that COX-2/CA-IX interplay promotes an aggressive phenotype (hypoxia survival and invasiveness) which can be modulated in vitro by COX-2 selective inhibition and which may play a role in determining the biological aggressiveness of colorectal tumours. Moreover, in vitro and ex vivo data also suggest that the signatures of inflammation (COX-2) and hypoxia (CA-IX) may be difficult to be disentangled in colon cancer, being both responsible for the up-regulation of the same pathways.
42
Paterini, Paola <1973>. "Infiammazione e cancro: l'interazione COX-2/CA-IX promuove il potenziale invasivo e la sopravvivenza in ipossia delle cellule del cancro colon-rettale." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/2579/.
Full textAbstract:
Cyclooxygenase-2/Carbonic anhydrase-IX up-regulation promotes invasive potential and hypoxia survival in colorectal cancer cells
Purpose: Cyclooxygenase-2 (COX-2) is a major mediator of inflammation, playing a pivotal role in colorectal carcinogenesis. Hypoxia is an universal hallmark of solid tumour in vivo. This investigation was prompted by the observation that in colorectal cancer cells the expression of COX-2 protein is positively correlated with that of the hypoxia survival gene Carbonic Anhydrase-IX (CA-IX).
Experimental Design: Since COX-2 gene expression and activity is increased in hypoxia, and that CA-IX is expressed also in normoxia in colorectal cancer cells, we tested the hypothesis that COX-2 activity in normoxia, as well as in hypoxia may be functionally linked to that of CA-IX gene. We investigated the role of COX-2 and CA-IX in colorectal cancer cell lines. In this regard, we performed RNA interference to knockdown COX-2 gene in vitro and immunohistochemistry to evaluate the protein expression of COX-2 and CA-IX in human colon cancer tissue specimens ex vivo.
Results: We found that COX-2, by PGE2 production, controls CA-IX gene expression in an ERK dependent manner. In line with this finding, we also showed that the COX-2 inhibition by a specific short harpin COX-2 RNA (shCOX-2) or by a specific drug (SC-236), down-regulated CA-IX expression in colon cancer cells. We then exposed colon cancer cells to hypoxia stimuli and found that COX-2/CA-IX interplay promoted hypoxia survival. Moreover, we also report that COX-2/CA-IX interplay triggers Matrix Metalloproteinase 2/9 (MMP-2/9) activation and enhances the invasiveness of colorectal cancer cells. Thus given our above observations, we found that CA-IX and COX-2 protein expressions correlate with more aggressive stage colorectal cancer tissues ex vivo.
Conclusions: Taken together these data indicate that COX-2/CA-IX interplay promotes an aggressive phenotype (hypoxia survival and invasiveness) which can be modulated in vitro by COX-2 selective inhibition and which may play a role in determining the biological aggressiveness of colorectal tumours. Moreover, in vitro and ex vivo data also suggest that the signatures of inflammation (COX-2) and hypoxia (CA-IX) may be difficult to be disentangled in colon cancer, being both responsible for the up-regulation of the same pathways.
43
Eleuteri, Simona Carmen <1979>. "Neuroprotective strategies against neurodegeneration in cellular model systems." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/2831/1/ELEUTERI_SIMONA-tesi.pdf.
Full textAbstract:
In the present study we analyzed new neuroprotective therapeutical strategies in PD (Parkinson’s disease) and AD (Alzheimer’s disease). Current therapeutic strategies for treating PD and AD offer mainly transient symptomatic relief but it is still impossible to block the loss of neuron and then the progression of PD and AD. There is considerable consensus that the increased production and/or aggregation of α- synuclein (α-syn) and β-amyloid peptide (Aβ), plays a central role in the pathogenesis of PD, related synucleinopathies and AD. Therefore, we identified antiamyloidogenic compounds and we tested their effect as neuroprotective drug-like molecules against α-syn and β-amyloid cytotoxicity in PC12. Herein, we show that two nitro-catechol compounds (entacapone and tolcapone) and 5 cathecol-containing compounds (dopamine, pyrogallol, gallic acid, caffeic acid and quercetin) with antioxidant and anti-inflammatory properties, are potent inhibitors of α-syn and β-amyloid oligomerization and fibrillization. Subsequently, we show that the inhibition of α-syn
and β-amyloid oligomerization and fibrillization is correlated with the neuroprotection of these compounds against the α-syn and β-amyloid-induced cytotoxicity in PC12. Finally, we focused on the study of the neuroprotective role of microglia and on the
possibility that the neuroprotection properties of these cells could be use as therapeutical strategy in PD and AD. Here, we have used an in vitro model to
demonstrate neuroprotection of a 48 h-microglial conditioned medium (MCM) towards cerebellar granule neurons (CGNs) challenged with the neurotoxin 6-hydroxydopamine (6-OHDA), which induces a Parkinson-like neurodegeneration,
with Aβ42, which induces a Alzheimer-like neurodegeneration, and glutamate, involved in the major neurodegenerative diseases. We show that MCM nearly completely protects CGNs from 6-OHDA neurotoxicity, partially from glutamate excitotoxicity but not from Aβ42 toxin.
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Eleuteri, Simona Carmen <1979>. "Neuroprotective strategies against neurodegeneration in cellular model systems." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/2831/.
Full textAbstract:
In the present study we analyzed new neuroprotective therapeutical strategies in PD (Parkinson’s disease) and AD (Alzheimer’s disease). Current therapeutic strategies for treating PD and AD offer mainly transient symptomatic relief but it is still impossible to block the loss of neuron and then the progression of PD and AD. There is considerable consensus that the increased production and/or aggregation of α- synuclein (α-syn) and β-amyloid peptide (Aβ), plays a central role in the pathogenesis of PD, related synucleinopathies and AD. Therefore, we identified antiamyloidogenic compounds and we tested their effect as neuroprotective drug-like molecules against α-syn and β-amyloid cytotoxicity in PC12. Herein, we show that two nitro-catechol compounds (entacapone and tolcapone) and 5 cathecol-containing compounds (dopamine, pyrogallol, gallic acid, caffeic acid and quercetin) with antioxidant and anti-inflammatory properties, are potent inhibitors of α-syn and β-amyloid oligomerization and fibrillization. Subsequently, we show that the inhibition of α-syn
and β-amyloid oligomerization and fibrillization is correlated with the neuroprotection of these compounds against the α-syn and β-amyloid-induced cytotoxicity in PC12. Finally, we focused on the study of the neuroprotective role of microglia and on the
possibility that the neuroprotection properties of these cells could be use as therapeutical strategy in PD and AD. Here, we have used an in vitro model to
demonstrate neuroprotection of a 48 h-microglial conditioned medium (MCM) towards cerebellar granule neurons (CGNs) challenged with the neurotoxin 6-hydroxydopamine (6-OHDA), which induces a Parkinson-like neurodegeneration,
with Aβ42, which induces a Alzheimer-like neurodegeneration, and glutamate, involved in the major neurodegenerative diseases. We show that MCM nearly completely protects CGNs from 6-OHDA neurotoxicity, partially from glutamate excitotoxicity but not from Aβ42 toxin.
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Piras, Alessandro <1980>. "Visual scanning in sports actions: comparison between soccer goalkeepers and judo fighters." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/3064/1/Piras_Alessandro_tesi.pdf.
Full textAbstract:
Visual search and oculomotor behaviour are believed to be very relevant for athlete performance, especially for sports requiring refined visuo-motor coordination skills. Modern coaches believe that a correct visuo-motor strategy may be part of advanced training programs.
In this thesis two experiments are reported in which gaze behaviour of expert and novice athletes were investigated while they were doing a real sport specific task. The experiments concern two different sports: judo and soccer. In each experiment, number of fixations, fixation locations and mean fixation duration (ms) were considered. An observational analysis was done at the end of the paper to see perceptual differences between near and far space.
Purpose: The aim of the judo study was to delineate differences in gaze behaviour characteristics between a population of athletes and one of non athletes. Aspects specifically investigated were: search rate, search order and viewing time across different conditions in a real-world task. The second study was aimed at identifying gaze behaviour in varsity soccer goalkeepers while facing a penalty kick executed with instep and inside foot. Then an attempt has been done to compare the gaze strategies of expert judoka and soccer goalkeepers in order to delineate possible differences related to the different conditions of reacting to events occurring in near (peripersonal) or far (extrapersonal) space.
Judo Methods: A sample of 9 judoka (black belt) and 11 near judoka (white belt) were studied. Eye movements were recorded at 500Hz using a video based eye tracker (EyeLink II). Each subject participated in 40 sessions for about 40 minutes. Gaze behaviour was considered as average number of locations fixated per trial, the average number of fixations per trial, and mean fixation duration.
Soccer Methods: Seven (n = 7) intermediate level male volunteered for the experiment. The kickers and goalkeepers, had at least varsity level soccer experience. The vision-in-action (VIA) system (Vickers 1996; Vickers 2007) was used to collect the coupled gaze and motor behaviours of the goalkeepers. This system integrated input from a mobile eye tracking system (Applied Sciences Laboratories) with an external video of the goalkeeper’s saving actions. The goalkeepers took 30 penalty kicks on a synthetic pitch in accordance with FIFA (2008) laws.
Judo Results: Results indicate that experts group differed significantly from near expert for fixations duration, and number of fixations per trial. The expert judokas used a less exhaustive search strategy involving fewer fixations of longer duration than their novice counterparts and focused on central regions of the body. The results showed that in defence and attack situation expert group did a greater number of transitions with respect to their novice counterpart.
Soccer Results: We found significant main effect for the number of locations fixated across outcome (goal/save) but not for foot contact (instep/inside). Participants spent more time fixating the areas in instep than inside kick and in goal than in save situation. Mean and standard error in search strategy as a result of foot contact and outcome indicate that the most gaze behaviour start and finish on ball interest areas.
Conclusions: Expert goalkeepers tend to spend more time in inside-save than instep-save penalty, differences that was opposite in scored penalty kick. Judo results show that differences in visual behaviour related to the level of expertise appear mainly when the test presentation is continuous, last for a relatively long period of time and present a high level of uncertainty with regard to the chronology and the nature of events. Expert judoist performers “anchor” the fovea on central regions of the scene (lapel and face) while using peripheral vision to monitor opponents’ limb movements. The differences between judo and soccer gaze strategies are discussed on the light of physiological and neuropsychological differences between near and far space perception.
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Piras, Alessandro <1980>. "Visual scanning in sports actions: comparison between soccer goalkeepers and judo fighters." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/3064/.
Full textAbstract:
Visual search and oculomotor behaviour are believed to be very relevant for athlete performance, especially for sports requiring refined visuo-motor coordination skills. Modern coaches believe that a correct visuo-motor strategy may be part of advanced training programs.
In this thesis two experiments are reported in which gaze behaviour of expert and novice athletes were investigated while they were doing a real sport specific task. The experiments concern two different sports: judo and soccer. In each experiment, number of fixations, fixation locations and mean fixation duration (ms) were considered. An observational analysis was done at the end of the paper to see perceptual differences between near and far space.
Purpose: The aim of the judo study was to delineate differences in gaze behaviour characteristics between a population of athletes and one of non athletes. Aspects specifically investigated were: search rate, search order and viewing time across different conditions in a real-world task. The second study was aimed at identifying gaze behaviour in varsity soccer goalkeepers while facing a penalty kick executed with instep and inside foot. Then an attempt has been done to compare the gaze strategies of expert judoka and soccer goalkeepers in order to delineate possible differences related to the different conditions of reacting to events occurring in near (peripersonal) or far (extrapersonal) space.
Judo Methods: A sample of 9 judoka (black belt) and 11 near judoka (white belt) were studied. Eye movements were recorded at 500Hz using a video based eye tracker (EyeLink II). Each subject participated in 40 sessions for about 40 minutes. Gaze behaviour was considered as average number of locations fixated per trial, the average number of fixations per trial, and mean fixation duration.
Soccer Methods: Seven (n = 7) intermediate level male volunteered for the experiment. The kickers and goalkeepers, had at least varsity level soccer experience. The vision-in-action (VIA) system (Vickers 1996; Vickers 2007) was used to collect the coupled gaze and motor behaviours of the goalkeepers. This system integrated input from a mobile eye tracking system (Applied Sciences Laboratories) with an external video of the goalkeeper’s saving actions. The goalkeepers took 30 penalty kicks on a synthetic pitch in accordance with FIFA (2008) laws.
Judo Results: Results indicate that experts group differed significantly from near expert for fixations duration, and number of fixations per trial. The expert judokas used a less exhaustive search strategy involving fewer fixations of longer duration than their novice counterparts and focused on central regions of the body. The results showed that in defence and attack situation expert group did a greater number of transitions with respect to their novice counterpart.
Soccer Results: We found significant main effect for the number of locations fixated across outcome (goal/save) but not for foot contact (instep/inside). Participants spent more time fixating the areas in instep than inside kick and in goal than in save situation. Mean and standard error in search strategy as a result of foot contact and outcome indicate that the most gaze behaviour start and finish on ball interest areas.
Conclusions: Expert goalkeepers tend to spend more time in inside-save than instep-save penalty, differences that was opposite in scored penalty kick. Judo results show that differences in visual behaviour related to the level of expertise appear mainly when the test presentation is continuous, last for a relatively long period of time and present a high level of uncertainty with regard to the chronology and the nature of events. Expert judoist performers “anchor” the fovea on central regions of the scene (lapel and face) while using peripheral vision to monitor opponents’ limb movements. The differences between judo and soccer gaze strategies are discussed on the light of physiological and neuropsychological differences between near and far space perception.
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Bosco, Annalisa <1980>. "Reaching to a target in the 3-D space." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/3133/1/Bosco_Annalisa_tesi.pdf.
Full textAbstract:
Reaching and grasping an object is an action that can be performed in light, under visual guidance, as well as in darkness, under proprioceptive control only. Area V6A is a visuomotor area involved in the control of reaching movements. V6A, besides neurons activated by the execution of reaching movements, shows passive somatosensory and visual responses. This suggests fro V6A a multimodal capability of integrating sensory and motor-related information, We wanted to know whether this integration occurrs in reaching movements and in the present study we tested whether the visual feedback influenced the reaching activity of V6A neurons. In order to better address this question, we wanted to interpret the neural data in the light of the kinematic of reaching performance.
We used an experimental paradigm that could examine V6A responses in two different visual backgrounds, light and dark. In these conditions, the monkey performed an istructed-delay reaching task moving the hand towards different target positions located in the peripersonal space. During the execution of reaching task, the visual feedback is processed in a variety of patterns of modulation, sometimes not expected. In fact, having already demonstrated in V6A reach-related discharges in absence of visual feedback, we expected two types of neural modulation: 1) the addition of light in the environment enhanced reach-related discharges recorded in the dark; 2) the light left the neural response unmodified. Unexpectedly, the results show a complex pattern of modulation that argues against a simple additive interaction between visual and motor-related signals.
48
Bosco, Annalisa <1980>. "Reaching to a target in the 3-D space." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/3133/.
Full textAbstract:
Reaching and grasping an object is an action that can be performed in light, under visual guidance, as well as in darkness, under proprioceptive control only. Area V6A is a visuomotor area involved in the control of reaching movements. V6A, besides neurons activated by the execution of reaching movements, shows passive somatosensory and visual responses. This suggests fro V6A a multimodal capability of integrating sensory and motor-related information, We wanted to know whether this integration occurrs in reaching movements and in the present study we tested whether the visual feedback influenced the reaching activity of V6A neurons. In order to better address this question, we wanted to interpret the neural data in the light of the kinematic of reaching performance.
We used an experimental paradigm that could examine V6A responses in two different visual backgrounds, light and dark. In these conditions, the monkey performed an istructed-delay reaching task moving the hand towards different target positions located in the peripersonal space. During the execution of reaching task, the visual feedback is processed in a variety of patterns of modulation, sometimes not expected. In fact, having already demonstrated in V6A reach-related discharges in absence of visual feedback, we expected two types of neural modulation: 1) the addition of light in the environment enhanced reach-related discharges recorded in the dark; 2) the light left the neural response unmodified. Unexpectedly, the results show a complex pattern of modulation that argues against a simple additive interaction between visual and motor-related signals.
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Bianchi, Patrizia <1979>. "Defective neurogenesis in the Ts65Dn mouse, a model for Down syndrome, can be restored by pharmacological treatments." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/3139/1/Bianchi_Patrizia_Tesi.pdf.
Full text
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Bianchi, Patrizia <1979>. "Defective neurogenesis in the Ts65Dn mouse, a model for Down syndrome, can be restored by pharmacological treatments." Doctoral thesis, Alma Mater Studiorum - Università di Bologna, 2010. http://amsdottorato.unibo.it/3139/.
Full text