Dissertations / Theses on the topic 'HDFC'
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Ozdarska, Katarzyna. "Synthèses d’inhibiteurs de HDAC et leurs tests biologiques (Cytotoxicité, HDAC inhibition)." Thesis, Reims, 2020. http://www.theses.fr/2020REIMS023.
Full textEpigenetics represents changes in gene expression without altering the nucleic sequence of DNA. One of the main mechanisms of regulation of gene expression is chromatin remodeling via histone acetyltransferases and histone deacetylases (HDAC), which may or may not allow gene transcription. An abnormal expression of HDACs is correlated with many diseases (alcohol dependence, inflammation as well as cardiovascular and neurodegenerative diseases, cancers...). It is essential to target the selectivity of one isoform among the 11 known zinc-dependent HDACs to avoid side effects. The aim of the research was to design and synthesize new compounds, verify their inhibitory activity against class I or II HDACs and their cytotoxicity on four cell lines: HaCaT, V79-4, SH-SY5Y and PC12. We focused on the pharmacomodulations of ZBG, the linker and the cap of known molecules such as MS-275 (selective for class I of HDACs), SAHA and TSA (spacer in C5 or C6) with a strong inhibitory activity towards HDACs, but not selective. We concentrated on the pharmacomodulations of known HDACI modifying the zinc binding domain (sulfonylhydrazide, catechol), the nature of the spacer (alkyl, aryl) and the surface recognition group (bis-aryl, adamantyl, indolopyridazinone). A library of 57 new compounds was designed in three series. None of them showed satisfactory inhibitory activity. The selected compounds did not show cytotoxic activity on neuronal cell lines. Based on this research, it is possible to create new compounds in the indolopyridazinone series in order to test them
Silva, Fernández Simón Yeco. "Photometric Redshifts in the HDFS." Tesis, Universidad de Chile, 2015. http://repositorio.uchile.cl/handle/2250/133104.
Full textSe presenta fotometría óptica en 11 bandas medias a partir de observaciones realizadas con el telescopio de 2.2m en LSO (WFI) sobre un campo de ~30'×30' deg extendido en el Hubble Deep Field-South (EHDF-S), el cual es uno de los campos que contiene información en multibandas como parte del Multiwavelength Survey by Yale-Chile (MUSYC). Este campo tiene una gran cantidad de datos públicos y datos auxiliares en bandas UV, óptico, infrarrojo cercano e infrarrojo lejano. Se determinaron aperturas óptimas para fotometría de alta precisión para diversas fuentes y brillos. Se proporcionan incertezas en magnitud a través de una técnica mejorada que considera correlaciones a mayor y menor escala en el ruido. Se incluyen datos auxiliares en el óptico a partir del catálogo de MUSYC en bandas UBVRIz ' hasta una magnitud total de R=25 (AB), además de datos en infrarrojo cercano JHK de dos campos de 10 '× 10' deg con profundidades de J~22.5, H~21.5 y K~21 (5σ; Vega). Se creó un catálogo fotométrico de ~62.000 galaxias detectadas en la imagen BVR de MUSYC. Se miden redshifts fotométricos mediante el código EAzY y se compara con ~500 fuentes identificadas espectroscópicamente con la finalidad de probar la precisión y desempeño de los filtros en bandas medias. Los redshifts fotométricos resultaron más confiables para R<24 cuando la muestra contiene ~12.000 galaxias, particularmente en 0.1 < z < 1.2, región de sampleo en el óptico de características como el quiebre de Balmer. La precisión de los redshifts fotométricos en Δz/(1+z) es de 0.029, lo cual es comparable a estudios recientes con un mejoramiento del 20%. Estos valores se degradan en calidad para galaxias más débiles o cuando se utilizan menos bandas. Como demostración de la calidad de los resultados, se derivan tipos espectrales de las fuentes, luego se construyen funciones de luminosidad para comparar con trabajos similares, y así confirmar la fuerte dependencia de las SEDs con la densidad numérica de fuentes. Se incorporan datos observacionales en radio en el HDFS del Australia Telescopio Hubble Deep Field-South para estudiar en detalle su población. Este proyecto realizó observaciones en cuatro longitudes de onda, 20, 11, 6 y 3 cm y alcanza una sensibilidad en rms alrededor de 10 μJy para cada longitud de onda. Utilizando una muestra de 227 fuentes en radio seleccionadas, se realiza una clasificación detallada de la población en AGNs (-loud de radio (9%) y -quiet (46%)), galaxias con formación estelar (SFG; 39%), y galaxias normales (6%), usando los redshifts fotométricos, información en multibanda, un template combinado quasares, índices espectrales, las SEDs derivadas y la dependencia redshift luminosidad. Se confirman los resultados recientes sobre la disribución de AGNs y SFGs. Asimismo las LFs muestran consistencia para las fuentes en radio para z~1.0. Los resultados obtenidos siguen la tendencia de los trabajos previos de los últimos 4 a 5 años en la distribución de las fuentes de radio, y sugiere nuevas metodologías en torno a la caracterizacón la población en radio.
Khan, Omar Ali. "HR23B, a biomarker for HDAC inhibitors." Thesis, University of Oxford, 2013. http://ora.ox.ac.uk/objects/uuid:9cd76c0b-e70e-43f7-a92d-a99f403a077e.
Full textPolášek, Jaromír. "Implementace protokolu HDLC v síťových simulátorech." Master's thesis, Vysoké učení technické v Brně. Fakulta elektrotechniky a komunikačních technologií, 2018. http://www.nusl.cz/ntk/nusl-377008.
Full textCareres, Gutierrez Franco Jesus. "Towards an S3-based, DataNode-lessimplementation of HDFS." Thesis, KTH, Skolan för elektroteknik och datavetenskap (EECS), 2020. http://urn.kb.se/resolve?urn=urn:nbn:se:kth:diva-291125.
Full textRelevansen av databehandling och analys idag kan inte överdrivas. Konvergensen av flera tekniska framsteg har främjat spridningen av system och infrastruk-tur som tillsammans stöder generering, överföring och lagring av nästan 15,000 exabyte digitala, analyserbara data. Hadoop Distributed File System (HDFS) är ett öppen källkodssystem som är utformat för att utnyttja lagringskapaciteten hos tusentals servrar och är filsystemkomponenten i ett helt ekosystem av verktyg för att omvandla och analysera massiva datamängder. HDFS används av organisationer i alla storlekar, men mindre är inte lika lämpade för att organiskt växa sina kluster för att tillgodose deras ständigt växande datamängder och behandlingsbehov. Detta beror på att större kluster är samtidigt med högre investeringar i servrar, större misslyckanden att återhämta sig från och behovet av att avsätta mer resurser i underhålls- och administrationsuppgifter. Detta utgör en potentiell begränsning på vägen för organisationer, och det kan till och med avskräcka en del från att våga sig helt in i datavärlden. Denna avhandling behandlar denna fråga genom att presentera en ny implementering av HopsFS, en redan förbättrad version av HDFS, som inte kräver några användarhanterade dataservrar. Istället förlitar sig det på S3, en ledande objektlagringstjänst, för alla dess användardata lagringsbehov. Vi jämförde prestandan för både S3-baserade och vanliga kluster och fann att sådan arkitektur inte bara är möjlig, utan också helt livskraftig när det gäller läs- och skrivgenomströmningar, i vissa fall till och med bättre än dess ursprungliga motsvarighet. Dessutom ger vår lösning förstklassig elasticitet, tillförlitlighet och tillgänglighet, samtidigt som den är anmärkningsvärt billigare.
Schreiner, Lindsay Marie. "HDAC Mediated Integration of NF-¿B Transcriptional Regulation." University of Toledo / OhioLINK, 2014. http://rave.ohiolink.edu/etdc/view?acc_num=toledo1404744801.
Full textAlqahtani, Abdulateef Alqarni. "Synthesis and Biological Evaluation of New HDAC Inhibitors." University of Toledo / OhioLINK, 2018. http://rave.ohiolink.edu/etdc/view?acc_num=toledo1525448898248748.
Full textSindi, Shaimaa Hesham. "Guanidine- Based HDAC-Inhibitors as Anti-Cancer Agents." University of Toledo / OhioLINK, 2019. http://rave.ohiolink.edu/etdc/view?acc_num=toledo1564676186975875.
Full textPerin, Stefano <1995>. "Sintesi di inibitori peptidici per interazione MEF2-HDAC." Master's Degree Thesis, Università Ca' Foscari Venezia, 2021. http://hdl.handle.net/10579/19004.
Full textSodji, Quaovi Hemeka. "Improving histone deacetylase inhibition therapy through isoform selectivity and targeted delivery." Diss., Georgia Institute of Technology, 2014. http://hdl.handle.net/1853/53445.
Full textDlamini, Samkeliso Mpendulo Dlamini. "Synthesis and Biological Evaluation of HDAC Inhibitors with 1-(1H-imidazol-2-yl)ethan-1-one Moiety as the Metal-Binding Group." University of Toledo / OhioLINK, 2017. http://rave.ohiolink.edu/etdc/view?acc_num=toledo1501770195684609.
Full textLee, Daniel T. (Daniel Tzonglin) 1974. "Configurable byte-wide HDLC controller supporting IP over SONET." Thesis, Massachusetts Institute of Technology, 1998. http://hdl.handle.net/1721.1/47577.
Full textKhandrika, Ananth Viswa Sai Kalyan. "ASHWHIN- Array Storage system on HadoopFS With HDF5 Interface." The Ohio State University, 2018. http://rave.ohiolink.edu/etdc/view?acc_num=osu1524063297966335.
Full textCaceres, Gutierrez Franco Jesus. "Towards an S3-based, DataNode-less implementation of HDFS." Thesis, KTH, Skolan för elektroteknik och datavetenskap (EECS), 2020. http://urn.kb.se/resolve?urn=urn:nbn:se:kth:diva-291125.
Full textRelevansen av databehandling och analys idag kan inte överdrivas. Konvergensen av flera tekniska framsteg har främjat spridningen av system och infrastruk-tur som tillsammans stöder generering, överföring och lagring av nästan 15,000 exabyte digitala, analyserbara data. Hadoop Distributed File System (HDFS) är ett öppen källkodssystem som är utformat för att utnyttja lagringskapaciteten hos tusentals servrar och är filsystemkomponenten i ett helt ekosystem av verktyg för att omvandla och analysera massiva datamängder. HDFS används av organisationer i alla storlekar, men mindre är inte lika lämpade för att organiskt växa sina kluster för att tillgodose deras ständigt växande datamängder och behandlingsbehov. Detta beror på att större kluster är samtidigt med högre investeringar i servrar, större misslyckanden att återhämta sig från och behovet av att avsätta mer resurser i underhålls- och administrationsuppgifter. Detta utgör en potentiell begränsning på vägen för organisationer, och det kan till och med avskräcka en del från att våga sig helt in i datavärlden. Denna avhandling behandlar denna fråga genom att presentera en ny implementering av HopsFS, en redan förbättrad version av HDFS, som inte kräver några användarhanterade dataservrar. Istället förlitar sig det på S3, en ledande objektlagringstjänst, för alla dess användardata lagringsbehov. Vi jämförde prestandan för både S3-baserade och vanliga kluster och fann att sådan arkitektur inte bara är möjlig, utan också helt livskraftig när det gäller läs- och skrivgenomströmningar, i vissa fall till och med bättre än dess ursprungliga motsvarighet. Dessutom ger vår lösning förstklassig elasticitet, tillförlitlighet och tillgänglighet, samtidigt som den är anmärkningsvärt billigare.
Stavropoulou, Alexandra Vassiliki. "Histone deacetylase (HDAC) inhibitors and FBXL20 in breast cancer." Thesis, Imperial College London, 2008. http://hdl.handle.net/10044/1/7389.
Full textLinares, Aurélien. "Histone désacétylases, signalisation œstrogénique et cancer du sein : établissement d’outils bioluminescents pour la détection d’inhibiteurs sélectifs de HDAC : expression et rôle de HDAC9 dans les lignées cellulaires de cancer du sein." Thesis, Montpellier 1, 2011. http://www.theses.fr/2011MON13504/document.
Full textThe estrogen receptor (ER) can modulate the gene expression with consequences in the cell proliferation, apoptosis. This modulation is possible by the recruitment of coactivator or corepressor complexes. The repression activity is in particular explained by the histones deacetylases (HDACs). This protein family is composed by eighteen members who have been classified in four groups. These HDACs are subdivided on structural and functional similarities. The class I isoforms (HDACs 1, 2, 3 and 8), class II (HDACs 4, 5, 6, 7, 9, 10) and class IV (HDAC11) are Zn-dependent enzymes, whereas class III HDACs (Sirtuins 1-7) are NAD+-dependent. Recent data from the laboratory have shown, at the mRNA level, there is an enormous expression differential of HDAC9 between breast cancer cell line ER positive and negative or OHT resistant cell line. During my thesis, I demonstrated that the regulations of the HDAC9 on the level of its expression as of its role in the various breast cancer cell lines were implicated in the estrogen signaling. This regulation takes place at the transcriptional level and in the ERet#945; activity.In addition, using broad spectrum HDAC inhibitors (HDIs) such as TSA (Tricostatin A), many studies have shown that these inhibitors had antiangiogenic activity. Thus, the design or the identification of selective and potent HDAC inhibitors as agents anti-tumoral and/or anti-metastatic can emerge in a novel opportunity used alone or in combination with the already existing agents for the treatment of cancers. In order to identify and characterize new HDIs, my thesis works consisted to establish bioluminescent cell lines for screening HDAC inhibitors. Different cell GAL4-VP16-HDACs chimeras' models were generated to determine the selectivity of HDIs for the different HDACs
Bonds, August. "Hash-based Eventual Consistency to Scale the HDFS Block Report." Thesis, KTH, Skolan för informations- och kommunikationsteknik (ICT), 2017. http://urn.kb.se/resolve?urn=urn:nbn:se:kth:diva-222363.
Full textDet distribuerade, hierarkiska filsystemet Apache HDFS arkitektur begränsar dess skalbarhet. All metadata lagras i minnet i ett av klustrets noder, och i praktiken begränsar detta ett HDFS-klusters storlek till ungefär 4000 noder. Större kluster tvingas partitionera filsystemet i isolerade delar, vilket förändrar beteendet vid operationer som korsar partitionens gränser (exempelvis fil-flytter blir ickeatomära kombinationer av kopiera och radera). I idealfallet kan organisationer sammanslå alla sina lagringslösningar i ett och samma filträd för att undvika sådana beteendeförändringar och därför minska administrationen, samt öka användningen av den hårdvara de väljer att behålla. HopsFS är en ny utgåva av Apache HDFS, utvecklad på KTH, som använder en minnesbaserad distribuerad databaslösning för att lagra metadata. Lösningen kan hantera en klusterstorlek på 10000 noder och har visat att det i princip kan stöda klusterstorlekar på upp till femton gånger Apache HDFS. Ett av de hinder som kvarstår för att HopsFS ska kunna nå dessa nivåer är en så-småningom-konsekvent algoritm för dataförlustskydd i Apache HDFS som kallas Block Report. Detta arbete föreslår en lösning för att öka skalbarheten i HDFS Block Report som använder sig av en hash-baserad så-småningom-konsekvent mekanism för att undvika dubbelt arbete. Simuleringar indikerar att den nya lösningen i genomsnitt kan minska trycket på databasen med en hel storleksordning, till en prestandakostnad om mindre än tio procent på filsystemets vanliga operationer, medan databasanvändningen i värsta-fallet är jämförbart med den gamla lösningen.
Kulkarni, Upendra M. "Performance analysis of HDLC protocol operating in asynchronous balanced mode." Thesis, Virginia Tech, 1988. http://hdl.handle.net/10919/45897.
Full textThe objective of this work is to analyze the performance of HDLC Balanced Class of
Procedures under saturated, full-duplex transmission on error prone links. This thesis
extends work done by Bux et al. [8] by considering errors on both the links. Satellite
links have long propogation delays compared to terrestrial links, and hence, have
longer error recovery times. For such links, errors in acknowledgements have considerable
impact on the throughput. In this analysis, the effect of errors in acknowledgements
is taken in to consideration. An analytical approach is used to derive
performance measures. The concept of "virtual transmission time" introduced by Bux
et al is redefined to accommodate the effect of errors in acknowledgements and
used in the analysis. Resulting throughput calculations show how various parameters,
(e.g. transmission rate, propagation delay, error rate and packet size), interact
and determine the performance.
Master of Science
Regna, Nicole Lynn. "Isoform-Selective HDAC Inhibition for the Treatment of Lupus Nephritis." Diss., Virginia Tech, 2014. http://hdl.handle.net/10919/49023.
Full textPh. D.
Manzo, Fabio. "Functional regulation of class II HDAC trough their catalytic inhibition." Université Louis Pasteur (Strasbourg) (1971-2008), 2008. http://www.theses.fr/2008STR13159.
Full textHuman HDACs comprise a family of 18 different members which are grouped into four classes. Class I (HDAC 1-3,8), class II (HDAC4-7,9,10 of which HDAC4, 5, 7 and 9 form a class II a subgroup due to a common structural organization, while HDAC6 is member of class IIb), class III, also referred to as sirtuins (SIRT1-7) and class IV (HDAC11). Classes I, II and IV HDACs share common features, as all their members are zinc-dependent and exhibit some sequence similarities, while class III HDACs are NAD+-dependent enzymes without homology the other HDACs(1). Pan-inhibitors like SAHA, which is currently in phase III clinical trials and has recently been approved for treatment of cutaneous T cell lymphoma, inhibit both classes I and II enzymes, while MS275 is a subclass I selective inhibitor, which blocks the activities of HDAC 1, 2 and much less efficiently HDAC 3. Also class II selective inhibitors have been generated, marking the onset of a dissection of the various activities of HDACs. Notably, while induction of TRAIL appears to be associated with inhibition of class I enzymes in cancerous systems, other cellular functions involve the action of class II HDACs, like the regulation of the differentiation, mainly the cardiac differentiation. In differentiation systems: C2C12 cells, F9 cells, 3T3L1 cells. We tested a new compound HDAC inhibitor, specific for HDAC class 2 in one leukemic model, U937 cells, and various differentiation systems, such as the C2C12 cells for muscle differentiation, the F9 cells for endodermal differentiation and 3t3l1 cells for adypocyte differentiation. Interestingly we found that in C2C12 cells the HDAC class 2 inhibitor blocked the catalytic action of the HDAC class 2, but stabilized the interaction between the transcriptional factor MEF2D and HDAC4. MEF2D is the main transcriptional factor, responsible for the terminal muscle differentiation, and its transcriptional activity inhibition consequently blocked the muscle differentiation. In a similar way in both the other two systems we evaluated the differentiation inhibition and we found that transcriptional activity of RAR and PPARγ, respectively essential for the differentiation of the two systems, was blocked either in vitro in the first case either in vivo in the second case. In the case of the PPARγ induced differentiation, the experiments were assayed in the 3T3L1 cells. The treatment of these cells with Troglitazone induced adypocyte differentiation, while the presence of the MC1568 blocked it completely. Analyzing the Pparg’s expression level for RT-PCR, we found that its level was highly decreased after treatment with the MC1568. Interestingly the treatment of a mouse stably expressing a PPRE-luc, PPAR responsive elements luciferase reporter, blocked the transcriptional activity of PPARγ, showing in this case that the compound was regulating both the nuclear receptor’s transcriptional activity and the transactivation. In tumour model: MCF7 cells In cancer systems, such as MCF7 cells we found that the HDAC class 2 inhibitor MC1568 was inducing HDAC4 sumoylation, that, as previously showed (2) increases the HDAC4 catalytic action. The transfection of a specific HDAC4 sumoylation mutant in F9 cells decreased the repressory power on a note RAR target gene, Collagen IV. We were able to demonstrate that the treatment with MC1568 was regulating the activity of two transcriptional factor, RAR alpha and NF-KB, on three target genes, IRF1, TNF and TRAIL. The HDAC4 sumoylation mediated by RANBP2 repressed transiently the expression of these target genes, that were up-regulated after the complete degradation of HDAC4. Acute promyelocitic leukemia (APL), NB4 cells The NB4 cells is a cellular system of acute promyelocitic leukemia (APL). This disease is characterized by the presence of a fusion protein, PMLRAR alpha, with a strong repressory activity, mediated by the enhanced recruitment of corepressory complexes. The patients are treated with the differentiation therapy with retinoic acid (ATRA). Even if it is quite efficient to treat it, it still remains the problem of resistances, recidives and toxicity, done by the longer treatments, that give the, as said, ATRA syndrome and teratogenicity. In these cells we found that the combination among ATRA and MC1568 seems synergic, inducing a caspase independent cell death, even if in presence of caspases activation. The ZVAD inhibitor (pan-inhibitor for all caspases) failed to block the death induced by the MC1568 and by the combination among the two compounds. Analyzing the activation of the caspases it seemed that the pathway activated was mainly mediated by caspase 8. At the same time we found a strong release of cytochrome C, demonstrating the involvement of the mitochondria in the death induced by these two compounds. The use of a specific inhibitor, the NAC inhibitor, was able to reduce the death mediated by ATRA and MC1568, showing that the pathway was mainly regulated by the NAC dependent way. At this time, we are arrived to select the pathway regulated by this compound. Knowing that an HDAC inhibitor like MS275, specific inhibitor for class 1 HDACs, induce in the same system a caspase-dependent cell death, mainly regulated by TRAIL3, our observation would suggest that the class 2 HDAC inhibition is specifically regulating a pathway that is mainly caspase-independent. This observation could be usefull for treatment therapy, not only ammeliorating the treatment with retinoids, but overcoming possible resistances mediated by mutations and alteration in receptor expression in tumoral cells. Conclusions In my work I have evaluated the effect of a class 2 HDAC inhibitor in several systems, differentiative and cancerous, highlighting its effects in transcriptional regulation and cell death
Nell’uomo gli enzimi de acetilanti gli istoni appartengono ad una famiglia di 18 membri che sono raggruppati in 4 classi. La classe I (HDAC1-3,8), classe II (HDAC4-7,9,10 di cui HDAC4, 5,7,9 formano un subgruppo dovuta ad una comune organizzazione strutturale, mentre HDAC6 è un membro della classe 2), classe III, denominata come sirtuine (SIRT1-7) e classe IV (HDAC11). Le HDAC appartenenti alle classi I, II, IV sono comunemente dipendenti dallo zinco, mentre le HDAC appartenenti alla classe III sono enzimi dipendenti dal NAD +(1). SAHA, un pan inibitore delle HDAC, inibisce entrambi le classi I e II. Attualmente è in phase III clinical trials ed è stato recentemente approvato per il trattamento del linfoma cutaneo delle cellule T. MS275, invece, è un inibitore selettivo per la subclasse I, bloccando preferenzialmente HDAC1,2. Recentemente sono stati sintetizzati anche inibitori selettivi per la classe II, rendendo possibile lo studio delle varie funzioni delle differenti classi delle HDAC. Come è noto, mentre l’induzione di TRAIL sembra essere associata con l’inibizione di enzimi classe I in sistemi cancerosi, le HDAC di classe II sembrano essere coinvolte in altra funzioni cellulari, come la regolazione del differenziamento, principalmente quello cardiaco. Inibitori delle HDAC in sistemi differenziativi: le cellule C2C12, le cellule F9 e le cellule 3T3L1. Abbiamo testato un nuovo composto inibitore HDAC, specifico per la classe 2 in un modello leucemico, le cellule U937, e vari sistemi differenziativi, come le cellule C2C12 per il differenziamento cardiaco, le cellule F9 per il differenziamento endodermico e le cellule 3T3L1 per il differenziamento adipocitario. Abbiamo scoperto che nelle cellule C2C12 l’inibitore HDAC classe 2 stabilizzò l’interazione tra il fattore trascrizionale MEF2D ed HDAC4, pur bloccando l’azione catalitica delle HDAC classe II. MEF2D è il principale fattore trascrizionale resposabile del differenziamento cardiaco terminale e l’inibizione della sua attività trascrizionale conseguentemente bloccò il differenziamento muscolare. Negli altri due sistemi, similmente, noi abbiamo riscontrato l’inibizione del differenziamento ed abbiamo trovato che l’attività trascrizionale di RAR e PPARγ, essenziali per il differenziamento dei relativi sistemi differenziativi, fu bloccata sia in vitro nel primo caso che anche in vivo nel secondo. Nel caso del sistema differenziativo indotto da PPARγ, gli esperimenti furono fatti nelle 3T3L1. Il trattamento di queste cellule con Troglitazione indusse il differenziamento adipocitario, mentre la presenza dell’MC1568 lo bloccò completamente. Analizzando il livello di espressione di PPARγ per RT-PCR, abbiamo ritrovato che il suo livello era altamente decrementato dopo trattamento con MC1568. Abbiamo notato inoltre che il trattamento di un topo transgenico esprimente stabilmente il PPRE-luc, reporter luciferasi degli elementi responsivi a PPAR, bloccò completamente l’attività trascrizionale di PPARγ, mostrando in questo caso che il composto regolava sia l’attività trascrizionale del nuclear receptor sia il suo livello di espressione. In modelli cancerosi: le cellule MCF7 In sistemi cancerosi, così come le cellule MCF7 abbiamo riscontrato che lo specifico inibitore delle HDAC di classe II induceva la sumoilazione di HDAC4, che, come previamente mostrato (2) incrementa l’azione catalitica di HDAC4. La trasfezione di un mutante di HDAC4 specifico per il sito di sumoilazione nelle cellule F9 decrementò il potere repressorio su un noto target di RAR, CollagenIV. Abbiamo dimostrato che il trattamento con MC1568 regolò l’attività di due fattori trascrizionali, quali RAR alpha ed NF-KB, su tre geni target, IFR1, TNF e TRAIL. La sumoilazione di HDAC4 mediata da RANBP2 represse in modo transiente l’espressione di questi geni target, che furono up-regolati dopo la completa degradazione di HDAC4. Leucemia promielocitica acuta (APL), NB4 cells Le cellule NB4 è un sistema cellulare di leucemia promielocitica acuta (APL). Questa malattia è caratterizzata dalla presenza di una proteina di fusione, PMLRAR alpha, con un forte attività repressoria. I pazienti sono attualmente curati con la terapia differenziativa con acido retinoico (ATRA). Anche se è un trattamento molto efficiente, vi sono ancora casi di recidività, resistenze e tossicità al trattamento, dovuto principalmente ai trattamenti prolungati, dando luogo alla cosiddetta ATRA sindrome e teratogenicità. In queste cellule abbiamo scoperto il sinergismo tra ATRA e MC1568. La combinazione delle due droghe ha indotto una morte caspasi-indipendente, anche se in presenza di attivazione delle caspasi. L’inibitore ZVAD, infatti, fallì a bloccare la morte indotta dall’MC1568 e dalla combinazione tra i due composti. Analizzando l’attivazione delle caspasi, abbiamo riscontrato che il pathway maggiormente attivato è quello della caspasi 8. Allo stesso tempo abbiamo ritrovato un forte rilascio del citocromo C, dimostrando il coinvolgimento del mitocondrio nella morte indotta da questi due composti. L’uso di un inibitore specifico dei reattivi dell’ossigeno, N-acetyl-cisteina, ridusse significativamente la morte indotta, definendo il ruolo chiave dei ROS. Sapendo che un inibitore delle HDAC quale MS275, un inibitore specifico delle HDAC di classe 1, inducesse nello stesso sistema una morte caspasi dipendente, principalmente regolata da TRAIL3, la nostra osservazione suggerirebbe che l’inibizione specifica delle HDAC di classe II regola specificamente un pathway caspasi-indipendente, utile per migliorare il trattamento con retinoidi, ma soprattutto per curare quei pazienti con resistenze dovute a mutazioni o alterazione nella espressione del recettore in cellule tumorali. In Conclusione Nel mio lavoro ho studiato l’effetto di un inibitore specifico delle HDAC di classe II in svariati sistemi, differenziativi e cancerosi, concentrandomi sugli effetti nella regolazione trascrizionale e la morte cellulare
Lehmann, Annika [Verfasser]. "Rolle der Histondeacetylase (HDAC) in humanen soliden Tumoren / Annika Lehmann." Berlin : Medizinische Fakultät Charité - Universitätsmedizin Berlin, 2009. http://d-nb.info/1023704358/34.
Full textTuttle, Camilla Susannah Laura. "The expression of HAT and HDAC enzymes in asthma airways." Thesis, Queensland University of Technology, 2013. https://eprints.qut.edu.au/62873/1/Camilla_Tuttle_Thesis.pdf.
Full textRoy, Jean-Sébastien. "HDAC-independent transcriptional repression by RBPI is modulated by SUMO modification." Thesis, McGill University, 2003. http://digitool.Library.McGill.CA:80/R/?func=dbin-jump-full&object_id=80869.
Full textHesping, Eva M. "New inhibitors and tools to advance HDAC drug discovery for malaria." Thesis, Griffith University, 2021. http://hdl.handle.net/10072/403646.
Full textThesis (PhD Doctorate)
Doctor of Philosophy (PhD)
School of Environment and Sc
Science, Environment, Engineering and Technology
Full Text
pinazza, marica. "HDAC INHIBITORS TARGET TRANSCRIPTION FACTORS DEREGULATED IN T-ACUTE LYMPHOBLASTIC LEUKAEMIA." Doctoral thesis, Università degli studi di Padova, 2014. http://hdl.handle.net/11577/3423668.
Full textLe Istone Deacetilasi (HDACs) sono enzimi coinvolti nel rimodellamento della cromatina. Negli ultimi anni è emerso come l’inibizione delle HDACs potrebbe essere utilizzata come strategia per ripristinare l’alterata regolazione epigenetica che si riscontra nei tumori. Infatti, gli inibitori delle HDAC (HDACi) inducono apoptosi, arresto del ciclo cellulare e differenziamento delle cellule tumorali, ma i meccanismi molecolari alla base di questi fenomeni rimangono poco chiari. La leucemia linfoblastica acuta a cellule T (T-ALL) è un tumore pediatrico caratterizzato dall’espansione clonale di progenitori linfoidi. Nonostante la maggioranza dei pazienti pediatrici affetti da T-ALL siano curati in modo efficace utilizzando gli attuali protocolli terapeutici, circa un quarto dei pazienti manifesta resistenza alla terapia o presenta ricadute e dunque emerge la necessità di nuovi approcci terapeutici. In questo studio abbiamo analizzato gli effetti degli HDACi nei confronti di sette fattori di trascrizione implicati nella patogenesi della T-ALL (NOTCH1, NOTCH3, c-MYB, TAL1, TLX1, TLX3 and LMO2) utilizzando sia linee cellulari stabilizzate, sia modelli murini di T-ALL precedentemente sviluppati nel nostro laboratorio a partire da cellule di pazienti. In particolare, ci siamo concentrati su fattori trascrizionali che identificano specifici sottogruppi di T-ALL (TAL/LMO, TLX1 e TLX3) e abbiamo incluso nell’analisi due membri della famiglia dei recettori Notch (NOTCH1 and NOTCH3) e c-MYB in virtù del loro ruolo oncogenico in questa patologia. Le analisi in vitro hanno evidenziato diversi meccanismi di regolazione dei vari fattori da parte degli HDACi. TAL1 e c-MYB risultano regolati a livello trascrizionale, NOTCH1 e NOTCH3 presentano una regolazione post-traduzionale e, nel caso di TLX 1 e TLX3, è presente una regolazione diretta della loro capacità trascrizionale. Gli effetti a livello di proteina si legano all’induzione di apoptosi e all’inibizione della proliferazione sia nelle linee cellulari, sia nelle cellule derivate da paziente e risultano essere parzialmente dovute alla down-modulazione di NOTCH1 e NOTCH3. In seguito siamo andati ad indagare la risposta in vivo di un HDACi in xenografts di T-ALL appartenenti a specifici sottogruppi genetici. E’ interessante notare che il trattamento ha avuto il maggiore risultato nelle PD-TALL8 (TLX1) e nelle PD-TALL16 (TLX3) rispetto alle PD-TALL12 e le PD-TALL9 (entrambe TAL/LMO). Infatti, il trattamento con HDACi negli xenografts di tipo TLX determina una riduzione dell’infiltrazione da parte delle cellule leucemiche nella milza e nel midollo mentre gli effetti ottenuti negli xenografts TAL/LMO risultano modesti o addirittura nulli. In conclusione, i dati ottenuti identificano i pazienti di T-ALL appartenenti ai sottogruppi TLX1 e TLX3 come potenziali candidati per il trattamento a scopo terapeutico con HDACi.
Fritah, Sabrina. "Implications des histones deacetylases de I et II dans la réponse au stress." Université Joseph Fourier (Grenoble), 2008. http://www.theses.fr/2008GRE10270.
Full textLn response to environmental stress (heat shock, hypoxia, heavy metals exposure), cells have developed rapid and transitory mechanisms to protect themselves from the stress-induced damages. This stress response is characterized by the activation of HSF1 (Heat Shock Factor1), a key factor involved in the induction of the HSP (Heat Shock Proteins) encoded genes. Ln contrast toheat shock genes induction, most of the genome is repressed du ring stress. If the mechanisms involved in the activation of HSP genes have been investigated in details, less is known about the global repression of the genome. We started to investigate the epigenetic mechanisms that underline this genome repression and identify the molecular basis of this phenomenon. By molecular and in situ approaches, we showed that HDACs (Histone Deacetylases) are new regulators of stress response. Heat shock induces major epigenetic changes, specially a global deacetylation of core histones. We showed that class 1 HDAC, HDACl and HDAC2 mediates the heat-induced deacetylation. This event is regulated by HSF1, probably through its interaction with HDACl and HDAC2. Ln the cytoplasm, HDACS are also able to regulate stress response. Indeed, upon proteotoxic stress for example, proteasome inhibition, we showed that HDAC6 play a critical role in initiating the stress response. It mediates the dissociation of HSFl from its repressor complex and HDAC6 has an impact in HSP induction in response to stress. Ln conclusion, we identify HDACs as new important factors of stress response. Thanks to this work, we have linked two classes of proteins that are targeted by anti-cancer therapy: HSPs and HDACs
Leteve, Mathieu. "EPIADDICT - Synthèses de nouveaux inhibiteurs des histones désacétylases et leur intérêt dans un modèle préclinique d’addiction à l’alcool." Thesis, Reims, 2016. http://www.theses.fr/2016REIMS026/document.
Full textThe imbalance HAT/HDAC would influence the development of cancers and alcohol or cocaine addiction. HDAC inhibition allows increase of both acetylation rate and gene expression. Today, there are many structurally diverse potent, but non-specific HDAC inhibitors displaying important side-effects. HDAC inhibitors such as sodium butyrate or MS-275 have been shown to alter the alcohol dependence in the rat. MS-275 inhibits mainly class I of HDAC and in line with these observations we are interested in more selective class I inhibitors such as Largazole thiol and RedFK228. Our purpose is to synthesize new cyclodepsipeptides analogues in order to obtain selective class I inhibitor. HDAC class I is a Zn-dependent enzyme and our target molecules have sulfonylhydrazide function as efficient Zinc binding group (ZBG). Additional pharmacomodulations concern the incorporation of different heterocycles (oxazole, thiazole, pyridine) and varying linker lengths (n = 2, 3). Inhibitions of these compounds have been tested on HDAC1, HDAC3 and HDAC6. A compound has specificity for HDAC3 and another has specificity for HDAC1. Tests on rats "binger" suggest that HDAC1 is involved in this model of consumption and not HDAC3
Wegener, Dennis. "Entwicklung eines HTS-geeigneten Enzymtests für Histondeacetylasen zur Entwicklung von HDAC-Inhibitoren." [S.l.] : [s.n.], 2003. http://deposit.ddb.de/cgi-bin/dokserv?idn=972620621.
Full textDi, Fruscia Paolo. "The design, synthesis and biological evaluation of novel small-molecule HDAC inhibitors." Thesis, Imperial College London, 2012. http://hdl.handle.net/10044/1/39126.
Full textHorton, Kyle L. "Synthesis and characterization of biodegradable poly(vinyl esters) with HDAC inhibitory activity." Thesis, Wayne State University, 2013. http://pqdtopen.proquest.com/#viewpdf?dispub=1537532.
Full textHDAC inhibitors are known to have anti-inflammatory properties. HDAC inhibitors are used in combination with Oct4 to generate induced pluripotent stem cells. I hypothesized that polyesters based on simple aliphatic HDAC inhibitors like valproic acid (VPA) and phenylbutyric acid (PBA) can serve as alternatives to existing polyester biomaterials with improved anti-inflammatory properties and as scaffolds for generation of iPSCs when used in combination with layer-by-layer thin films delivering reprogramming transcription factors. Vinyl ester of phenylbutyric acid (VEPA) and vinyl ester of valproic acid (VEVA) were synthesized from their carboxylic acid precursors using an iridium complex catalyst at yields as high as 97% and 73%, respectively. Amorphous poly(VEPA) and poly(VEVA) polymers were prepared by free radical solution polymerization and characterized for molecular weight and glass transition temperature. Poly(VEPA) and poly(VEVA) microparticles of 20-40 um diameter were prepared by an emulsion-solvent evaporation method and examined under scanning electron microscopy (SEM). Their hydrolytic degradation was studied by dry weight loss and HDAC inhibitor release via high performance liquid chromatography (HPLC) in the presence of varied pH and lipase-containing buffers. No significant degradation occurred within 5 days, and an MTT assay conducted on HeLa cells in the presence of these microparticles confirmed an absence of cytotoxicity. Poly(VEPA) and poly(VEVA) microparticles were not found to be a suitable biomaterial for hypothesized applications in light of their poor degradation characteristics in vitro.
Santhanagopalan, Vignesh. "A Metadata Based Approach For Supporting Subsetting Queries Over Parallel HDF5 Datasets." The Ohio State University, 2011. http://rave.ohiolink.edu/etdc/view?acc_num=osu1314713754.
Full textMusatoiu, Mihai. "An approach to choosing the right distributed file system : Microsoft DFS vs. Hadoop DFS." Thesis, Blekinge Tekniska Högskola, Institutionen för programvaruteknik, 2015. http://urn.kb.se/resolve?urn=urn:nbn:se:bth-844.
Full textHuang, Rui. "Roles of HDACs in chromatin remodelling and response to chemotherapy in cancer." Thesis, University of Edinburgh, 2014. http://hdl.handle.net/1842/9626.
Full textKim, Wanhui. "Rôle de l'acétylation des histones dans le contrôle de l'expression du génome d'Arabidopsis thaliana." Paris 11, 2008. http://www.theses.fr/2008PA112156.
Full textHistone acetylation appears as a central switch for interconversion between permissive and repressive state of chromatin domains. Homeostasis of histone acetylation is made sure by histones acetyltransferases (HAT) and histones desacetylases (HDAC). But their role on chromatin and transcriptional/posttranscriptional regulation was not clear. The objective of my work was to study the role of histone acetylation in the control of gene expression in Arabidopsis thaliana. For this reason, HAT and HDAC mutants had been identified and characterized. First of all, we show that AtGCN5 interfere, in the pathway of miRNA, on transcriptional and posttranscriptional regulation of gene. It indicates that histone acetylation/desacetylation is an epigenetic mechanism involved in the regulation of miRNA production. Characterization of the mutants reveled that AtHDA9 mutation induces a phenotype of early flowering in short days. This characteristics is associated with overexpression of activator genes in the pathway of flowering. AtHDA9 and AtSRT2 mutation affect also DNA méthylation of pericentromeric sequence repeat 180 bp and retroelement AtSN1. Our results reveal the different role of individual HAT and HDAC in the control of genome expression of Arabidopsis
Zagni, Chiara. "Progettazione e sintesi di nuovi inibitori delle istone deacetilasi." Thesis, Università degli Studi di Catania, 2011. http://hdl.handle.net/10761/253.
Full textThe epigenetic control of gene expression is operated through post-translational modifications of chromatin such as acetylation and deacetylation. Two enzymes are responsable for these processes: HAT (histone acetyl transferase) and HDAC (histone deacetylase). HDAC is a group of enzymes involved in regulating gene expression, DNA repair and stress response. Acetylation plays an important role in trascription because it remodels chromatin structure enhancing access to DNA-binding factors. In general, increased levels of histone acetylation are associated with increased transcriptional activity, whereas decreased levels of acetylation are associated with repression of gene expression. In tumor cells abnormal gene expression is frequently observed. HDAC inhibitors have been shown to be potent inducers of growth arrest, differentiation, and apoptotic cell death both in vitro and in vivo transformed cells. To date there are seven distinct classes of HDAC inhibitors and all contain three key structural elements to their pharmacophore: a) a zinc-binding group which coordinates the zinc ion at the bottom of the long narrow active site cavity; b) a capping group which interacts both with the amino acids on the rim of the binding cavity and the protein surface; c) a linker domain whose role is to ensure the correct positioning of the two former groups and to in-teract with the lipophilic binding tunnel. Following our recent interest in the research of more potent HDAC inhibitors, we have projected and synthesized a new series of compounds containing four new zinc chelant moieties, i.e. formylhydrazonomethyl, 2-formylhydrazinocarbonyl, 2,2,2-trifluoro-N-methylideneacetamidic and N-(trifluoroacetyl)amidic, linked by an aromatic spacer to an aromatic sulfonamide, that is responsible of hydrophobic interaction with HDAC. Docking studies have shown that these new molecules fit very good in the HDAC enzymatic pocket with a best ï Gbind of â 7,9 kcal/mol that is 1 kcal/mol lower of the corresponding one for SAHA, a good HDAC.
Traore, Mohamed Dit Mady. "Synthèse et études de modélisation moléculaire dans l'optimisation de la sélectivité de nouveaux agents antiparasitaires inspirés de produits naturels." Thesis, Université Grenoble Alpes (ComUE), 2016. http://www.theses.fr/2016GREAV027/document.
Full textAculeatins and FR235222 are two families of natural products that are highly effective against apicomplexan parasites, responsible for malaria and toxoplasmosis. In the first part of this work, we developed a new reaction involving a “one pot” phenolic oxidation cascade sequence using a hypervalent iodine reagent in catalytic condition. This flexible synthetic strategy will increase accessibility to new aculeatin derivatives to achieve bioactive compounds. In the second part, we were interested in FR235222, an HDACi (histone deacetylase inhibitor) which targets the class I human HDAC and parasite T. gondii HDAC3 responsible for toxoplasmosis. HDACs are proteins that play an important role in the control of epigenetic mechanisms. In this study, a FR235222 fluorescent derivative was synthesized to confirm the FR235222 target in human cells through cellular localization studies. The synthesis and assessment of the activity of new HDACi analogues, combined with molecular modelisation studies, allowed to demonstrate for the first time that the keto-hydroxyl zinc binding group and the flexibility of the linker would be responsible for this selectivity on human class I HDACs. Finally, with these results in hand and the identification of structural differences between human and parasitic HDAC3, prediction studies (docking) have revealed structural determinants to design inhibitors selective for apicomplexan parasites HDACi
Sena, Elena. "The Transcription Factor Barhl2 Inhibits Wnt Canonical Signaling during Xenopus Embryogenesis." Thesis, Université Paris-Saclay (ComUE), 2018. http://www.theses.fr/2018SACLS090/document.
Full textEmbryonic development is a highly controlled process where different signaling pathways participate into the elaboration of an organism. One of the main signaling pathways is the Wnt canonical pathway. The long-lasting search to understand Wnt/β-catenin transduction cascade revealed that the net transcriptional read out of Wnt/β-catenin signaling is highly dependent on the cellular context. In X. laevis embryos Wnt/β-catenin signaling is the informative signal for the Spemann Organizer induction. However little is known on what limits Wnt activity in this territory and consequently the size of the Spemann Organizer. The results presented in this manuscript provide evidence that the evolutionarily conserved transcription factor Barhl2 limits the development of the Spemann organizer. In this territory Barhl2 inhibits Wnt activity via its interaction with the co-repressor Groucho and the transcription factor Tcf. It participates to the recruitment of the chromatin remodeling enzyme, Hdac1 that represses the expression of Spemann organizer genes. Using a Xenopus tropicalis Tcf reporter line we demonstrate that Barhl2 inhibitory effect on Groucho-Tcf activities is maintained during embryogenesis and plays a role in the confinement of neural progenitors in the brain. Together, our results provide a new and important mechanism for the control of Wnt transcriptional activity
Lockard, Michael T., R. Rajagopalan, and James A. Garling. "MINING IRIG-106 CHAPTER 10 AND HDF-5 DATA." International Foundation for Telemetering, 2006. http://hdl.handle.net/10150/604264.
Full textRapid access to ever-increasing amounts of test data is becoming a problem. The authors have developed a data-mining methodology solution approach to provide a solution to catalog test files, search metadata attributes to derive test data files of interest, and query test data measurements using a web-based engine to produce results in seconds. Generated graphs allow the user to visualize an overview of the entire test for a selected set of measurements, with areas highlighted where the query conditions were satisfied. The user can then zoom into areas of interest and export selected information.
Palma, Camila de Souza. "Avaliação de alterações proteômicas em diferentes modelos de indução da transição epitelial-mesenquimal (EMT) em células de adenocarcinoma de mama." Universidade de São Paulo, 2018. http://www.teses.usp.br/teses/disponiveis/17/17131/tde-01022019-102412/.
Full textTumor development is a process comprising several steps and consists in the progressive development of normal cells into a neoplastic state through various biochemical and phenotypic changes. Among the major marks of cancer are the capacity for tissue invasion and metastasis. Metastasis accounts for approximately 90% of cancer deaths. Thus, the most effective methods for improving cancer-related morbidity and mortality rates are early detection, prevention and treatment of metastasis. The EMT process, which occurs naturally during embryogenesis and tissue repair, is also involved in cancer progression and metastasis. EMT induces complex cellular and microenvironmental changes that result in the acquisition of a mesenchymal phenotype by epithelial cells, together with an increase in migratory and invasive cellular capacities. EMT can be induced by various extracellular factors, such as TGF?, EGF, HGF and PDGF. In addition, overexpression of some transcription factors such as SNAIL, SLUG, ZEB1 and TWIST1 is also capable of inducing EMT in vitro. In order to increase the knowledge of the mechanisms involved in the EMT process, we performed proteomic analysis in different models of EMT induction in the MCF7 breast adenocarcinoma cell line, which were the overexpression of SNAIL, treatment with the histone deacetylase inhibitor SAHA and treatment with the growth factor EGF. The detailed proteomic analysis by LC-MS/MS of the subcellular fractions of nucleus, cytoplasm and membrane of the overexpressing SNAIL cells generated a list of regulated proteins related to the EMT process and that were evaluated in the other models of induction. Among these, the HDAC1 protein, which had its levels decreased by SNAIL overexpression. Treatment of the MCF7 cell line with the histone deacetylase inhibitor SAHA showed a positive correlation with the increase of SNAIL levels, suggesting a cross-talk between both proteins. In addition, SAHA treatment induced cellular and protein alterations that also suggest the induction of the EMT process in MCF7 cells. Finally, the treatment with the growth factor EGF was also able to induce the EMT in MCF7 cells and showed involvement in the regulation of the cell cycle, changes in proteins in common with the other treatments and differential regulation of proteins among thesubcompartiments, indicating similarities between the processes and potential mechanisms of subcellular translocation. In conclusion, this study revealed target proteins related to EMT, opening possibilities to try to alter processes related to tumor progression and metastatic process.
Bernard, Julia M., Amber Seidel, Mary Oglesby, and Colleen Pagnan. "Mothers in HDFS Academic Life: When Your Professional Life and Real Life Intertwine." Digital Commons @ East Tennessee State University, 2018. https://dc.etsu.edu/etsu-works/5808.
Full textBridgeman, Stephanie Claire. "Epigenetics, cholesterol lowering and diabetes: a comparative study of statins and HDAC inhibitors." Thesis, Curtin University, 2022. http://hdl.handle.net/20.500.11937/88742.
Full textAnderson, Letícia. "Regulação epigenética da expressão gênica de Schistosoma mansoni induzida por inibidor de histona deacetilase." Universidade de São Paulo, 2016. http://www.teses.usp.br/teses/disponiveis/46/46131/tde-20092016-094835/.
Full textSchistosomiasis is a serious public health problem, with high mortality and morbidity in endemic countries, caused by trematode worms of the genus Schistosoma. Praziquantel is the only available drug for treatment of the disease; it is used extensively to treat populations in endemic areas, but does not prevent reinfection and is effective only in adult worms. Drugs studied in cancer as histone deacetylase inhibitors (iHDACs) modify the epigenetic status of the cell, triggering cell death, and it has been shown in Schistosoma mansoni that inhibition of HDACs increase histone acetylation, alter the phenotype of miracidia and cause death in schistosomules and adult worms. The present study investigated the effect of iHDAC Trichostatin A (TSA) on the regulation of gene transcription in schistosomules, detecting by means of microarray assays hundreds of differentially expressed genes related to DNA replication, metabolism and histone remodeling complexes. Inhibition of HDAC in adult worms led to an increase in histone acetylation marks H3K9ac, and H3K14ac H4K5ac related to transcriptional induction. With chromatin immunoprecipitation followed PCR (ChIP-qPCR) we detected an increased deposition of H3K9ac and H3K14ac at the promoter region of genes with increased or decreased expression, but the repressive mark H3K27me3 was not changed at all analyzed gene promoter regions. Additional analysis indicated a set of differentially expressed genes that encode histone reader proteins that are part of histone modifier complexes such as EED, which is able to identify the repression mark H3K27me3 and to regulate EZH2 activity, pointing to a new therapeutic target. The synergistic effect between iHDAC and one iEZH2 has been tested and found to cause an increase in schistosomules mortality. The SmEZH2 structure was modeled by homology and used for computational analyses, which suggested a high affinity binding of SmEZH2 with iEZH2, opening the opportunity for development of new specific drugs for treatment of schistosomiasis.
Al-Hamashi, Ayad Abed Ali Chiad A. "Design, Synthesis, and Biological Evaluation of Novel Histone Deacetylase Inhibitors as Anti-Cancer Agents." University of Toledo / OhioLINK, 2018. http://rave.ohiolink.edu/etdc/view?acc_num=toledo1525945712448479.
Full textPradeep, Aakash. "P2PHDFS: AN IMPLEMENTATION OF STATISTIC MULTIPLEXED COMPUTING ARCHITECTURE IN HADOOP FILE SYSTEM." Master's thesis, Temple University Libraries, 2012. http://cdm16002.contentdm.oclc.org/cdm/ref/collection/p245801coll10/id/214757.
Full textM.S.
The Peer to Peer Hadoop Distributed File System (P2PHDFS) is designed to store and process extremely large-scale data sets reliably. This is a first attempt implementation of the Statistic Multiplexed Computing Architecture concept proposed by Dr. Shi for the existing Hadoop File System (HDFS) to eliminate all single point failures. Unlike HDFS, in P2PHDFS every node is designed to be equal and behaves as a file system server as well as slave, which enable it to attain higher performance and higher reliability at the same time as the infrastructure up scales. Due to the data intensive nature, a full implementation of P2PHDFS must address CAP Theorem challenges. This MS project is only intended as the ground breaking point using only sequential replication at this time.
Temple University--Theses
Peiro, Sajjad Hooman, and Harirbaf Mahmoud Hakimzadeh. "Maintaining Strong Consistency Semantics in a Horizontally Scalable and Highly Available Implementation of HDFS." Thesis, KTH, Skolan för informations- och kommunikationsteknik (ICT), 2013. http://urn.kb.se/resolve?urn=urn:nbn:se:kth:diva-127464.
Full textServatius, Phil [Verfasser], and Uli [Akademischer Betreuer] Kazmaier. "Total synthesis of natural HDAC inhibitors and derivatives thereof / Phil Servatius ; Betreuer: Uli Kazmaier." Saarbrücken : Saarländische Universitäts- und Landesbibliothek, 2018. http://d-nb.info/1172288003/34.
Full textArndt, David L. "Role of HDAC inhibition and environmental condition in altering phases of amphetamine self-administration." Diss., Kansas State University, 2016. http://hdl.handle.net/2097/32694.
Full textPsychological Sciences
Mary E. Cain
Gene-environment interactions play a significant role in drug abuse and addiction. Epigenetics (the study of how environmental stimuli alter gene expression) has gained attention in recent years as a significant contributor to many behavioral phenotypes of drug addiction. The current study sought to determine if differential rearing conditions can alter a specific epigenetic mechanism, histone deacetylase (HDAC), and how HDAC inhibition can affect drug-taking and drug-seeking behaviors differently among enriched, isolated, or standard-housed rats. Ninety male Sprague-Dawley rats were reared for 30 days in enriched (EC), isolated (IC), or standard (SC) conditions prior to amphetamine (0.03, 0.05, 0.1 mg/kg/infusion, i.v.) self-administration, extinction, or reinstatement sessions. Trichostatin A (TsA; 0.3 mg/kg, i.v.), an HDAC inhibitor, was injected 30 min prior to drug-taking or drug-seeking sessions. Results indicated that EC rats self-administered less amphetamine (0.03 mg/kg/infusion) than IC rats. No significant effects of TsA administration were found on general self-administration for any of the three amphetamine doses. While enrichment facilitated the extinction of active lever pressing, there was also a mild facilitation of extinction in IC-TsA rats compared to IC-vehicle counterparts. Lastly, TsA administration decreased cue-, but not drug-induced reinstatement, with IC-TsA rats exhibiting significantly attenuated cue-induced reinstatement compared to IC-vehicle rats. These findings suggest that differential rearing can alter HDAC mechanisms that can change drug-seeking behaviors, particularly in rats reared in isolated conditions. While TsA-induced HDAC inhibition may be less protective against general amphetamine self-administration, it may decrease drug-seeking tendencies during relapse that are induced by the reintroduction of contextual environmental cues heavily associated with drug reward.
Perikala, V. "Understanding the relevance of epigenetic reprogramming for resistance to HDAC inhibitors in cancer cells." Thesis, University of Liverpool, 2016. http://livrepository.liverpool.ac.uk/3004805/.
Full textServatius, Phil Verfasser], and Uli [Akademischer Betreuer] [Kazmaier. "Total synthesis of natural HDAC inhibitors and derivatives thereof / Phil Servatius ; Betreuer: Uli Kazmaier." Saarbrücken : Saarländische Universitäts- und Landesbibliothek, 2018. http://nbn-resolving.de/urn:nbn:de:bsz:291-scidok-ds-275430.
Full textMatsubara, Hiroshi. "Involvement of ERK activation in human osteosarcoma cell resistance to the HDAC inhibitor FK228." Kyoto University, 2009. http://hdl.handle.net/2433/126457.
Full text