Literatura científica selecionada sobre o tema "Metabolism"
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Artigos de revistas sobre o assunto "Metabolism"
Anton-Păduraru, Dana-Teodora. "URGENŢE METABOLICE – PARTEA I". Romanian Journal of Pediatrics 64, n.º 1 (31 de março de 2015): 44–47. http://dx.doi.org/10.37897/rjp.2015.1.9.
Texto completo da fonteKordyum, E. L., e О. М. Nedukha. "Proposals for the ISS: «Starch» Experiment Structural-metabolic aspects of carbohydrate metabolism in microgravity". Kosmìčna nauka ì tehnologìâ 6, n.º 4 (30 de julho de 2000): 97. http://dx.doi.org/10.15407/knit2000.04.972.
Texto completo da fonteStrashok, L. A., O. V. Buznytska e О. М. Meshkova. "Indicators of lipid metabolism disorders in the blood serum of adolescents with metabolic syndrome". Ukrainian Biochemical Journal 92, n.º 6 (24 de dezembro de 2020): 137–42. http://dx.doi.org/10.15407/ubj92.06.137.
Texto completo da fonteŠnejdrlová, Michaela. "Metabolism and sex, sex and metabolism". Urologie pro praxi 18, n.º 1 (1 de março de 2017): 22–25. http://dx.doi.org/10.36290/uro.2017.006.
Texto completo da fonteLitvyak, V. S., e V. V. Litvyak. "Possible Explanation of Metabolism Process". Nutrition and Food Processing 5, n.º 1 (1 de fevereiro de 2022): 01–13. http://dx.doi.org/10.31579/2637-8914/073.
Texto completo da fonteWahyono, Sri, Sulistyoweni Widanarko, Setyo S. Moersidik e Surna T. Djajadiningrat. "METABOLISME PENGELOLAAN SAMPAH ORGANIK MELALUI TEKNOLOGI KOMPOSTING DI WILAYAH INTERNAL PERKOTAAN". Jurnal Teknologi Lingkungan 13, n.º 2 (13 de dezembro de 2016): 179. http://dx.doi.org/10.29122/jtl.v13i2.1417.
Texto completo da fontePospisilik, J. Andrew. "Metabolism shaping chromatin shaping metabolism". Cellular and Molecular Life Sciences 70, n.º 9 (9 de março de 2013): 1493–94. http://dx.doi.org/10.1007/s00018-013-1292-6.
Texto completo da fontePathak, Aishwarya. "EXPLORING METABOLISM: UNDERSTANDING THE FUNDAMENTAL PROCESSES". International Journal of Prevention Practice and Research 02, n.º 01 (2 de janeiro de 2022): 01–06. http://dx.doi.org/10.55640/medscience-abcd612.
Texto completo da fonteUmbu Henggu, Krisman, e Yopi Nurdiansyah. "Review dari Metabolisme Karbohidrat, Lipid, Protein, dan Asam Nukleat". QUIMICA: Jurnal Kimia Sains dan Terapan 3, n.º 2 (2 de agosto de 2022): 9–17. http://dx.doi.org/10.33059/jq.v3i2.5688.
Texto completo da fonteHao, Min, De Ji, Lin Li, Lianlin Su, Wei Gu, Liya Gu, Qiaohan Wang, Tulin Lu e Chunqin Mao. "Mechanism of Curcuma wenyujin Rhizoma on Acute Blood Stasis in Rats Based on a UPLC-Q/TOF-MS Metabolomics and Network Approach". Molecules 24, n.º 1 (27 de dezembro de 2018): 82. http://dx.doi.org/10.3390/molecules24010082.
Texto completo da fonteTeses / dissertações sobre o assunto "Metabolism"
Beard, Katherine F. M. "Investigating metabolite channelling in primary plant metabolism". Thesis, University of Oxford, 2013. http://ora.ox.ac.uk/objects/uuid:8172377f-5eca-4825-b6f1-5c10f02bede5.
Texto completo da fonteEichler, Paula. "Diminuição da proteína GLUT4 em tecido adiposo de ratos tratados com injeções subcutâneas de óleos de soja ou de girassol". Universidade de São Paulo, 2008. http://www.teses.usp.br/teses/disponiveis/42/42137/tde-16092008-115901/.
Texto completo da fonteWe treated rats for 7 days with subcutaneous soybean (SB) oil or sunflower (SF)oil injections. Insulin resistance was developed, with a decrease in GLUT4 quantity and translocation in adipose tissue in the rats treated with those oils, despite GLUT4 mRNA increase in muscle and adipose tissue. Sunflower treatment led to decrease in GLUT1mRNA in adipose tissue, where NF- kB mRNA was also decreased (other transcriptional factors did not change: PPARg, MEF2A e MF2D). Fatty acids were measured in the plasma, the liver (no changes), muscle (palmitoleic increased in SF, linolenic decreased in SB and SF and arachidonic increased in SB) and adipose tissue (palmitic and stearic increased and linoleico decreased in SB and SF, besides increasing in saturated/ unsaturated ratio.
Bojanowska, Magdalena. "Wpływ opóźniania terminu pierwszego unasieniania krów z zaburzeniami metabolizmu energetycznego na ich płodność". Rozprawa doktorska, Uniwersytet Technologiczno-Przyrodniczy w Bydgoszczy, 2018. http://dlibra.utp.edu.pl/Content/1229.
Texto completo da fonteThe aim of the research was to assess the effectiveness of the use of data from periodic control of dairy utility in the selection of cows with energy metabolism disturbances and the impact of their delay in the first insemination on the reproductive indicators of the herd
Valor, Ivars Teresa. "The effects of prescribed burning on the vigour of Mediterranean pine species". Doctoral thesis, Universitat Autònoma de Barcelona, 2018. http://hdl.handle.net/10803/664281.
Texto completo da fontePrescribed burning is the planned use of fire to meet clear management objectives under suitable environmental conditions. It is usually executed to reduce fire hazard, but also to manage range and conserve biodiversity. Prescribed burning applied under a forest canopy can reduce crown fire hazard; however, underburning might affect the primary and secondary metabolism of trees. Planning underburning to reduced fire hazard, while minimizing the negative effects and maximizing the positive effects on trees, requires understanding how specific components of the fire regime, such as fire intensity, severity and season, affect tree performance. The goal of this doctoral thesis is to understand the influence of prescribed burning regime factors and related fire impacts on the primary and secondary metabolisms of three pine species with contrasting fire tolerances: Pinus nigra ssp. salzmannii (Dunal) Franco, P. sylvestris L. and P. halepensis Mill., using a combination of dendrochronological, isotope and terpene quantification techniques. Post-burning growth variations depended on the time since burning, the pine species, tree resistance, fire severity and tree performance before burning. In the year of burning, growth was reduced in P. halepensis and unaffected in P. nigra and P. sylvestris. However, as time passed, growth increased in P. nigra, recovered in P. halepensis and decreased in P. sylvestris. P. nigra had a lower probability of dying than P. sylvestris. Burning season emerged as an important factor for explaining initial post-burning pine mortality, since for a certain level of crown injury the probability of a pine dying was higher in spring than in fall. In contrast, delayed pine mortality was higher in fall than in spring burns probably due to the longer combustion times recorded during the fall burns at the base of the trunk. A relevant release of tree competition increased growth through a positive effect on the latewood of P. nigra and P. sylvestris as stem injury decreased. Moreover, we showed that burning just after a dry year did not reduce the growth resilience of pines in comparison with unburned pines. In P. halepensis a relevant competition release, especially in pines with lower crown volume scorched, resulted in higher growth rates as time since burning increased. This growth response coincided with a dry year and was associated with higher stomatal conductance, suggesting that water availability was enhanced after burning. Burning also affected the secondary metabolism of pines, and specifically the amount and type of terpene production depending on the pine species and fire severity. Thus, as crown injury increased, needle terpene concentration 24h post-burning also augmented. However, a remarkable decrease occurred at one year post-burning. This reduction was more pronounced in pines benefited by the increase in resource availability after burning, suggesting that pines were allocating assimilates to growth rather than to defence. From a fuel management point of view, this thesis provides valuable information that can be used to better plan prescribed burning in Mediterranean Pinus forests, in terms of required fire intensity, severity and burning season, offering a new window of opportunity for the use of prescribed burning as a forest management tool.
Treitinger, Aricio. "Alterações metabólicas e do sistema de defesa antioxidante no plasma e em células mononucleares decorrentes da infecção pelo vírus da imunodeficiência humana". Universidade de São Paulo, 1996. http://www.teses.usp.br/teses/disponiveis/9/9136/tde-10032015-110940/.
Texto completo da fonteA total number of 101 individuals, including 26 controls and 75 patients classified according to the Walter Reed Army Institute (28 WR 1, 31 WR 2 and 16 WR 3/4) was studied. HIV infected individuals presented, during the early stages, a progressive reduction of body weigth, as well as urea, albumin, total cholesterol, HDL cholesterol and LDL cholesterol in blood serum. However, increased serum levels of total protein, globulin, IgG, IgA, α1 acid glycoprotein, haptoglobin, AST and LD were observed in HIV infected individuals during the evolution of infection. Decreased serum iron and a trend for increasing triglyceride was shown only for those individuals classified as WR 3/4. Transferrin was diminished only in the WR 2 group. A trend for enhancing serum ferritin following the progession of HIV infection was also observed. No alteration was observed on the levels of reactive \"C\" protein. Decreased EC-SOD activities were observed in HIV infected individuals as compared to controls, whereas in mononuclear cells the SOD activity was diminished only in WR 3/4 patients. HIV infection did not alter GSH-Px activity. A trend for decreasing α-tocopherol and ascorbate plasma levels was shown during the evolution of HIV infected patients, while no difference was observed for β-carotene levels in the studied groups. The above results suggest that haptoglobin, globulins and IgA can be used to assess the evolution of the HIV infection. Moreover, the decreased levels of the antioxidant defense system components observed in HIV infected patients may indicate that they are under an oxidative stress that could favor HIV replication.
Mc, Grail Fernández Kimberley Anne. "Targeting NRAS mutant melanomas through metabolic stress". Doctoral thesis, Universitat Autònoma de Barcelona, 2021. http://hdl.handle.net/10803/673108.
Texto completo da fonteLos genes BRAF y NRAS presentan una mayor incidencia mutacional en melanoma cutáneo. Alteraciones en estos genes resultan en la activación constitutiva de la vía de RAS-ERK1/2, lo que contribuye activamente al desarrollo y la progresión tumoral del melanoma. Aunque ambas mutaciones dan lugar a alteraciones de la misma vía de señalización, ha sido ampliamente descrito que los tumores que se generan de las mismas, constituyen dos entidades diferentes tanto a nivel molecular como desde el punto de vista clínico. Una cuestión relevante reside en el hecho de que mientras los melanomas mutados en BRAF disponen de terapias específicas dirigidas contra el oncogén, los melanomas que presentan mutaciones en NRAS carecen de tratamientos específicos. Como consecuencia, estos pacientes son tratados con tratamientos antitumorales más genéricos, que desembocan en tasas de respuesta mucho menores y en una elevada toxicidad. En este contexto, el desenmascaramiento de las diferencias moleculares existentes entre los tumores con mutaciones en BRAF y en NRAS es esencial para el establecimiento de nuevas estrategias terapéuticas dirigidas a pacientes que presentan mutaciones en NRAS. Resultados obtenidos previamente en nuestro grupo de investigación, sumados a los de otras investigaciones, han confirmado la presencia de diferentes patrones metabólicos sujetos a la regulación por BRAFV600E. Sin embargo, apenas existe evidencia sobre el papel de las mutaciones en NRAS en la regulación metabólica. El establecimiento de características metabólicas específicas de melanomas con mutaciones en NRAS podría contribuir al desarrollo de nuevos enfoques terapéuticos dirigidos contra este tipo de tumor. Durante el desarrollo de este estudio hemos investigado las implicaciones moleculares derivadas de la falta de glucosa en células de melanoma mutadas en NRASQ61 y BRAFV600E, con el fin de establecer si la presencia de características metabólicas dependientes de NRAS podría ser explotada para el desarrollo de nuevas terapias contra este tipo de tumor. En este estudio, hemos demostrado la presencia de patrones metabólicos bajo el control de NRASQ61. Las células que presentan mutaciones en NRASQ61 muestran una respuesta diferencial al estrés metabólico, en comparación con las células mutadas en BRAFV600E, que desemboca en la hiperactivación de la vía de RAS-ERK1/2 y en la sensibilización de estas células al inhibidor multi-quinasa Sorafenib. PFKFB2, PFKFB3 y PFK-1 son elementos clave en la regulación de este proceso. Adicionalmente, proponemos una nueva aproximación terapéutica para el tratamiento dirigido de los melanomas mutados en NRASQ61, basada en la combinación de 2-deoxi-D-glucosa (2DG) y Sorafenib. Tras los resultados obtenidos, podemos concluir que los tumores que presentan mutaciones en NRAS y BRAF son entidades diferentes a distintos niveles, no solo a nivel clínico y molecular, sino también a nivel metabólico, lo que implica la existencia de nuevas ventanas terapéuticas para el tratamiento de tumores que presentan mutaciones en NRAS.
BRAF and NRAS are the most commonly found mutated genes in cutaneous melanoma. Alterations in these genes result in the constitutive activation of the RAS-ERK1/2 pathway, contributing to tumor development and progression. Beside both genes are consecutive located in the same signaling cascade, BRAF and NRAS mutated tumors are considered two different entities at clinical and molecular levels, resulting in distinct signaling patterns and different biological behavior. Furthermore, while there is a first line of treatment using targeted therapy against BRAF mutant melanomas, NRAS mutant tumors remain without specific line of treatment, showing low response rates and high toxicity to the currently applied therapies. Thus, the understanding of the molecular differences between BRAF and NRAS mutant tumors is essential to improve therapeutic opportunities for the treatment of patients carrying NRAS mutations. Previous results in our group, together with additional investigations, have highlighted the presence of different metabolic settings subjected to BRAFV600E oncogene regulation. However, little is known about the role of NRAS mutations in metabolic rewiring. Deciphering metabolic settings in NRAS mutant melanomas could provide new avenues for the establishment of specific therapeutic approaches against these, until now, untargetable tumors. In this study, we have investigated the molecular implications of glucose starvation in NRASQ61 and BRAFV600E mutant cells in order to establish whether the presence of NRAS-dependent metabolic settings can be exploited for the development of targeted therapies against NRAS mutant melanomas. Overall, in this study we have demonstrated the presence of NRASQ61 oncogene-dependent metabolic settings. NRASQ61 mutant cells show a differential response to metabolic stress when compared to BRAFV600E mutant cells, which results in the hyperactivation of the RAS-ERK1/2 pathway and the sensitization to the multikinase inhibitor Sorafenib. PFKFB2, PFKFB3 and PFK-1 are key players in the regulation of this process. We also propose a novel approach for the specific targeting of NRASQ61 mutant melanomas based on the combination of 2-deoxy-D-glucose (2DG) and Sorafenib. We conclude that NRAS and BRAF mutant tumors are different entities at different levels, not only at molecular and clinical levels but also at metabolic level and this fact provides a new therapeutic window for the targeting of NRAS mutant tumors.
Universitat Autònoma de Barcelona. Programa de Doctorat en Bioquímica, Biologia Molecular i Biomedicina
Mota, Martorell Natàlia. "Oxidative stress homeostasis and longevity in mammals". Doctoral thesis, Universitat de Lleida, 2021. http://hdl.handle.net/10803/672775.
Texto completo da fonteLas especies más longevas han evolucionado disminuyendo la producción endógena de especies reactivas de oxígeno y proveyéndose de estructuras resistentes a la oxidación. Por lo tanto, aquellas especies que viven más disfrutan de mitocondrias metabólicamente más eficientes y estructuralmente más estables. De hecho, características fenotípicas de la longevidad incluyen la reducción del contenido del complejo I y de amino ácidos sulfurados. Por lo tanto, la activad de determinadas vías de señalización intracelular juegan un papel clave regulando la expresión de genes asociados a un fenotipo longevo. En este contexto, esta tesis pretende determinar i) la modulación de determinadas subunidades del complejo I asociada a la longevidad; ii) los cambios en el contenido de amino acido sulfurados y de sus intermediarios metabólicos en tejidos post-mitóticos y iii) plasma de especies más longevas; iv) la regulación del contenido de distintos elementos específicos del complejo 1 de mTOR en términos de longevidad; y v) la existencia de un perfil metabólico asociado a humanos de longevidad extrema. Los resultados obtenidos muestran la existencia de perfiles metabólicos asociados a la longevidad de las especies que, en algunos casos, son diferentes a aquellos perfiles asociados a la longevidad individual. Además, las especies más longevas han evolucionado disminuyendo el contenido de determinadas subunidades del complejo I que podrían ser responsables de la menor producción de especies reactivas de oxígeno. Por otra parte, existen factores genéticos que podrían determinar la actividad basal de mTOR, y que podrían, al menos en parte, explicar el fenotipo asociado a la longevidad. Por lo tanto, parece que lograr una mayor longevidad implica una adaptación metabólica y estructural.
Long-lived species have evolved by decreasing the rate of endogenous reactive oxygen species production and providing them of oxidation-resistant structures. Hence, species that live longer benefit from metabolically efficient and structurally stable mitochondria. In fact, phenotypic traits of longevity include reduced content of complex I and sulphur-containing amino acids. Then, the activity of selected intracellular signalling pathways plays a key role regulating the expression of genes associated to a longevity phenotype. In this context, this thesis aims to determine i) the modulation of specific complex I subunits associated to longevity; ii) the changes on sulphur amino acids content and its metabolic intermediates in post-mitotic tissues and ii) plasma from long-lived species; iv) the content regulation of the different mTOR complex 1 specific forming elements in terms of longevity; and v) the existence of a metabolic profile associated to human extreme longevity. The obtained results reveal the existence of metabolic profiles associated to species longevity that, in some cases, differ from those profile associated to individual longevity. Furthermore, longer lived species have evolved reducing the content of specific complex 1 subunits that might be responsible for the limited reactive oxygen species production. Otherwise, genetic factors that might determine the basal activity of mTORC1 exist, and that could, at least In part, explain the longevity associated phenotype. Thus, it seems that the achievement of an extended longevity implies a metabolic and structural adaptation.
Aarts, Michelle M. "Metabolism and immune effects of sulfamethoxazole and hydroxylamine metabolite". Thesis, National Library of Canada = Bibliothèque nationale du Canada, 1997. http://www.collectionscanada.ca/obj/s4/f2/dsk2/ftp04/mq21080.pdf.
Texto completo da fonteJorge, Letícia Galhardo. "Desempenho fotossintético, perfil e atividade do óleo essencial de Xylopia aromatica (Lam.) Mart. nas fases vegetativa e reprodutiva no cerrado paulista". Botucatu, 2020. http://hdl.handle.net/11449/192182.
Texto completo da fonteResumo: Espécies vegetais são capazes de produzir diversidade de substâncias, que desempenham funções importantes para sua sobrevivência e adaptação ao ecossistema. O metabolismo primário, é essencial para o crescimento, desenvolvimento, maturação e reprodução de qualquer espécie. O metabolismo especializado, dependente do primário, é responsável por originar o óleo essencial, que são misturas de metabólitos especializados voláteis, representados principalmente por monoterpenos e sesquiterpenos. Cada espécie vegetal produz um óleo essencial de composição característica específica, podendo ser influenciado por fatores bióticos e abióticos. A fenologia pode influenciar processos bioquímicos e rotas metabólicas capazes de modificar a formação de substâncias biologicamente ativas, alterando diretamente o conteúdo e a qualidade dos óleos essenciais. Sendo assim, o objetivo deste trabalho foi avaliar se as fases fenológicas, vegetativa e reprodutiva modificam o desempenho fotossintético e o perfil do óleo essencial de Xylopia aromatica (Lam.) Mart., influenciando sua atividade biológica na defesa antioxidante e ação antifúngica. As variáveis, fluorescência da clorofila a, trocas gasosas, carboidratos, atividade enzimática e peroxidação lipídica, potencial água, conteúdo relativo de água das folhas, extração, rendimento, caracterização química e atividade antifúngica do óleo essencial de Xylopia aromatica foram avaliadas em 24 plantas, 12 no estádio vegetativo e 12 no reprodutivo, coletadas... (Resumo completo, clicar acesso eletrônico abaixo)
Abstract: Research aimed at the knowledge of plant species allows the elaboration of projects that aim at the understanding of development, conservation of biodiversity and sustainable exploitation of natural resources. The primary metabolism, represented by photosynthesis and the specialized one, that synthesizes the essential oil, can be influenced by the environmental and phenological conditions, which can influence the chemical profile of the essential oil and the biological activity in the vegetal defense, including against fungi, bacteria and virus. Compounds from the specialized metabolism present biological activity and potential for the production of bactericides and fungicides. Therefore, it is necessary to know the stage of development of plant species in which the substances of interest, with economic potential, are more concentrated, thus orienting, if appropriate, the collection period, aiming at the conservation and sustainable use. There are scientific studies that reveal biological activity of essential oils, as observed for the genus Xylopia, but none of them relates the primary and specialized metabolism to the stage of development in which the species is found. In this way, the objective of this research was to evaluate if the phenological, vegetative and reproductive phases of Xylopia aromatica (Lam.) Mart. modify the photosynthetic performance and the profile of the essential oil, which may influence its biological activity in the antioxidant defense and antifunga... (Complete abstract click electronic access below)
Mestre
Vidal, Alabró Anna. "Estudi de l’activació de la glucocinasa (GKA456V) en fetge perivenós". Doctoral thesis, Universitat de Barcelona, 2011. http://hdl.handle.net/10803/32022.
Texto completo da fonteSynthetic glucokinase activators have been used in the context of type 2 diabetes therapy, mainly for their insulin secretagogue activity. However, the impact of these drugs on liver GK has not been studied in vivo. Since GK activators and activating GK mutations confer identical kinetic properties to GK, we hypothesize that hepatic overexpression of a mutated form of GK, GKA456V, described in a patient with Persistent Hyperinsulinemic Hypoglycemia of Infancy (PHHI), shall mimic the liver-specific effects of GK-activating drugs. GKA456V was overexpressed in the liver of streptozotocin diabetic mice and also in healthy mice. Metabolite profiling in serum and liver extracts, together with key components of glucose and lipid homeostasis, were analyzed and compared to GK wild-type transfected animals. Cell compartmentalization of mutant and wild-type GK was also examined in vivo. In the type 1 diabetic mice, GKA456V overexpression markedly reduced blood glucose in the absence of dislipidemia, in contrast to wild-type GK-overexpressing mice. Enhanced glucose utilization did not correlate with glycogen synthesis or lactate production. PEPCK mRNA was not affected, whereas the mRNA for the catalytic subunit of glucose-6-phosphatase was upregulated ~4-fold in the liver of GKA456V treated animals. Moreover, GKA456V was not translocated to the nucleus after a short fast, confirming that this activating mutation disrupted GKRP regulation. In healthy mice, the overexpression of hepatic GK resulted in insulin resistance. Otherwise, GKA456V overepxressing animals were not insulin resistant. They showed increased mRNA and protein content of the catalytic subunit of glucose-6-phosphatase in the liver, and an idnuction of catabolism in their adipose tissue. Our results validate liver specific GK activation as a strategy for diabetes therapy and provide new insights into the complex GK regulatory network.
Livros sobre o assunto "Metabolism"
American, Chemical Society Symposium "Biosynthesis and Metabolismof Secondary-Metabolite Natural Products" (1991 Atlanta Ga ). Secondary-metabolite biosynthesis and metabolism. New York: London, 1992.
Encontre o texto completo da fontePetroski, Richard J., e Susan P. McCormick, eds. Secondary-Metabolite Biosynthesis and Metabolism. Boston, MA: Springer US, 1992. http://dx.doi.org/10.1007/978-1-4615-3012-1.
Texto completo da fonteJ, Petroski Richard, McCormick Susan P e American Chemical Society, eds. Secondary-metabolite biosynthesis and metabolism. New York: Plenum Press, 1992.
Encontre o texto completo da fonteJiang, Xian-Cheng, ed. Sphingolipid Metabolism and Metabolic Disease. Singapore: Springer Nature Singapore, 2022. http://dx.doi.org/10.1007/978-981-19-0394-6.
Texto completo da fonteR, Verpoorte, e Alfermann A. W, eds. Metabolic engineering of plant secondary metabolism. Dordrecht: Kluwer Academic Publishers, 2000.
Encontre o texto completo da fonteVerpoorte, Robert, e A. W. Alfermann, eds. Metabolic Engineering of Plant Secondary Metabolism. Dordrecht: Springer Netherlands, 2000. http://dx.doi.org/10.1007/978-94-015-9423-3.
Texto completo da fonteMcCandless, David W., ed. Cerebral Energy Metabolism and Metabolic Encephalopathy. Boston, MA: Springer US, 1985. http://dx.doi.org/10.1007/978-1-4684-1209-3.
Texto completo da fonte1941-, McCandless David W., ed. Cerebral energy metabolism and metabolic encephalopathy. New York: Plenum Press, 1985.
Encontre o texto completo da fonte(Firm), Knovel, ed. Metabolic engineering of plant secondary metabolism. Dordrecht: Kluwer Academic Publishers, 2000.
Encontre o texto completo da fonteVerpoorte, Robert. Metabolic Engineering of Plant Secondary Metabolism. Dordrecht: Springer Netherlands, 2000.
Encontre o texto completo da fonteCapítulos de livros sobre o assunto "Metabolism"
Guo, Shenghao, Yanni Gu, Jiayin Qu e Anne Le. "Bridging the Metabolic Parallels Between Neurological Diseases and Cancer". In The Heterogeneity of Cancer Metabolism, 229–48. Cham: Springer International Publishing, 2021. http://dx.doi.org/10.1007/978-3-030-65768-0_17.
Texto completo da fonteSackmann-Sala, Lucila, D. R. Bailey Miles e John J. Kopchick. "Metabolism and Metabolic Regulation". In Laron Syndrome - From Man to Mouse, 451–63. Berlin, Heidelberg: Springer Berlin Heidelberg, 2010. http://dx.doi.org/10.1007/978-3-642-11183-9_52.
Texto completo da fonteVerpoorte, R. "Secondary Metabolism". In Metabolic Engineering of Plant Secondary Metabolism, 1–29. Dordrecht: Springer Netherlands, 2000. http://dx.doi.org/10.1007/978-94-015-9423-3_1.
Texto completo da fonteGünther, Ulrich L., Mei G. Chong, Tatiana Volpari, Katarzyna M. Koczula, Karen Atkins, Christopher M. Bunce e Farhat L. Khanim. "Metabolic Fluxes in Cancer Metabolism". In Tumor Cell Metabolism, 315–48. Vienna: Springer Vienna, 2015. http://dx.doi.org/10.1007/978-3-7091-1824-5_14.
Texto completo da fonteSaghiv, Moran S., e Michael S. Sagiv. "Metabolism". In Basic Exercise Physiology, 33–147. Cham: Springer International Publishing, 2020. http://dx.doi.org/10.1007/978-3-030-48806-2_2.
Texto completo da fonteDavidson, Debra J. "Metabolism". In Environment and Society, 47–70. Cham: Springer International Publishing, 2018. http://dx.doi.org/10.1007/978-3-319-76415-3_3.
Texto completo da fonteLeong, Wen B., Shahrad Taheri, Anna M. Stone e G. Neil Thomas. "Metabolism". In Encyclopedia of Behavioral Medicine, 1377–81. Cham: Springer International Publishing, 2020. http://dx.doi.org/10.1007/978-3-030-39903-0_472.
Texto completo da fonteKhanfer, Riyad, John Ryan, Howard Aizenstein, Seema Mutti, David Busse, Ilona S. Yim, J. Rick Turner et al. "Metabolism". In Encyclopedia of Behavioral Medicine, 1231–35. New York, NY: Springer New York, 2013. http://dx.doi.org/10.1007/978-1-4419-1005-9_472.
Texto completo da fonteCárdenas, María Luz, e Athel Cornish-Bowden. "Metabolism". In Encyclopedia of Astrobiology, 1–3. Berlin, Heidelberg: Springer Berlin Heidelberg, 2014. http://dx.doi.org/10.1007/978-3-642-27833-4_963-2.
Texto completo da fonteKooyman, Gerald L. "Metabolism". In Zoophysiology, 119–28. Berlin, Heidelberg: Springer Berlin Heidelberg, 1989. http://dx.doi.org/10.1007/978-3-642-83602-2_10.
Texto completo da fonteTrabalhos de conferências sobre o assunto "Metabolism"
Rogers, Hannah, e Adam Bencard. "Metabolism and Art". In 28th International Symposium on Electronic Art. Paris: Ecole des arts decoratifs - PSL, 2024. http://dx.doi.org/10.69564/isea2023-25-short-rogers-et-al-metabolism-and-art.
Texto completo da fonteAmaral, Cisnara Pires, Eduarda Pires Amaral e Cézane Priscila Reuter. "Cellular metabolism, genetics and lifestyle". In VI Seven International Multidisciplinary Congress. Seven Congress, 2024. http://dx.doi.org/10.56238/sevenvimulti2024-107.
Texto completo da fonteDorokhina, Yu A., e G. F. Ryzhkova. "Morphological and biochemical parameters of blood in rabbits when using energymetabolic compositions". In SPbVetScience. FSBEI HE St. Petersburg SUVM, 2023. http://dx.doi.org/10.52419/3006-2022-7-18-23.
Texto completo da fonteEl-fadl, Rihab, Nasser Rizk, Amena Fadel e Abdelrahman El Gamal. "The Profile of Hepatic Gene Expression of Glucose Metabolism in Mice on High Fat Diet". In Qatar University Annual Research Forum & Exhibition. Qatar University Press, 2020. http://dx.doi.org/10.29117/quarfe.2020.0213.
Texto completo da fonteMachado, Luiza, Camila Santos, Bianca Leonardi, Andréia Rocha, Igor Fontana, Bruna Bellaver, Gianina Venturin et al. "ACUTE PERIPHERAL INFLAMMATION IMPACT ON CEREBRAL GLUCOSE METABOLISM". In XIII Meeting of Researchers on Alzheimer's Disease and Related Disorders. Zeppelini Editorial e Comunicação, 2021. http://dx.doi.org/10.5327/1980-5764.rpda072.
Texto completo da fonteKisljakova, A. A. "ASSESSMENT OF INDICATORS OF METABOLIC DISORDERS IN WORKERS OCCUPATIONALLY EXPOSED BY POWER FREQUENCY ELECTRIC AND MAGNETIC FIELDS". In The 4th «OCCUPATION and HEALTH» International Youth Forum (OHIYF-2022). FSBSI «IRIOH», 2022. http://dx.doi.org/10.31089/978-5-6042929-6-9-2022-1-110-114.
Texto completo da fonteOcchipinti, Annalisa, e Claudio Angione. "A Computational Model of Cancer Metabolism for Personalised Medicine". In Building Bridges in Medical Science 2021. Cambridge Medicine Journal, 2021. http://dx.doi.org/10.7244/cmj.2021.03.001.3.
Texto completo da fonteHassenkam, Tue, Ester Tsai, Henning Osholm, Kim Dalby, David Mackenzie, Mirko Holler, Dario Ferreira, Daniel Grolimund, Stephan Bruns e Minik T. Rosing. "Eoarchean Iron Metabolism?" In Goldschmidt2020. Geochemical Society, 2020. http://dx.doi.org/10.46427/gold2020.973.
Texto completo da fonteSantos, Lucas, Gabriel Yarmush e Timothy Maguire. "A metabolic flux analyis to quantify the hepatic metabolism during defatting". In 2014 40th Annual Northeast Bioengineering Conference (NEBEC). IEEE, 2014. http://dx.doi.org/10.1109/nebec.2014.6972929.
Texto completo da fonteLatzer, Itay Tokatly, Melissa DiBacco, Thomas Opladen, Kathrin Jeltsch, Angels Garcia-Cazorla, Deniz Aygun, Alexander Rotenberg, Jean-Baptiste Roullet, Michael Gibson e Phillip Pearl. "Pathophysiology of Epilepsy in Inherited Metabolic Disorders of GABA Metabolism (S35.006)". In 2023 Annual Meeting Abstracts. Lippincott Williams & Wilkins, 2023. http://dx.doi.org/10.1212/wnl.0000000000201787.
Texto completo da fonteRelatórios de organizações sobre o assunto "Metabolism"
Corscadden, Louise, e Anjali Singh. Metabolism And Measurable Metabolic Parameters. ConductScience, dezembro de 2022. http://dx.doi.org/10.55157/me20221213.
Texto completo da fontePopov, V. S., N. V. Vorobeva e G. A. Svazlian. The relationship of energy metabolism and metabolism in pigs. Вестник Курской государственной сельскохозяйственной академии, 2019. http://dx.doi.org/10.18411/issn1997-0749.2019-03-74-79.
Texto completo da fonteGlaser, M. Cellular energy metabolism. Office of Scientific and Technical Information (OSTI), junho de 1991. http://dx.doi.org/10.2172/5714213.
Texto completo da fonteCroteau, R. [Regulation of terpene metabolism]. Office of Scientific and Technical Information (OSTI), janeiro de 1991. http://dx.doi.org/10.2172/6984681.
Texto completo da fonteCroteau, R. [Regulation of terpene metabolism]. Office of Scientific and Technical Information (OSTI), novembro de 1989. http://dx.doi.org/10.2172/6984921.
Texto completo da fonteCroteau, Rodney. Regulation of Terpene Metabolism. Office of Scientific and Technical Information (OSTI), março de 2004. http://dx.doi.org/10.2172/822599.
Texto completo da fonteCroteau, R. [Regulation of terpene metabolism]. Office of Scientific and Technical Information (OSTI), janeiro de 1992. http://dx.doi.org/10.2172/6687649.
Texto completo da fonteStarr, Robert C., Brennon R. Orr, M. Hope Lee e Mark Delwiche. Final Project Report - Coupled Biogeochemical Process Evaluation for Conceptualizing Trichloriethylene Co-Metabolism: Co-Metabolic Enzyme Activity Probes and Modeling Co-Metabolism and Attenuation. Office of Scientific and Technical Information (OSTI), fevereiro de 2010. http://dx.doi.org/10.2172/972652.
Texto completo da fonteKokurina, Olga Yu. SOCIETAL-METABOLIC SYSTEM OF THE STATE: EXPERIENCE OF SYNTHETIC RESEARCH. THE ELECTRONIC MANUAL. SIB-Expertise, dezembro de 2023. http://dx.doi.org/10.12731/er0756.18122023.
Texto completo da fonteClark, D. P. Thiophene metabolism by E. coli. Office of Scientific and Technical Information (OSTI), janeiro de 1991. http://dx.doi.org/10.2172/5512649.
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