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The physiological cost of antibiotic resistance /Mačvanin, Mirjana, January 2003 (has links)
Diss. (sammanfattning) Uppsala : Univ., 2003. / Härtill 4 uppsatser.
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Lipoprotein lipase : mechanism for adaptation of activity to the nutritional state /Wu, Gengshu, January 2004 (has links)
Diss. (sammanfattning) Umeå : Univ., 2004. / Härtill 4 uppsatser.
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Memória do medo condicionado ao contexto : alterações por inibição da síntese proteica ou por bloqueio de receptores de glutamato do tipo NMDA no hipocampo / Retrieval of the aversive memory : impairments by protein synthesis inhibition or blockade of NMDA glutamatergic receptor in the hippocampusSperandeo, Maria Luiza Antunes, 1949- 28 August 2013 (has links)
Orientador: Elenice Aparecida de Moraes Ferrari / Tese (doutorado) - Universidade Estadual de Campinas, Instituto de Biologia / Made available in DSpace on 2018-08-23T21:27:10Z (GMT). No. of bitstreams: 1
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Previous issue date: 2013 / Resumo: O estudo do condicionamento clássico aversivo contribuiu para caracterizar as fases da formação da memória (aquisição, consolidação, reconsolidação, persistência e extinção) e os mecanismos de plasticidade neuronal subjacentes. Entre estes, a ativação de receptores glutamatérgicos NMDA, de transcrição gênica e síntese proteica parecem fundamentais. O fator neurotrófico derivado de cérebro (BDNF) e o gene de expressão imediata (IEG) zenk são ativados no hipocampo de mamíferos durante a reconsolidação e a extinção. Este estudo investigou os efeitos da inibição da síntese proteica e do bloqueio dos receptores NMDA no hipocampo de pombos na reconsolidação e extinção da memória de medo contextual. No Experimento 1, pombos foram condicionados, testados ao contexto (reativação), submetidos à infusão intra-hipocampo de salina (SAL-PR), de anisomicina (ANI-PR) ou de MK-801 (MK-PR) após o teste (pós-reativação; PR), e retestados 2 dias depois (Rt 2d). No Experimento 2, três grupos tiveram um segundo reteste, 9 dias após a infusão (Rt 9d), enquanto que outros três grupos não passaram pelo teste (sem reativação- SR). O treino (20 min) teve três pareamentos som-choque. No teste e no Rt 2d houve exposição ao contexto do condicionamento por 5 min e no reteste Rt 9d, por 30 min. Nos dois experimentos, todos os grupos apresentaram alta ocorrência de congelamento (CONG) nas sessões de treino e de teste, mas no Rt 2d os grupos ANI-PR e MK-PR mostraram uma redução significativa de CONG (p < 0,05). Os grupos SR exibiram alta ocorrência de CONG tanto no Rt 2d, quanto no início do Rt 9d (p > 0,05). No Rt 9d o grupo MK-PR não teve recuperação espontânea de CONG, sugerindo prejuízo irreversível provocado pelo MK-801 na memória de medo contextual. Os grupos, SAL-PR, SAL-SR, ANI-PR, ANI-SR e MK-SR mostraram diminuição gradual de CONG durante a sessão de Rt 9d, evidenciando a extinção. Análises com Western blotting após o Rt 9d indicaram que o conteúdo de BDNF-maduro no hipocampo dos pombos SAL-PR foi significativamente maior em comparação aos demais grupos (p < 0,05), mas não foram observadas diferenças entre os grupos para o Zenk (p > 0,05). Isso sugere a participação do BDNF hipocampal na reconsolidação e na extinção da memória de medo contextual em pombos. Assim, a inibição da síntese proteica e o bloqueio dos receptores NMDA no hipocampo de pombos, após o teste ao contexto, prejudicaram a reconsolidação da memória de medo condicionado ao contexto. Além disso, os prejuízos observados foram dependentes da reativação da memória durante o teste / Abstract: The study of classical aversive conditioning has contributed to the characterization of different phases in memory formation (acquisition, consolidation, reconsolidation, extinction and persistence) and the underlying mechanisms of neuronal plasticity. Among these, the activation of NMDA glutamate receptors, gene transcription and protein synthesis are pointed as essentials. The brain-derived neurotrophic factor (BDNF) and immediate expression gene (IEG) zenk are activated in the hippocampus of mammals during reconsolidation and extinction. This study investigated the effects of protein synthesis inhibition and blockade of NMDA receptors in the hippocampus of pigeons on reconsolidation and extinction of contextual fear memory. In Experiment 1, pigeons were conditioned, tested in the context (reactivation), received intra-hippocampus infusion of saline (SAL-PR), anisomycin (ANI-PR) or MK-801 (MK-PR) after the test (post-reactivation, PR), and had a retest two days later (Rt 2d). Experiment 2, had a retest 9 days after intra-hippocampus infusion (Rt 9d) for three PR groups, and other three groups that were not tested 24h after training served as control for reactivation (no reactivation-NR). Three tone-shock pairings were presented during training (20 min). Pigeons were exposed to the context during 5 min in the test and Rt 2d sessions and during 30 min in Rt 9d. In both experiments, the occurrence of freezing (FRZ) was high in training and testing sessions for all the groups, but ANI-PR and MK-PR pigeons showed a significant decrease in FRZ during the Rt 2d (p < 0.05). The NR groups exhibited high occurrence of FRZ both in the Rt 2d and in the beginning of Rt 9d (p > 0.05). MK-PR pigeons had no spontaneous recovery of FRZ, suggesting irreversible impairment caused by MK-801 in contextual fear memory. The groups, SAL-PR, SAL-NR, ANI-PR, ANI-NR and MK-NR showed a gradual decrease in FRZ during the Rt 9d session, evidencing extinction. Western Blotting analysis indicated that the content of mature BDNF in the hippocampus of SAL-PR group after Rt 9d session was higher than that seen for the other groups (p < 0.05), but no between-group differences for Zenk were observed (p > 0.05). This suggests the involvement of hippocampal BDNF in reconsolidation and extinction of contextual fear memory in pigeons. The present data show that inhibition of protein synthesis and blockade of NMDA receptors in the hippocampus of pigeons, after the testing session to context, impaired reconsolidation of contextual fear conditioning memory and affected the process of extinction. Furthermore, the impairments were dependent on the reactivation of fear memory during the test / Doutorado / Fisiologia / Doutor em Biologia Funcional e Molecular
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Antibiotic Efficacy and Interaction in Escherichia coli during Varying Nutrient ConditionsMillar, Kristina K 01 January 2016 (has links)
Due to the recent rise in antibiotic resistant pathogens, and the difficulties surrounding the quest for new antibiotics, many researchers have started revisiting antibiotic interactions in hopes of finding new treatment options. The primary outcome of this project was to examine the efficacy of concomitant antibiotic use under varying nutrient conditions, to identify variations in antibiotic interactions. Antibiotic interactions were studied, utilizing E. coli as a model bacterial system, grown in four different media types. E. coli cultures were treated with streptomycin, tobramycin, erythromycin, and amikacin individually and in a pairwise fashion at varying doses. We found that at least some antibiotic efficacies were dependent on the environmental nutrient conditions E. coli was grown in, as the antibiotics were not equally effective in all media types. E. coli grown in potato dextrose broth, in particular, showed extremely high tolerance to antibiotic inhibition. In addition, we observed several variations in antibiotic interactions, depending on the combination of antibiotics and environmental conditions utilized. It is predicted that differences in available nutrients is the primary cause of the observed discrepancies in antibiotic properties between media. The observation of changes in antibiotic efficacy under different environmental and nutrient conditions has serious implications for use of antibiotic combinations as drug treatments. Not all microenvironments within the human body have identical nutrient make-up. If the interactions antibiotics are reported to have in one environmental condition change under another, reckless prescription of combinations could lead to a serious adverse reaction. Thus, this is an important area for future in vitro and in vivo research.
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The Effect of Light on Carotenoid Synthesis in Corynebacterium 7E1CEndicott, George R. 05 1900 (has links)
The effects of light, light "mimicking" chemicals, and protein synthesis inhibitors on the photo-induced carotenogenesis of Corynebacterium 7EIC were studied. Changes in the dosage of fluorescent light applied to dark grown cells showed a dose related carotenogenic response. Maintaining the same dosage but varying the wavelength of monochromatic light revealed that light with a wavelength of 280 to 450nm was responsible for photo-induction. It further showed a peak of photo-induction between the wavelengths of 370 and 430nm. The light "mimicking" chemicals antimycin A and p-Chloromercurybenzoate were shown to have no light "mimicking" effects. The transcriptional inhibitor of protein synthesis actinomycin D partially inhibited, and chloramphenicol a translational inhibitor, completely inhibited photo-induced carotenogenesis.
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Crystallographic characterization of the ribosomal binding site and molecular mechanism of action of Hygromycin A.Kaminishi, Tatsuya, Schedlbauer, Andreas, Fabbretti, Attilio, Brandi, Letizia, Ochoa Lizarralde, Borja, He, Cheng-Guang, Milon, Pohl, Connell, Sean R, Gualerzi, Claudio O, Fucini, Paola 16 November 2015 (has links)
Hygromycin A (HygA) binds to the large ribosomal subunit and inhibits its peptidyl transferase (PT) activity. The presented structural and biochemical data indicate that HygA does not interfere with the initial binding of aminoacyl-tRNA to the A site, but prevents its subsequent adjustment such that it fails to act as a substrate in the PT reaction. Structurally we demonstrate that HygA binds within the peptidyl transferase center (PTC) and induces a unique conformation. Specifically in its ribosomal binding site HygA would overlap and clash with aminoacyl-A76 ribose moiety and, therefore, its primary mode of action involves sterically restricting access of the incoming aminoacyl-tRNA to the PTC. / Bizkaia:Talent and the European Union's Seventh Framework Program (Marie Curie Actions; COFUND; to S.C., A.S., T.K.); Marie Curie Actions Career Integration Grant (PCIG14-GA-2013-632072 to P.F.); Ministerio de Economía Y Competitividad (CTQ2014-55907-R to P.F., S.C.); FIRB Futuro in Ricerca from the Italian Ministero dell'Istruzione, dell'Universitá e della Ricerca (RBFR130VS5_001 to A.F.); Peruvian Programa Nacional de Innovación para la Competitividad y Productividad (382-PNICP-PIBA-2014 (to P.M. and A.F.)). Funding for open access charge: Institutional funding. / Revisión por pares
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