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Le vieillissement chronologique de Schizosaccharomyces pombe: Implication des voies de detection du glucose.

机译:粟酒裂殖酵母的时间序列老化:葡萄糖检测途径的含义。

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摘要

The first increase in life span due to man's intervention was obtained with rats subjected to a diet reduced in calorie intake. Later, this phenomenon was repeated with many other species and referred as diet restriction or calorie restriction. The development of modern Molecular Biology approaches and the use of simple model organisms demonstrated that the rate of aging was regulated by genetic traits. Indeed, several cellular mechanisms were identified as responsible for the control of aging. These regulatory pathways appear to be conserved throughout species, from yeast to multicellular organisms like nematode, fly and mice, thus suggesting the existence of a universal program of aging.;Research in the molecular mechanisms of aging propose holds the promise to bring precious clues as to this mysterious processes affecting all living creatures, and paves the way to unravel the underlying causes of many human diseases. Indeed, aging is the first cause of numerous late-onset pathologies including cancers, cardiovascular diseases or neurodegenerative diseases like Alzheimer and Parkinson syndromes.;Keywords: aging, longevity, life span, yeast, schizosaccharomyces pombe, stationary phase, pka, sck2;Yeast proved several times to be a powerful and reliable model for discovering genes involved in the regulation of aging. My study consisted in developing Schizosaccharomyces pombe (also called fission yeast) as a new unicellular model to study aging. The first step of my work was to show that pathways of nutrient detection through kinases involving Pka1 and Sck2 control chronological aging in S. pombe, as it was previously demonstrated in Saccharomyces cerevisiae. This first work validated the use of fission yeast for the study of aging. Subsequently, we analysed in more detail the pro-aging effect of glucose focusing on the role of its signalling through the G-protein Gpa2-coupled membrane receptor Git3, which acts upstream of Pka1. The loss of the glucose signal due to deletion of Git3 mimics partially the effect of increasing longevity by reducing glucose in the medium. Moreover, detrimental effects of glucose signal are maintained in absence of sugar metabolism following loss of hexokinases, the first enzymes of glycolysis. Together, these results suggest that the pro-aging effects of glucose signalling are predominant over those due to metabolism of this sugar. Moreover, both obliteration of this signalling pathway and decrease of glucose availability extend life span, and correlate with an increase in stress resistance, in mitochondrial activity and a lower production of free radicals. Finally, screening a cDNA-overexpression library allowed us to identify several genes candidates responsible for the effects on longevity downstream of Git3/Pka1.
机译:饮食减少卡路里摄入的大鼠获得了由于人为干预而导致的寿命的首次增加。后来,这种现象在许多其他物种中屡见不鲜,被称为饮食限制或卡路里限制。现代分子生物学方法的发展和简单模型生物的使用表明,衰老的速度受遗传特性的调节。实际上,已确定几种细胞机制负责衰老的控制。这些调节途径似乎在整个物种中都是保守的,从酵母到线虫,果蝇和小鼠等多细胞生物,因此表明存在衰老的通用程序。衰老的分子机制研究提出了带来宝贵线索的希望。这一影响所有生物的神秘过程,为揭示许多人类疾病的根本原因铺平了道路。的确,衰老是许多迟发性病理的首要原因,包括癌症,心血管疾病或神经退行性疾病,例如阿尔茨海默氏症和帕金森综合症;关键词:衰老,寿命,寿命,酵母,裂殖酵母,固定相,pka,sck2;酵母多次证明是发现衰老调控基因的有力且可靠的模型。我的研究包括开发粟酒裂殖酵母(也称为裂变酵母)作为研究衰老的新单细胞模型。我工作的第一步是证明通过涉及Pka1和Sck2的激酶进行营养物检测的途径可以控制粟酒裂殖酵母按时间顺序的老化,正如先前在酿酒酵母中所证明的那样。这项第一项工作验证了裂变酵母在衰老研究中的应用。随后,我们更详细地分析了葡萄糖的促衰老作用,重点是其通过G蛋白Gpa2偶联的膜受体Git3(在Pka1上游起作用)的信号传导作用。由于缺失Git3而导致的葡萄糖信号损失部分模拟了通过减少培养基中的葡萄糖来延长寿命的效果。此外,在己糖激酶(糖酵解的第一种酶)丢失后,在没有糖代谢的情况下,葡萄糖信号的不利影响得以维持。总之,这些结果表明,葡萄糖信号转导的衰老效应比由于该糖的代谢而产生的衰老效应更为重要。而且,消除该信号传导途径和减少葡萄糖的利用都延长了寿命,并且与抗逆性的增加,线粒体活性和自由基产生的降低相关。最后,筛选cDNA过表达文库使我们能够鉴定出几个基因,这些基因对Git3 / Pka1下游的寿命产生影响。

著录项

  • 作者

    Antoine, Emile Roux.;

  • 作者单位

    Universite de Montreal (Canada).;

  • 授予单位 Universite de Montreal (Canada).;
  • 学科 Chemistry Biochemistry.;Health Sciences Aging.
  • 学位 Ph.D.
  • 年度 2009
  • 页码 335 p.
  • 总页数 335
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学;
  • 关键词

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