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酿酒酵母的黄素蛋白质组

The flavoproteome of the yeast Saccharomyces cerevisiae.

作者信息

Gudipati Venugopal, Koch Karin, Lienhart Wolf-Dieter, Macheroux Peter

机构信息

Graz University of Technology, Institute of Biochemistry, Petersgasse 12, A-8010 Graz, Austria.

Graz University of Technology, Institute of Biochemistry, Petersgasse 12, A-8010 Graz, Austria.

出版信息

Biochim Biophys Acta. 2014 Mar;1844(3):535-44. doi: 10.1016/j.bbapap.2013.12.015. Epub 2013 Dec 27.

Abstract

Genome analysis of the yeast Saccharomyces cerevisiae identified 68 genes encoding flavin-dependent proteins (1.1% of protein encoding genes) to which 47 distinct biochemical functions were assigned. The majority of flavoproteins operate in mitochondria where they participate in redox processes revolving around the transfer of electrons to the electron transport chain. In addition, we found that flavoenzymes play a central role in various aspects of iron metabolism, such as iron uptake, the biogenesis of iron-sulfur clusters and insertion of the heme cofactor into apocytochromes. Another important group of flavoenzymes is directly (Dus1-4p and Mto1p) or indirectly (Tyw1p) involved in reactions leading to tRNA-modifications. Despite the wealth of genetic information available for S. cerevisiae, we were surprised that many flavoproteins are poorly characterized biochemically. For example, the role of the yeast flavodoxins Pst2p, Rfs1p and Ycp4p with regard to their electron donor and acceptor is presently unknown. Similarly, the function of the heterodimeric Aim45p/Cir1p, which is homologous to the electron-transferring flavoproteins of higher eukaryotes, in electron transfer processes occurring in the mitochondrial matrix remains to be elucidated. This lack of information extends to the five membrane proteins involved in riboflavin or FAD transport as well as FMN and FAD homeostasis within the yeast cell. Nevertheless, several yeast flavoproteins, were identified as convenient model systems both in terms of their mechanism of action as well as structurally to improve our understanding of diseases caused by dysfunctional human flavoprotein orthologs.

摘要

对酿酒酵母的基因组分析鉴定出68个编码黄素依赖性蛋白的基因(占蛋白编码基因的1.1%),并赋予了它们47种不同的生化功能。大多数黄素蛋白在线粒体中发挥作用,参与围绕电子传递至电子传递链的氧化还原过程。此外,我们发现黄素酶在铁代谢的各个方面发挥核心作用,如铁摄取、铁硫簇的生物合成以及血红素辅因子插入脱辅基细胞色素中。另一类重要的黄素酶直接(Dus1 - 4p和Mto1p)或间接(Tyw1p)参与导致tRNA修饰的反应。尽管酿酒酵母有丰富的遗传信息,但我们惊讶地发现许多黄素蛋白的生化特性却知之甚少。例如,酵母黄素氧还蛋白Pst2p、Rfs1p和Ycp4p的电子供体和受体作用目前尚不清楚。同样,与高等真核生物的电子传递黄素蛋白同源的异二聚体Aim45p/Cir1p在线粒体基质中发生的电子传递过程中的功能仍有待阐明。这种信息缺乏也延伸到参与核黄素或FAD转运以及酵母细胞内FMN和FAD稳态的五种膜蛋白。然而,一些酵母黄素蛋白,无论是从其作用机制还是结构方面,都被确定为方便的模型系统,以增进我们对由功能失调的人类黄素蛋白直系同源物引起的疾病的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec26/3991850/30d57f82d9d8/sc1.jpg

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