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DPL-1 DP、LIN-35 Rb和EFL-1 E2F与MCD-1锌指蛋白共同作用,促进秀丽隐杆线虫的程序性细胞死亡。

DPL-1 DP, LIN-35 Rb and EFL-1 E2F act with the MCD-1 zinc-finger protein to promote programmed cell death in Caenorhabditis elegans.

作者信息

Reddien Peter W, Andersen Erik C, Huang Michael C, Horvitz H Robert

机构信息

Department of Biology, Howard Hughes Medical Institute, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, USA.

出版信息

Genetics. 2007 Apr;175(4):1719-33. doi: 10.1534/genetics.106.068148. Epub 2007 Jan 21.

DOI:10.1534/genetics.106.068148
PMID:17237514
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1855110/
Abstract

The genes egl-1, ced-9, ced-4, and ced-3 play major roles in programmed cell death in Caenorhabditis elegans. To identify genes that have more subtle activities, we sought mutations that confer strong cell-death defects in a genetically sensitized mutant background. Specifically, we screened for mutations that enhance the cell-death defects caused by a partial loss-of-function allele of the ced-3 caspase gene. We identified mutations in two genes not previously known to affect cell death, dpl-1 and mcd-1 (modifier of cell death). dpl-1 encodes the C. elegans homolog of DP, the human E2F-heterodimerization partner. By testing genes known to interact with dpl-1, we identified roles in cell death for four additional genes: efl-1 E2F, lin-35 Rb, lin-37 Mip40, and lin-52 dLin52. mcd-1 encodes a novel protein that contains one zinc finger and that is synthetically required with lin-35 Rb for animal viability. dpl-1 and mcd-1 act with efl-1 E2F and lin-35 Rb to promote programmed cell death and do so by regulating the killing process rather than by affecting the decision between survival and death. We propose that the DPL-1 DP, MCD-1 zinc finger, EFL-1 E2F, LIN-35 Rb, LIN-37 Mip40, and LIN-52 dLin52 proteins act together in transcriptional regulation to promote programmed cell death.

摘要

egl-1、ced-9、ced-4和ced-3基因在秀丽隐杆线虫的程序性细胞死亡中起主要作用。为了鉴定具有更细微活性的基因,我们在一个遗传敏感突变背景中寻找能导致强烈细胞死亡缺陷的突变。具体而言,我们筛选了能增强由ced-3半胱天冬酶基因的部分功能丧失等位基因所引起的细胞死亡缺陷的突变。我们在两个先前未知会影响细胞死亡的基因dpl-1和mcd-1(细胞死亡修饰因子)中鉴定到了突变。dpl-1编码人类E2F异二聚化伴侣DP的秀丽隐杆线虫同源物。通过测试已知与dpl-1相互作用的基因,我们鉴定出另外四个基因在细胞死亡中的作用:efl-1 E2F、lin-35 Rb、lin-37 Mip40和lin-52 dLin52。mcd-1编码一种含有一个锌指的新型蛋白质,并且它与lin-35 Rb在合成上是动物存活所必需的。dpl-1和mcd-1与efl-1 E2F和lin-35 Rb共同作用来促进程序性细胞死亡,并且它们是通过调节杀伤过程而非影响生存与死亡之间的决定来做到这一点的。我们提出DPL-1 DP、MCD-1锌指、EFL-1 E2F、LIN-35 Rb、LIN-37 Mip40和LIN-52 dLin52蛋白在转录调控中共同作用以促进程序性细胞死亡。

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