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A functional genomics screen identifies PCAF and ADA3 as regulators of human granzyme B-mediated apoptosis and Bid cleavage

机译：功能基因组学筛选确定PCAF和ADA3是人类粒酶B介导的细胞凋亡和Bid裂解的调节因子

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The human lymphocyte toxins granzyme B (hGrzB) and perforin cooperatively induce apoptosis of virus-infected or transformed cells: perforin pores enable entry of the serine protease hGrzB into the cytosol, where it processes Bid to selectively activate the intrinsic apoptosis pathway. Truncated Bid (tBid) induces Bax/Bak-dependent mitochondrial outer membrane permeability and the release of cytochrome c and Smac/Diablo. To identify cellular proteins that regulate perforin/hGrzB-mediated Bid cleavage and subsequent apoptosis, we performed a gene-knockdown (KD) screen using a lentiviral pool of short hairpin RNAs embedded within a miR30 backbone (shRNAmiR). We transduced HeLa cells with a lentiviral pool expressing shRNAmiRs that target 1213 genes known to be involved in cell death signaling and selected cells with acquired resistance to perforin/hGrzB-mediated apoptosis. Twenty-two shRNAmiRs were identified in the positive-selection screen including two, PCAF and ADA3, whose gene products are known to reside in the same epigenetic regulatory complexes. Small interfering (si)RNA-mediated gene-KD of PCAF or ADA3 also conferred resistance to perforin/hGrzB-mediated apoptosis providing independent validation of the screen results. Mechanistically, PCAF and ADA3 exerted their pro-apoptotic effect upstream of mitochondrial membrane permeabilization, as indicated by reduced cytochrome c release in PCAF-KD cells exposed to perforin/hGrzB. While overall levels of Bid were unaltered, perforin/hGrzB-mediated cleavage of Bid was reduced in PCAF-KD or ADA3-KD cells. We discovered that PCAF-KD or ADA3-KD resulted in reduced expression of PACS2, a protein implicated in Bid trafficking to mitochondria and importantly, targeted PACS2-KD phenocopied the effect of PCAF-KD or ADA3-KD. We conclude that PCAF and ADA3 regulate Bid processing via PACS2, to modulate the mitochondrial cell death pathway in response to hGrzB.

机译：人淋巴细胞毒素颗粒酶B（hGrzB）和穿孔素协同诱导病毒感染或转化的细胞凋亡：穿孔素孔使丝氨酸蛋白酶hGrzB进入细胞质，在其中处理Bid以选择性激活内在的凋亡途径。截短出价（tBid）诱导Bax / Bak依赖的线粒体外膜通透性以及细胞色素c和Smac / Diablo的释放。为了鉴定调节穿孔素/ hGrzB介导的Bid裂解和随后的细胞凋亡的细胞蛋白，我们使用了嵌入在miR30骨架（shRNAmiR）中的短发夹RNA的慢病毒池，进行了基因敲低（KD）筛选。我们用表达shRNAmiR的慢病毒池转导了HeLa细胞，该shRNAmiR靶向已知参与细胞死亡信号转导的1213个基因，并选择了对穿孔素/ hGrzB介导的凋亡具有抗性的选定细胞。在正选择筛选中鉴定出22个shRNAmiR，包括两个PCAF和ADA3，已知它们的基因产物位于相同的表观遗传调控复合物中。 PCAF或ADA3的小干扰（si）RNA介导的基因KD也赋予了对穿孔素/ hGrzB介导的细胞凋亡的抗性，从而独立验证了筛选结果。从机理上讲，PCAF和ADA3在线粒体膜通透性上游发挥其促凋亡作用，这表明暴露于穿孔素/ hGrzB的PCAF-KD细胞中细胞色素C释放减少。虽然Bid的总体水平没有改变，但在PCAF-KD或ADA3-KD细胞中穿孔素/ hGrzB介导的Bid切割减少了。我们发现PCAF-KD或ADA3-KD降低了PACS2的表达，该蛋白与线粒体的标价运输有关，重要的是，靶向PACS2-KD表彰了PCAF-KD或ADA3-KD的作用。我们得出的结论是PCAF和ADA3通过PACS2调节出价处理，以调节响应hGrzB的线粒体细胞死亡途径。

著录项

期刊名称 Cell Death and Differentiation
作者
D Brasacchio; T Noori; C House; A J Brennan; K J Simpson; O Susanto; P I Bird; R W Johnstone; J A Trapani;
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作者单位

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年(卷),期 2014(21),5
年度 2014
页码 748–760
总页数 13
原文格式 PDF
正文语种
中图分类分子生物学;细胞生物学;
关键词
granzyme B perforin cell death PCAF ADA3 Bid;

机译：颗粒酶B;穿孔素;细胞死亡;PCAF;ADA3;出价;

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专利

1. A functional genomics screen identifies PCAF and ADA3 as regulators of human granzyme B-mediated apoptosis and Bid cleavage [J] . Brasacchio D., Noori T., House C., Cell death and differentiation . 2014,第5期

机译：功能基因组学筛选确定PCAF和ADA3是人类粒酶B介导的细胞凋亡和Bid裂解的调节因子
2. Initiation of Apoptosis by Granzyme B Requires Direct Cleavage of Bid, but Not Direct Granzyme B–Mediated Caspase Activation [J] . Vivien R. Sutton, Joanne E. Davis, Michael Cancilla, The Journal of Experomental Medicine . 2000,第10期

机译：粒酶B启动细胞凋亡需要直接切割出价，但不需要粒酶B介导的半胱天冬酶激活。
3. Response to Comment on “TCR Activation Eliminates Glutamate Receptor GluR3 from the Cell Surface of Normal Human T Cells, via an Autocrine/Paracrine Granzyme B-Mediated Proteolytic Cleavage” [J] . Mia Levite The journal of immunology . 2008,第4期

机译：对评论“ TCR激活通过自分泌/旁分泌颗粒酶B介导的蛋白水解裂解作用消除了正常人T细胞细胞表面的谷氨酸受体GluR3”的评论。
4. Real-time single cell analysis of Bid cleavage and translocation in cisplatin-induced apoptosis [C] . Lei Liu, Da Xing, Yihui Pei, Biophotonics and Immune Responses II; Progress in Biomedical Optics and Imaging; vol.8 no.15; Proceedings of SPIE-The International Society for Optical Engineering; vol.6438 . 2007

机译：实时单细胞分析顺铂诱导的凋亡中的卵裂和转运
5. Mutations to Bid cleavage sites protect hepatocytes from death receptor- and cell-mediated apoptosis. [D] . Riddle, Erica Delores. 2006

机译：出价切割位点的突变可保护肝细胞免受死亡受体和细胞介导的细胞凋亡。
6. Initiation of Apoptosis by Granzyme B Requires Direct Cleavage of Bid but Not Direct Granzyme B–Mediated Caspase Activation [O] . Vivien R. Sutton, Joanne E. Davis, Michael Cancilla, 2000

机译：粒酶B启动细胞凋亡需要直接切割出价但不需要粒酶B介导的半胱天冬酶激活。
7. A functional genomics screen identifies PCAF and ADA3 as regulators of human granzyme B-mediated apoptosis and Bid cleavage [O] . D Brasacchio, T Noori, C House, 2014

机译：功能基因组筛网将PCAF和ADA3识别为人类颗粒Zyme B介导的细胞凋亡和BID切割的调节器
8. Parallel Genomic and Chemical Screens to Identify Both Therapeutic Targets and Inhibitors of These Targets in the Treatment of Neurofibromatosis [R] . Perrimon, N. 2006

机译：平行基因组和化学筛选，以确定这些目标的治疗目标和抑制剂治疗神经纤维瘤病

A functional genomics screen identifies PCAF and ADA3 as regulators of human granzyme B-mediated apoptosis and Bid cleavage

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