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首页> 外文期刊>Molecular and Cellular Biology >Control of programmed cell death by the baculovirus genes p35 and iap.
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Control of programmed cell death by the baculovirus genes p35 and iap.

机译:通过杆状病毒基因p35和iap控制程序性细胞死亡。

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摘要

The SF-21 insect cell line undergoes rapid and widespread apoptosis when treated with actinomycin D or when infected with a mutant of the baculovirus Autographa californica nuclear polyhedrosis virus lacking a p35 gene or a functionally active iap (inhibitor of apoptosis) gene. Here we provide evidence that the basis for the induction of apoptosis by these two different stimuli is the cessation of RNA synthesis. We also show that expression of either p35 or two different functional iap homologs blocks apoptosis independently of other viral genes, indicating that these gene products act directly on the cellular apoptotic pathway. The iap genes encode a C3HC4 (or RING) finger motif found in a number of transcriptional regulatory proteins, as well as two additional Cys/His motifs (baculovirus iap repeats). We show that specific amino acids within both the C3HC4 finger and the N-terminal baculovirus iap repeat are critical for anti-apoptosis function. Overexpression of either mammalian bcl-2 or adenovirus E1B-19K, genes which block apoptosis when overexpressed in a number of mammalian cells, does not block actinomycin D-induced apoptosis in SF-21 cells.
机译:当用放线菌素D处理或感染了缺乏p35基因或功能性iap(凋亡抑制剂)基因的杆状病毒加州致病原核多角体病毒的突变体时,SF-21昆虫细胞系会迅速而广泛地凋亡。在这里,我们提供证据表明,这两种不同刺激诱导细胞凋亡的基础是停止RNA合成。我们还显示p35或两个不同的功能性iap同源物的表达独立于其他病毒基因阻止细胞凋亡,表明这些基因产物直接作用于细胞凋亡途径。 Iap基因编码在许多转录调节蛋白中发现的C3HC4(或RING)手指基序,以及两个其他Cys / His基序(杆状病毒Iap重复序列)。我们显示,C3HC4手指和N末端杆状病毒Iap重复序列内的特定氨基酸对于抗凋亡功能至关重要。哺乳动物bcl-2或腺病毒E1B-19K(在许多哺乳动物细胞中过表达时会阻止细胞凋亡的基因)的过表达不会阻止放线菌素D诱导的SF-21细胞凋亡。

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