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真核生物翻译起始因子3k(eIF3k)通过从含角蛋白的包涵体中释放半胱天冬酶3来调节上皮细胞的凋亡。

eIF3k regulates apoptosis in epithelial cells by releasing caspase 3 from keratin-containing inclusions.

作者信息

Lin Yu-Min, Chen Yi-Ru, Lin Jia-Ren, Wang Won-Jing, Inoko Akihito, Inagaki Masaki, Wu Yi-Chun, Chen Ruey-Hwa

机构信息

Institute of Biochemical Sciences, National Taiwan University, Taiwan.

出版信息

J Cell Sci. 2008 Jul 15;121(Pt 14):2382-93. doi: 10.1242/jcs.021394. Epub 2008 Jun 24.

Abstract

Keratins 8 and 18 (collectively referred to as K8/K18) are the major components of intermediate filaments of simple epithelial cells. Recent studies have revealed the function of K8/K18 in apoptosis modulation. Here, we show that eIF3k, originally identified as the smallest subunit of eukaryotic translation initiation factor 3 (eIF3) complexes, also localizes to keratin intermediate filaments and physically associates with K18 in epithelial cells. Upon induction of apoptosis, eIF3k colocalizes with K8/K18 in the insoluble cytoplasmic inclusions. Depletion of endogenous eIF3k de-sensitizes simple epithelial cells to various types of apoptosis through a K8/K18-dependent mechanism and promotes the retention of active caspase 3 in cytoplasmic inclusions by increasing its binding to keratins. Consequently, the cleavage of caspase cytosolic and nuclear substrates, such as ICAD and PARP, respectively, is reduced in eIF3k-depleted cells. This study not only reveals the existence of eIF3k in a subcellular compartment other than the eIF3 complex, but also identifies an apoptosis-promoting function of eIF3k in simple epithelial cells by relieving the caspase-sequestration effect of K8/K18, thereby increasing the availability of caspases to their non-keratin-residing substrates.

摘要

角蛋白8和18(统称为K8/K18)是单层上皮细胞中间丝的主要成分。最近的研究揭示了K8/K18在细胞凋亡调控中的功能。在此,我们表明,最初被鉴定为真核翻译起始因子3(eIF3)复合体最小亚基的eIF3k,也定位于角蛋白中间丝,并在上皮细胞中与K18发生物理结合。在诱导细胞凋亡时,eIF3k与K8/K18共定位于不溶性细胞质内含物中。内源性eIF3k的缺失通过一种依赖K8/K18的机制使单层上皮细胞对各种类型的细胞凋亡不敏感,并通过增加活性半胱天冬酶3与角蛋白的结合促进其在细胞质内含物中的保留。因此,在eIF3k缺失的细胞中,半胱天冬酶的胞质和核底物(如ICAD和PARP)的切割减少。这项研究不仅揭示了eIF3k在eIF3复合体以外亚细胞区室中的存在,还通过减轻K8/K18对半胱天冬酶的隔离作用,从而增加半胱天冬酶对其非角蛋白驻留底物的可用性,确定了eIF3k在单层上皮细胞中的促凋亡功能。

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