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在最佳生长条件下抑制巨自噬的激酶的综合性 siRNA 筛选。

A comprehensive siRNA screen for kinases that suppress macroautophagy in optimal growth conditions.

机构信息

Apoptosis Department and Centre for Genotoxic Stress Research, Institute of Cancer Biology, Danish Cancer Society, Copenhagen, Denmark.

出版信息

Autophagy. 2011 Aug;7(8):892-903. doi: 10.4161/auto.7.8.15770. Epub 2011 Aug 1.

Abstract

Macroautophagy is a catabolic process that maintains cellular homeostasis and protects cells against various external stresses including starvation. Except for the identification of the Akt-mTORC1 pathway as a major negative regulator, little is known about signaling networks that control macroautophagy under optimal growth conditions. Therefore, we screened a human kinome siRNA library for siRNAs that increase the number of autophagosomes in normally growing MCF-7 human breast carcinoma cells, and identified 10 kinases as regulators of constitutive macroautophagy. Further analysis of these kinases with respect to the autophagic flux, kinase signaling and endolysosomal function identified WNK2 as a positive regulator of autophagosome maturation and nine others as macroautophagy inhibitors. The depletion of MK2, PACSIN1, DAPK2, CDKL3 and SCYL1 functioned upstream of Akt-mTORC1 pathway, whereas CSNK1A1, BUB1, PKLR and NEK4 suppressed autophagosome formation downstream or independent of mTORC1. Importantly, all identified kinases except for BUB1 regulated macroautophagy also in immortalized MCF-10A breast epithelial cells. The kinases identified here shed light to the complex regulation of macroautophagy and open new possibilities for its pharmacological manipulation.

摘要

自噬是一种分解代谢过程,它维持细胞内环境的稳定,并保护细胞免受各种外部应激,包括饥饿。除了鉴定 Akt-mTORC1 途径作为主要的负调控因子外,在最佳生长条件下控制自噬的信号网络知之甚少。因此,我们筛选了人激酶组 siRNA 文库,以寻找在正常生长的 MCF-7 人乳腺癌细胞中增加自噬体数量的 siRNA,并鉴定出 10 种激酶作为组成型自噬的调节剂。对这些激酶进行进一步分析,关于自噬流、激酶信号和内溶酶体功能,WNK2 被鉴定为自噬体成熟的正调节剂,另外 9 种则为自噬抑制剂。MK2、PACSIN1、DAPK2、CDKL3 和 SCYL1 的耗竭作用在前 Akt-mTORC1 途径上游,而 CSNK1A1、BUB1、PKLR 和 NEK4 则抑制自噬体的形成,位于 mTORC1 下游或独立于 mTORC1。重要的是,除了 BUB1 之外,所有鉴定出的激酶都在永生化 MCF-10A 乳腺上皮细胞中调节自噬。这里鉴定出的激酶阐明了自噬的复杂调控,并为其药理学操纵开辟了新的可能性。

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