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SG2NA 是内质网(ER)稳态的调节剂,因为其缺失会导致 ER 应激。

SG2NA is a regulator of endoplasmic reticulum (ER) homeostasis as its depletion leads to ER stress.

机构信息

School of Life Sciences, Jawaharlal Nehru University, New Mehrauli Road, New Delhi, 110067, India.

Department of Zoology, School of Life Sciences, Mahatma Gandhi Central University Bihar, Motihari, 845401, India.

出版信息

Cell Stress Chaperones. 2017 Nov;22(6):853-866. doi: 10.1007/s12192-017-0816-7. Epub 2017 Jun 21.

Abstract

SG2NA belongs to a three-member striatin subfamily of WD40 repeat superfamily of proteins. It has multiple protein-protein interaction domains involved in assembling supramolecular signaling complexes. Earlier, we had demonstrated that there are at least five variants of SG2NA generated by alternative splicing, intron retention, and RNA editing. Such versatile and dynamic mode of regulation implicates it in tissue development. In order to shed light on its role in cell physiology, total proteome analysis was performed in NIH3T3 cells depleted of 78 kDa SG2NA, the only isoform expressing therein. A number of ER stress markers were among those modulated after knockdown of SG2NA. In cells treated with the ER stressors thapsigargin and tunicamycin, expression of SG2NA was increased at both mRNA and protein levels. The increased level of SG2NA was primarily in the mitochondria and the microsomes. A mouse injected with thapsigargin also had an increase in SG2NA in the liver but not in the brain. Cell cycle analysis suggested that while loss of SG2NA reduces the level of cyclin D1 and retains a population of cells in the G1 phase, concurrent ER stress facilitates their exit from G1 and traverse through subsequent phases with concomitant cell death. Thus, SG2NA is a component of intrinsic regulatory pathways that maintains ER homeostasis.

摘要

SG2NA 属于 WD40 重复超家族的三成员条纹蛋白亚家族。它具有多个参与组装超分子信号复合物的蛋白质-蛋白质相互作用结构域。早期,我们已经证明至少有五种变体的 SG2NA 通过选择性剪接、内含子保留和 RNA 编辑产生。这种多样和动态的调节模式表明它参与了组织发育。为了阐明其在细胞生理学中的作用,在缺乏其中唯一表达的 78 kDa SG2NA 的 NIH3T3 细胞中进行了总蛋白质组分析。在敲低 SG2NA 后,许多 ER 应激标志物被调节。在用 ER 应激剂 thapsigargin 和 tunicamycin 处理的细胞中,SG2NA 的表达在 mRNA 和蛋白质水平上均增加。增加的 SG2NA 水平主要在线粒体和微粒体中。用 thapsigargin 注射的小鼠在肝脏中 SG2NA 也增加,但在大脑中没有增加。细胞周期分析表明,尽管 SG2NA 的缺失降低了细胞周期蛋白 D1 的水平并使一部分细胞保留在 G1 期,但同时发生的 ER 应激促进它们从 G1 期退出并通过随后的阶段,伴随着细胞死亡。因此,SG2NA 是维持内质网稳态的内在调节途径的组成部分。

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