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含三联基序蛋白22在细胞核和核仁体中的动态定位

Dynamic localization of tripartite motif-containing 22 in nuclear and nucleolar bodies.

作者信息

Sivaramakrishnan Gayathri, Sun Yang, Tan Si Kee, Lin Valerie C L

机构信息

School of Biological Sciences, Nanyang Technological University, 60 Nanyang Drive, Singapore 637551, Singapore.

出版信息

Exp Cell Res. 2009 May 1;315(8):1521-32. doi: 10.1016/j.yexcr.2009.01.028. Epub 2009 Feb 10.

Abstract

Tripartite motif-containing 22 (TRIM22) exhibits antiviral and growth inhibitory properties, but there has been no study on the localization and dynamics of the endogenous TRIM22 protein. We report here that TRIM22 is dramatically induced by progesterone in MDA-MB-231-derived ABC28 cells and T47D cells. This induction was associated with an increase in TRIM22 nuclear bodies (NB), and an even more prominent increase in nucleolar TRIM22 bodies. Distinct endogenous TRIM22 NB were also demonstrated in several other cell lines including MCF7 and HeLa cells. These TRIM22 NB resemble Cajal bodies, co-localized with these structures and co-immunoprecipitated with p80-coilin. However, IFNgamma-induced TRIM22 in HeLa and MCF7 cells did not form NB, implying the forms and distribution of TRIM22 are regulated by specific cellular signals. This notion is also supported by the observation that TRIM22 NB undergoes dynamic cell-cycle dependent changes in distribution such that TRIM22 NB started to form in early G0/G1 but became dispersed in the S-phase. In light of its potential antiviral and antitumor properties, the findings here provide an interesting gateway to study the relationship between the different forms and functions of TRIM22.

摘要

含三联基序蛋白22(TRIM22)具有抗病毒和生长抑制特性,但目前尚无关于内源性TRIM22蛋白定位和动态变化的研究。我们在此报告,在源自MDA-MB-231的ABC28细胞和T47D细胞中,孕酮可显著诱导TRIM22表达。这种诱导与TRIM22核体(NB)数量增加相关,而核仁TRIM22体的增加更为显著。在包括MCF7和HeLa细胞在内的其他几种细胞系中也证实了不同的内源性TRIM22 NB。这些TRIM22 NB类似于卡哈尔体,与这些结构共定位,并与p80卷曲螺旋蛋白共免疫沉淀。然而,干扰素γ诱导HeLa和MCF7细胞中的TRIM22并不形成NB,这意味着TRIM22的形式和分布受特定细胞信号调控。TRIM22 NB在细胞周期中分布呈现动态变化,即TRIM22 NB在G0/G1早期开始形成,但在S期分散,这一观察结果也支持了这一观点。鉴于其潜在的抗病毒和抗肿瘤特性,本文的研究结果为研究TRIM22不同形式与功能之间的关系提供了一个有趣的切入点。

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