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TSPO基因插入后能量和细胞代谢的功能增强。

Functional gains in energy and cell metabolism after TSPO gene insertion.

作者信息

Liu Guo-Jun, Middleton Ryan J, Kam Winnie Wai-Ying, Chin David Y, Hatty Claire R, Chan Ronald H Y, Banati Richard B

机构信息

a Australian Nuclear Science and Technology Organisation , Lucas Heights , NSW , Australia.

b Faculty of Health Science and Brain and Mind Centre, University of Sydney , NSW , Australia.

出版信息

Cell Cycle. 2017 Mar 4;16(5):436-447. doi: 10.1080/15384101.2017.1281477. Epub 2017 Jan 19.

Abstract

Recent loss-of-function studies in tissue-specific as well as global Tspo (Translocator Protein 18 kDa) knockout mice have not confirmed its long assumed indispensability for the translocation of cholesterol across the mitochondrial inter-membrane space, a rate-limiting step in steroid biosynthesis. Instead, recent studies in global Tspo knockout mice indicate that TSPO may play a more fundamental role in cellular bioenergetics, which may include the indirect down-stream regulation of transport or metabolic functions. To examine whether overexpression of the TSPO protein alters the cellular bioenergetic profile, Jurkat cells with low to absent endogenous expression were transfected with a TSPO construct to create a stable cell line with de novo expression of exogenous TSPO protein. Expression of TSPO was confirmed by RT-qPCR, radioligand binding with [3H]PK11195 and immunocytochemistry with a TSPO antibody. We demonstrate that TSPO gene insertion causes increased transcription of genes involved in the mitochondrial electron transport chain. Furthermore, TSPO insertion increased mitochondrial ATP production as well as cell excitability, reflected in a decrease in patch clamp recorded rectified K channel currents. These functional changes were accompanied by an increase in cell proliferation and motility, which were inhibited by PK11195, a selective ligand for TSPO. We suggest that TSPO may serve a range of functions that can be viewed as downstream regulatory effects of its primary, evolutionary conserved role in cell metabolism and energy production.

摘要

最近在组织特异性以及全身性Tspo(转位蛋白18 kDa)基因敲除小鼠中的功能丧失研究并未证实其长期以来被认为的对于胆固醇跨线粒体内膜间隙转运(类固醇生物合成中的限速步骤)不可或缺。相反,最近在全身性Tspo基因敲除小鼠中的研究表明,TSPO可能在细胞生物能量学中发挥更基本的作用,这可能包括对转运或代谢功能的间接下游调节。为了研究TSPO蛋白的过表达是否会改变细胞生物能量学特征,将内源性表达低或无表达的Jurkat细胞用TSPO构建体转染,以创建一个稳定的细胞系,使其从头表达外源性TSPO蛋白。通过RT-qPCR、用[3H]PK11195进行放射性配体结合以及用TSPO抗体进行免疫细胞化学来确认TSPO的表达。我们证明,TSPO基因插入会导致参与线粒体电子传递链的基因转录增加。此外,TSPO插入增加了线粒体ATP的产生以及细胞兴奋性,这反映在膜片钳记录的整流钾通道电流的减少上。这些功能变化伴随着细胞增殖和运动性的增加,而PK11195(一种TSPO的选择性配体)可抑制这些变化。我们认为,TSPO可能具有一系列功能,这些功能可被视为其在细胞代谢和能量产生中主要的、进化保守作用的下游调节效应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5643/5351937/14aa0ffbfab3/kccy-16-05-1281477-g001.jpg

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