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补体触发Mortalin/GRP75从线粒体重新定位到质膜。

Complement triggers relocation of Mortalin/GRP75 from mitochondria to the plasma membrane.

作者信息

Mazkereth Niv, Rocca Francesco, Schubert Jennifer-Rose, Geisler Claudia, Hillman Yaron, Egner Alexander, Fishelson Zvi

机构信息

Department of Cell and Developmental Biology, Sackler School of Medicine, Tel Aviv University, Tel Aviv 69978, Israel.

Optical Nanoscopy, Laser-Laboratorium Göttingen e.V., D-37077 Göttingen, Germany.

出版信息

Immunobiology. 2016 Dec;221(12):1395-1406. doi: 10.1016/j.imbio.2016.07.005. Epub 2016 Jul 21.

DOI:10.1016/j.imbio.2016.07.005
PMID:27475989
Abstract

Mortalin/GRP75 is a ubiquitously expressed mitochondrial chaperon that is overexpressed in cancer. Mortalin protects cells from complement-dependent cytotoxicity (CDC) and facilitates elimination of the complement C5b-9 complexes from the cell surface. We performed a nanoscopical study aimed at imaging the distribution of the C5b-9 complexes in the plasma membrane and the postulated relocation of mortalin from the mitochondria to the plasma membrane. To gain a resolution of 35nm, the locations of the C5b-9 complex and mortalin were imaged with a STED (Stimulated Emission Depletion) microscope at sub-diffraction resolution. Early changes in the spatial distribution of the C5b-9 on the cell surface are described. Juxtaposition of the labeled mortalin and C5b-9 at the plasma membrane region within minutes after complement attack is evident. Microscopical analysis of the distribution of mortalin in the vicinity of the mitochondria of complement-treated cells shows a more diffused pattern relative to control cells, proposing exit of mortalin from the mitochondria in response to complement-induced stress. In support, analysis of cytoplasmic mortalin by immunoblotting shows enhanced level of mortalin in the cytoplasm in complement-treated cells. Our data demonstrates that cells can sense complement activation at the plasma membrane and in response, swiftly send mortalin to this region in order to deactivate it.

摘要

Mortalin/GRP75是一种在全身广泛表达的线粒体伴侣蛋白,在癌症中过表达。Mortalin可保护细胞免受补体依赖性细胞毒性(CDC)的影响,并促进从细胞表面清除补体C5b-9复合物。我们进行了一项纳米显微镜研究,旨在对质膜中C5b-9复合物的分布以及Mortalin从线粒体到质膜的假定重新定位进行成像。为了获得35nm的分辨率,使用受激发射损耗(STED)显微镜以亚衍射分辨率对C5b-9复合物和Mortalin的位置进行成像。描述了细胞表面C5b-9空间分布的早期变化。补体攻击后几分钟内,标记的Mortalin和C5b-9在质膜区域并列是明显的。对补体处理细胞线粒体附近的Mortalin分布进行显微镜分析,结果显示相对于对照细胞,其分布模式更为分散,这表明Mortalin因补体诱导的应激而从线粒体中逸出。作为支持,通过免疫印迹对细胞质中的Mortalin进行分析,结果显示补体处理细胞的细胞质中Mortalin水平升高。我们的数据表明,细胞可以感知质膜上的补体激活,并作为响应迅速将Mortalin输送到该区域以使其失活。

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Complement triggers relocation of Mortalin/GRP75 from mitochondria to the plasma membrane.补体触发Mortalin/GRP75从线粒体重新定位到质膜。
Immunobiology. 2016 Dec;221(12):1395-1406. doi: 10.1016/j.imbio.2016.07.005. Epub 2016 Jul 21.
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