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分泌小泡介导的细胞分裂需要中心粒蛋白将外泌体和SNARE复合体锚定在中体上。

Centriolin anchoring of exocyst and SNARE complexes at the midbody is required for secretory-vesicle-mediated abscission.

作者信息

Gromley Adam, Yeaman Charles, Rosa Jack, Redick Sambra, Chen Chun-Ting, Mirabelle Stephanie, Guha Minakshi, Sillibourne James, Doxsey Stephen J

机构信息

Program in Molecular Medicine, University of Massachusetts Medical Center, Worcester, Massachusetts 01605, USA.

出版信息

Cell. 2005 Oct 7;123(1):75-87. doi: 10.1016/j.cell.2005.07.027.

Abstract

The terminal step in cytokinesis, called abscission, requires resolution of the membrane connection between two prospective daughter cells. Our previous studies demonstrated that the coiled-coil protein centriolin localized to the midbody during cytokinesis and was required for abscission. Here we show that centriolin interacts with proteins of vesicle-targeting exocyst complexes and vesicle-fusion SNARE complexes. These complexes require centriolin for localization to a unique midbody-ring structure, and disruption of either complex inhibits abscission. Exocyst disruption induces accumulation of v-SNARE-containing vesicles at the midbody ring. In control cells, these v-SNARE vesicles colocalize with a GFP-tagged secreted polypeptide. The vesicles move to the midbody ring asymmetrically from one prospective daughter cell; the GFP signal is rapidly lost, suggesting membrane fusion; and subsequently the cell cleaves at the site of vesicle delivery/fusion. We propose that centriolin anchors protein complexes required for vesicle targeting and fusion and integrates membrane-vesicle fusion with abscission.

摘要

胞质分裂的最后一步称为切割,需要解决两个预期子细胞之间的膜连接问题。我们之前的研究表明,卷曲螺旋蛋白中心粒素在胞质分裂期间定位于中体,并且是切割所必需的。在这里,我们表明中心粒素与囊泡靶向外泌体复合物和囊泡融合SNARE复合物的蛋白质相互作用。这些复合物需要中心粒素才能定位于独特的中体环结构,并且任一复合物的破坏都会抑制切割。外泌体破坏会导致含v-SNARE的囊泡在中体环处积累。在对照细胞中,这些v-SNARE囊泡与绿色荧光蛋白标记的分泌多肽共定位。囊泡从一个预期子细胞不对称地移动到中体环;绿色荧光蛋白信号迅速消失,表明膜融合;随后细胞在囊泡递送/融合的部位分裂。我们提出,中心粒素锚定囊泡靶向和融合所需的蛋白质复合物,并将膜-囊泡融合与切割整合在一起。

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