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小窝蛋白21(VIP21-caveolin)是小窝衣被的一种膜蛋白成分,在体内和体外都会发生寡聚化。

VIP21-caveolin, a membrane protein constituent of the caveolar coat, oligomerizes in vivo and in vitro.

作者信息

Monier S, Parton R G, Vogel F, Behlke J, Henske A, Kurzchalia T V

机构信息

Department of Cell Biology, Max-Delbrück Centre for Molecular Medicine, Berlin-Buch, Germany.

出版信息

Mol Biol Cell. 1995 Jul;6(7):911-27. doi: 10.1091/mbc.6.7.911.

Abstract

VIP21-caveolin is a membrane protein, proposed to be a component of the striated coat covering the cytoplasmic surface of caveolae. To investigate the biochemical composition of the caveolar coat, we used our previous observation that VIP21-caveolin is present in large complexes and insoluble in the detergents CHAPS or Triton X-114. The mild treatment of these insoluble structures with sodium dodecyl sulfate leads to the detection of high molecular mass complexes of approximately 200, 400, and 600 kDa. The 400-kDa complex purified to homogeneity from dog lung is shown to consist exclusive of the two isoforms of VIP21-caveolin. Pulse-chase experiments indicate that the oligomers form early after the protein is synthesized in the endoplasmic reticulum (ER). VIP21-caveolin does indeed insert into the ER membrane through the classical translocation machinery. Its hydrophobic domain adopts an unusual loop configuration exposing the N- and C-flanking regions to the cytoplasm. Similar high molecular mass complexes can be produced from the in vitro-synthesized VIP21-caveolin. The complex formation occurs only if VIP21-caveolin isoforms are properly inserted into the membrane; formation is cytosol-dependent and does not involve a vesicle fusion step. We propose that high molecular mass oligomers of VIP21-caveolin represent the basic units forming the caveolar coat. They are formed in the ER and later, between the ER and the plasma membrane, these oligomers could associate into larger detergent-insoluble structures.

摘要

小窝蛋白21(VIP21-caveolin)是一种膜蛋白,被认为是覆盖小窝细胞质表面的条纹状衣被的组成成分。为了研究小窝衣被的生化组成,我们利用了之前的观察结果,即VIP21-caveolin存在于大的复合物中,并且不溶于去污剂CHAPS或 Triton X-114。用十二烷基硫酸钠对这些不溶性结构进行温和处理,可检测到大约200、400和600 kDa的高分子量复合物。从狗肺中纯化至同质的400 kDa复合物被证明仅由VIP21-caveolin的两种同工型组成。脉冲追踪实验表明,寡聚体在蛋白质在内质网(ER)中合成后不久就形成了。VIP21-caveolin确实通过经典的转运机制插入到ER膜中。其疏水结构域采用了一种不寻常的环构型,使N端和C端侧翼区域暴露于细胞质中。类似的高分子量复合物也可以由体外合成的VIP21-caveolin产生。只有当VIP21-caveolin同工型正确插入膜中时才会发生复合物形成;形成过程依赖于细胞质,并且不涉及囊泡融合步骤。我们提出,VIP21-caveolin的高分子量寡聚体代表了形成小窝衣被的基本单位。它们在内质网中形成,随后,在内质网和质膜之间,这些寡聚体可以结合形成更大的不溶于去污剂的结构。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c87e/301248/22dc2ec79242/mbc00076-0158-a.jpg

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