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TRAPP亚基TPC6的结构提示了一种TRAPP亚复合物模型。

The structure of the TRAPP subunit TPC6 suggests a model for a TRAPP subcomplex.

作者信息

Kümmel Daniel, Müller Jürgen J, Roske Yvette, Misselwitz Rolf, Büssow Konrad, Heinemann Udo

机构信息

Max-Delbrück Center for Molecular Medicine, Berlin, Germany.

出版信息

EMBO Rep. 2005 Aug;6(8):787-93. doi: 10.1038/sj.embor.7400463.

Abstract

The TRAPP (transport protein particle) complexes are tethering complexes that have an important role at the different steps of vesicle transport. Recently, the crystal structures of the TRAPP subunits SEDL and BET3 have been determined, and we present here the 1.7 Angstroms crystal structure of human TPC6, a third TRAPP subunit. The protein adopts an alpha/beta-plait topology and forms a dimer. In spite of low sequence similarity, the structure of TPC6 strikingly resembles that of BET3. The similarity is especially prominent at the dimerization interfaces of the proteins. This suggests heterodimerization of TPC6 and BET3, which is shown by in vitro and in vivo association studies. Together with TPC5, another TRAPP subunit, TPC6 and BET3 are supposed to constitute a family of paralogous proteins with closely similar three-dimensional structures but little sequence similarity among its members.

摘要

TRAPP(转运蛋白颗粒)复合物是在囊泡运输的不同步骤中起重要作用的拴系复合物。最近,已确定了TRAPP亚基SEDL和BET3的晶体结构,在此我们展示人TPC6(TRAPP的第三个亚基)的1.7埃晶体结构。该蛋白采用α/β-褶拓扑结构并形成二聚体。尽管序列相似性较低,但TPC6的结构与BET3的结构惊人地相似。这种相似性在蛋白质的二聚化界面处尤为突出。这表明TPC6和BET3会形成异源二聚体,体外和体内结合研究都证实了这一点。TPC6与另一个TRAPP亚基TPC5以及BET3一起,被认为构成了一个旁系同源蛋白家族,其成员具有非常相似的三维结构,但序列相似性较低。

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