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从 PEX3 与 PEX19 的可溶性片段复合物的结构中洞察过氧化物酶体的功能。

Insights into peroxisome function from the structure of PEX3 in complex with a soluble fragment of PEX19.

机构信息

Interfaculty Institute for Biochemistry, University of Tübingen, 72076 Tübingen, Germany.

出版信息

J Biol Chem. 2010 Aug 13;285(33):25410-7. doi: 10.1074/jbc.M110.138503. Epub 2010 Jun 16.

Abstract

The human peroxins PEX3 and PEX19 play a central role in peroxisomal membrane biogenesis. The membrane-anchored PEX3 serves as the receptor for cytosolic PEX19, which in turn recognizes newly synthesized peroxisomal membrane proteins. After delivering these proteins to the peroxisomal membrane, PEX19 is recycled to the cytosol. The molecular mechanisms underlying these processes are not well understood. Here, we report the crystal structure of the cytosolic domain of PEX3 in complex with a PEX19-derived peptide. PEX3 adopts a novel fold that is best described as a large helical bundle. A hydrophobic groove at the membrane-distal end of PEX3 engages the PEX19 peptide with nanomolar affinity. Mutagenesis experiments identify phenylalanine 29 in PEX19 as critical for this interaction. Because key PEX3 residues involved in complex formation are highly conserved across species, the observed binding mechanism is of general biological relevance.

摘要

人源过氧化物酶体生物发生蛋白 PEX3 和 PEX19 在过氧化物酶体膜生物发生中发挥核心作用。膜锚定蛋白 PEX3 作为胞质 PEX19 的受体,PEX19 反过来识别新合成的过氧化物酶体膜蛋白。将这些蛋白质递送到过氧化物酶体膜后,PEX19 被循环回细胞质。这些过程背后的分子机制尚不清楚。在这里,我们报告了与 PEX19 衍生肽复合物的胞质域的 PEX3 的晶体结构。PEX3 采用一种新颖的折叠结构,最好描述为一个大型螺旋束。PEX3 的膜远端末端的一个疏水性凹槽以纳摩尔亲和力与 PEX19 肽结合。突变实验确定 PEX19 中的苯丙氨酸 29 对这种相互作用至关重要。由于参与复合物形成的关键 PEX3 残基在物种间高度保守,因此观察到的结合机制具有普遍的生物学意义。

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