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Two independent pathways traffic the interperoxisomal peroxin PpPex8p into peroxisomes: Mechanism and evolutionary implications

机译:过氧化物酶体间过氧化物酶PpPex8p进入过氧化物酶体的两个独立途径:机制和进化意义

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Among peroxins involved in peroxisome biogenesis, only Pex8p is predominantly intraperoxisomal at steady state. Pex8p is necessary for peroxisomal matrix protein import via the PTS1 and PTS2 pathways. It is proposed to bridge two peroxisomal membrane subcomplexes comprised of the docking (Pex13p, Pex14p, Pex17p) and RING (Pex2p, Pex10p, Pex12p) peroxins and is also implicated in cargo release of PTS1 proteins in the matrix. We show that Pichia pastoris Pex8p (PpPex8p) enters the peroxisome matrix using two redundant pathways in a Pex14p-dependent, but Pex2p-independent, manner, showing that the intact importomer and RING subcomplex are not required for its import. One pathway depends on the TPR motifs in Pex5p, the C-terminal PTS1 sequence (AKL) in PpPex8p, and the intraperoxisomal presence of this peroxin. The alternative pathway uses the PTS2 receptor, Pex7p, its accessory protein, Pex20p, and a putative PTS2 motif in PpPex8p, but does not require intraperoxisomal PpPex8p. Pex20p interaction with PpPex8p is independent of Pex7p, but the interaction of PpPex8p with Pex7p requires Pex20p. These data suggest a direct interaction between PpPex8p and Pex20p. Our studies shed light on the mechanism and evolution of the dual import pathways for PpPex8p.
机译:在与过氧化物酶体生物发生有关的过氧化物酶中,只有Pex8p在稳态下主要为过氧化物酶体内。 Pex8p对于通过PTS1和PTS2途径导入过氧化物酶体基质蛋白是必需的。提议桥接由过氧化物(Pex13p,Pex14p,Pex17p)和RING(Pex2p,Pex10p,Pex12p)过氧化物组成的两个过氧化物酶体膜亚复合物,并且还涉及基质中PTS1蛋白的货物释放。我们显示巴斯德毕赤酵母Pex8p(PpPex8p)使用两个冗余途径以Pex14p依赖但不依赖Pex2p的方式进入过氧化物酶体基质,表明完整的importomer和RING亚复合体对其导入并不需要。一种途径取决于Pex5p中的TPR基序,PpPex8p中的C末端PTS1序列(AKL)以及该过氧化物酶的过氧化物酶体内存在。替代途径使用PTS2受体Pex7p,其辅助蛋白Pex20p和PpPex8p中的推定PTS2基序,但不需要过氧化物酶体内PpPex8p。 Pex20p与PpPex8p的交互独立于Pex7p,但是PpPex8p与Pex7p的交互需要Pex20p。这些数据表明PpPex8p和Pex20p之间存在直接的相互作用。我们的研究揭示了PpPex8p双重导入途径的机制和进化。

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