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含有氨基末端嵌合信号的细胞色素P450蛋白的线粒体靶向涉及一种不寻常的TOM20/TOM22旁路机制。

Mitochondrial targeting of cytochrome P450 proteins containing NH2-terminal chimeric signals involves an unusual TOM20/TOM22 bypass mechanism.

作者信息

Anandatheerthavarada Hindupur K, Sepuri Naresh Babu V, Avadhani Narayan G

机构信息

From the Department of Animal Biology and the Mari Lowe Center for Comparative Oncology, School of Veterinary Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104.

From the Department of Animal Biology and the Mari Lowe Center for Comparative Oncology, School of Veterinary Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104.

出版信息

J Biol Chem. 2009 Jun 19;284(25):17352-17363. doi: 10.1074/jbc.M109.007492. Epub 2009 Apr 28.

Abstract

Previously we showed that xenobiotic inducible cytochrome P450 (CYP) proteins are bimodally targeted to the endoplasmic reticulum and mitochondria. In this study, we investigated the mechanism of delivery of chimeric signal containing CYP proteins to the peripheral and channel-forming mitochondrial outer membrane translocases (TOMs). CYP+33/1A1 and CYP2B1 did not require peripheral TOM70, TOM20, or TOM22 for translocation through the channel-forming TOM40 protein. In contrast, CYP+5/1A1 and CYP2E1 were able to bypass TOM20 and TOM22 but required TOM70. CYP27, which contains a canonical cleavable mitochondrial signal, required all of the peripheral TOMs for its mitochondrial translocation. We investigated the underlying mechanisms of bypass of peripheral TOMs by CYPs with chimeric signals. The results suggested that interaction of CYPs with Hsp70, a cytosolic chaperone involved in the mitochondrial import, alone was sufficient for the recognition of chimeric signals by peripheral TOMs. However, sequential interaction of chimeric signal containing CYPs with Hsp70 and Hsp90 resulted in the bypass of peripheral TOMs, whereas CYP27A1 interacted only with Hsp70 and was not able to bypass peripheral TOMs. Our results also show that delivery of a chimeric signal containing client protein by Hsp90 required the cytosol-exposed NH(2)-terminal 143 amino acids of TOM40. TOM40 devoid of this domain was unable to import CYP proteins. These results suggest that compared with the unimodal mitochondrial targeting signals, the chimeric mitochondrial targeting signals are highly evolved and dynamic in nature.

摘要

此前我们发现,外源性诱导细胞色素P450(CYP)蛋白以双峰形式靶向内质网和线粒体。在本研究中,我们探究了含有CYP蛋白的嵌合信号传递至外周及形成通道的线粒体外膜转位酶(TOM)的机制。CYP+33/1A1和CYP2B1通过形成通道的TOM40蛋白进行转位时,不需要外周TOM70、TOM20或TOM22。相比之下,CYP+5/1A1和CYP2E1能够绕过TOM20和TOM22,但需要TOM70。含有典型可裂解线粒体信号的CYP27,其线粒体转位需要所有外周TOM。我们研究了具有嵌合信号的CYPs绕过外周TOM的潜在机制。结果表明,CYPs与参与线粒体导入的胞质伴侣Hsp70的相互作用, alone足以让外周TOM识别嵌合信号。然而,含有嵌合信号的CYPs与Hsp70和Hsp90的顺序相互作用导致绕过外周TOM,而CYP27A1仅与Hsp70相互作用,无法绕过外周TOM。我们的结果还表明,Hsp90传递含有客户蛋白的嵌合信号需要TOM40胞质暴露的NH(2)末端143个氨基酸。缺乏该结构域的TOM40无法导入CYP蛋白。这些结果表明,与单峰线粒体靶向信号相比,嵌合线粒体靶向信号在本质上高度进化且具有动态性。 (注:原文中“alone”一词在此处似乎表意不明,可能影响准确理解,按照字面意思翻译为“单独地”或“仅”,但结合语境不太能清晰其确切含义。)

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