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The full length of a mitochondrial presequence is required for efficient monolayer insertion and interbilayer contact formation.

作者信息

Leenhouts J M, Török Z, Demel R A, de Gier J, de Kruijff B

机构信息

Department of Biochemistry of Membranes, Utrecht University, The Netherlands.

出版信息

Mol Membr Biol. 1994 Jul-Sep;11(3):159-64. doi: 10.3109/09687689409162234.

DOI:10.3109/09687689409162234
PMID:7742880
Abstract

The peptide specificity of both presequence-monolayer interactions and the ability of presequences to induce interbilayer contacts between large unilamellar vesicles was investigated. A range of different synthetic peptides that are documented for their mitochondrial protein import abilities were used for this purpose. Both monolayer insertion and vesicle aggregation were found to be strongly dependent on the primary structure of the studied presequence peptides. The combination of monolayer data and results of vesicle aggregation experiments leads to the overall suggestion that monolayer insertion and interbilayer contact formation are mechanistically related. For maximal effects the full length of a presequence peptide is required. The cardiolipin specificity of presequence-induced interbilayer contact formation previously reported was found to be a more general property among presequence peptides. The peptide's ability to induce vesicle-vesicle contacts seems to parallel the efficiency of its import ability into mitochondria. These results lead to an extended hypothesis on the role of presequence-induced contact site formation during the mitochondrial protein import process.

摘要

相似文献

1
The full length of a mitochondrial presequence is required for efficient monolayer insertion and interbilayer contact formation.
Mol Membr Biol. 1994 Jul-Sep;11(3):159-64. doi: 10.3109/09687689409162234.
2
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Early events in the transport of proteins into mitochondria. Import competition by a mitochondrial presequence.蛋白质转运至线粒体的早期事件。线粒体前导序列的导入竞争。
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