The content of mitochondrial proteome is maintained through two highly dynamic processes, the influx of newly synthesized proteins from the cytosol and the protein degradation. Mitochondrial proteins are targeted to the intermembrane space by the mitochondrial intermembrane space assembly pathway that couples their import and oxidative folding. The folding trap was proposed to be a driving mechanism for the mitochondrial accumulation of these proteins. Whether the reverse movement of unfolded proteins to the cytosol occurs across the intact outer membrane is unknown. We found that reduced, conformationally destabilized proteins are released from mitochondria in a size-limited manner. We identified the general import pore protein Tom40 as an escape gate. We propose that the mitochondrial proteome is not only regulated by the import and degradation of proteins but also by their retro-translocation to the external cytosolic location. Thus, protein release is a mechanism that contributes to the mitochondrial proteome surveillance.
Retro-translocation of mitochondrial intermembrane space proteins.
线粒体膜间隙蛋白的逆向转位
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作者:Bragoszewski Piotr, Wasilewski Michal, Sakowska Paulina, Gornicka Agnieszka, Böttinger Lena, Qiu Jian, Wiedemann Nils, Chacinska Agnieszka
| 期刊: | Proceedings of the National Academy of Sciences of the United States of America | 影响因子: | 9.100 |
| 时间: | 2015 | 起止号: | 2015 Jun 23; 112(25):7713-8 |
| doi: | 10.1073/pnas.1504615112 | 研究方向: | 免疫/内分泌 |
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