AI Article Synopsis
- Fis1, a protein in yeast, is known for recruiting Dnm1, which regulates mitochondrial fission, but its role in mammals is less clear as it seems unnecessary for Drp1 recruitment.
- Researchers found that TBC1D15 binds to Fis1 in HeLa cells and forms a stable complex, while Drp1 does not interact with Fis1.
- The study shows that knockdown of TBC1D15 leads to abnormal mitochondrial shapes, similar to Fis1 knockdown, indicating that both proteins work together to regulate mitochondrial morphology in mammals independently of Drp1.
Article Abstract
In yeast, C-tail-anchored mitochondrial outer membrane protein Fis1 recruits the mitochondrial-fission-regulating GTPase Dnm1 to mitochondrial fission sites. However, the function of its mammalian homologue remains enigmatic because it has been reported to be dispensable for the mitochondrial recruitment of Drp1, a mammalian homologue of Dnm1. We identified TBC1D15 as a Fis1-binding protein in HeLa cell extracts. Immunoprecipitation revealed that Fis1 efficiently interacts with TBC1D15 but not with Drp1. Bacterially expressed Fis1 and TBC1D15 formed a direct and stable complex. Exogenously expressed TBC1D15 localized mainly in cytoplasm in HeLa cells, but when coexpressed with Fis1 it localized to mitochondria. Knockdown of TBC1D15 induced highly developed mitochondrial network structures similar to the effect of Fis1 knockdown, suggesting that the TBC1D15 and Fis1 are associated with the regulation of mitochondrial morphology independently of Drp1. These data suggest that Fis1 acts as a mitochondrial receptor in the recruitment of mitochondrial morphology protein in mammalian cells.
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| http://dx.doi.org/10.1242/jcs.111211 | DOI Listing |
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