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- W3037308384 abstract "Mitochondrial biogenesis requires efficient sorting of various proteins into different mitochondrial sub-compartments mediated by dedicated protein machinery present in the outer and inner membrane. Among them, the TIM22 complex enables the integration of complex membrane proteins with internal targeting signals into the inner membrane. Although the Tim22 forms the core of the complex, the dynamic recruitment of subunits to the channel is still enigmatic. The present study first-time highlights that IMS and TM4 regions of Tim22 are critically required for the interaction of the membrane-embedded subunits including, Tim54, Tim18, and Sdh3, thereby maintain the functional architecture of TIM22 translocase. On the other hand, TM1 and TM2 regions of Tim22 are important for the Tim18 association, while TM3 is exclusively required for the Sdh3 interaction. Moreover, the impairment in TIM22 complex assembly influences its translocase activity, mitochondrial network, and the viability of cells lacking mitochondrial DNA. Overall our findings provide compelling evidence to highlight the significance of conserved regions of Tim22 that are important for the maintenance of the TIM22 complex and mitochondrial integrity." @default.
- W3037308384 created "2020-07-02" @default.
- W3037308384 creator A5016194841 @default.
- W3037308384 creator A5032583699 @default.
- W3037308384 creator A5066113590 @default.
- W3037308384 date "2020-01-01" @default.
- W3037308384 modified "2023-09-23" @default.
- W3037308384 title "Role of conserved regions of Tim22 in the structural organization of the carrier translocase" @default.
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- W3037308384 doi "https://doi.org/10.1242/jcs.244632" @default.
- W3037308384 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/34005247" @default.
- W3037308384 hasPublicationYear "2020" @default.
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