International Journal of Molecular Sciences (Jan 2024)

Unique Interactions of the Small Translocases of the Mitochondrial Inner Membrane (Tims) in <i>Trypanosoma brucei</i>

  • Linda S. Quiñones,
  • Fidel Soto Gonzalez,
  • Chauncey Darden,
  • Muhammad Khan,
  • Anuj Tripathi,
  • Joseph T. Smith,
  • Jamaine Davis,
  • Smita Misra,
  • Minu Chaudhuri

DOI
https://doi.org/10.3390/ijms25031415
Journal volume & issue
Vol. 25, no. 3
p. 1415

Abstract

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The infectious agent for African trypanosomiasis, Trypanosoma brucei, possesses a unique and essential translocase of the mitochondrial inner membrane, known as the TbTIM17 complex. TbTim17 associates with six small TbTims (TbTim9, TbTim10, TbTim11, TbTim12, TbTim13, and TbTim8/13). However, the interaction patterns of these smaller TbTims with each other and TbTim17 are not clear. Through yeast two-hybrid (Y2H) and co-immunoprecipitation analyses, we demonstrate that all six small TbTims interact with each other. Stronger interactions were found among TbTim8/13, TbTim9, and TbTim10. However, TbTim10 shows weaker associations with TbTim13, which has a stronger connection with TbTim17. Each of the small TbTims also interacts strongly with the C-terminal region of TbTim17. RNAi studies indicated that among all small TbTims, TbTim13 is most crucial for maintaining the steady-state levels of the TbTIM17 complex. Further analysis of the small TbTim complexes by size exclusion chromatography revealed that each small TbTim, except for TbTim13, is present in ~70 kDa complexes, possibly existing in heterohexameric forms. In contrast, TbTim13 is primarily present in the larger complex (>800 kDa) and co-fractionates with TbTim17. Altogether, our results demonstrate that, relative to other eukaryotes, the architecture and function of the small TbTim complexes are specific to T. brucei.

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