Single p197 molecules of the mitochondrial genome segregation system of Trypanosoma brucei determine the distance between basal body and outer membrane

Author:

Aeschlimann Salome12ORCID,Kalichava Ana23ORCID,Schimanski Bernd1ORCID,Berger Bianca Manuela23ORCID,Jetishi Clirim23ORCID,Stettler Philip12ORCID,Ochsenreiter Torsten3ORCID,Schneider André1ORCID

Affiliation:

1. Department of Chemistry, Biochemistry, and Pharmaceutical Sciences, University of Bern, Bern CH-3012, Switzerland

2. Graduate School for Cellular and Biomedical Sciences, University of Bern, Bern CH-3012, Switzerland

3. Institute of Cell Biology, University of Bern, Bern CH-3012, Switzerland

Abstract

The tripartite attachment complex (TAC) couples the segregation of the single unit mitochondrial DNA of trypanosomes with the basal body (BB) of the flagellum. Here, we studied the architecture of the exclusion zone filament (EZF) of the TAC, the only known component of which is p197, that connects the BB with the mitochondrial outer membrane (OM). We show that p197 has three domains that are all essential for mitochondrial DNA inheritance. The C terminus of p197 interacts with the mature and probasal body (pro-BB), whereas its N terminus binds to the peripheral OM protein TAC65. The large central region of p197 has a high α-helical content and likely acts as a flexible spacer. Ultrastructure expansion microscopy (U-ExM) of cell lines exclusively expressing p197 versions of different lengths that contain both N- and C-terminal epitope tags demonstrates that full-length p197 alone can bridge the ∼270-nm distance between the BB and the cytosolic face of the OM. Thus U-ExM allows the localization of distinct domains within the same molecules and suggests that p197 is the TAC subunit most proximal to the BB. In addition, U-ExM revealed that p197 acts as a spacer molecule, as two shorter versions of p197, with the repeat domain either removed or replaced by the central domain of the Trypanosoma cruzi p197 ortholog reduced the distance between the BB and the OM in proportion to their predicted molecular weight.

Funder

NCCR RNA & Disease a National Center of Competence in Research

Swiss National Science Foundation

Uniscientia Foundation

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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