Tom70 enhances mitochondrial preprotein import efficiency by binding to internal targeting sequences

Author:

Backes Sandra1ORCID,Hess Steffen1,Boos Felix1,Woellhaf Michael W.1,Gödel Sabrina2ORCID,Jung Martin3ORCID,Mühlhaus Timo2ORCID,Herrmann Johannes M.1ORCID

Affiliation:

1. Cell Biology, University of Kaiserslautern, Kaiserslautern, Germany

2. Computational Systems Biology, University of Kaiserslautern, Kaiserslautern, Germany

3. Medical Biochemistry, Saarland University, Homburg, Germany

Abstract

The biogenesis of mitochondria depends on the import of hundreds of preproteins. N-terminal matrix-targeting signals (MTSs) direct preproteins to the surface receptors Tom20, Tom22, and Tom70. In this study, we show that many preproteins contain additional internal MTS-like signals (iMTS-Ls) in their mature region that share the characteristic properties of presequences. These features allow the in silico prediction of iMTS-Ls. Using Atp1 as model substrate, we show that iMTS-Ls mediate the binding to Tom70 and have the potential to target the protein to mitochondria if they are presented at its N terminus. The import of preproteins with high iMTS-L content is significantly impaired in the absence of Tom70, whereas preproteins with low iMTS-L scores are less dependent on Tom70. We propose a stepping stone model according to which the Tom70-mediated interaction with internal binding sites improves the import competence of preproteins and increases the efficiency of their translocation into the mitochondrial matrix.

Funder

Deutsche Forschungsgemeinschaft

Publisher

Rockefeller University Press

Subject

Cell Biology

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