Literature DB >> 30910814

Homotypic and heterotypic trans-assembly of human Rab-family small GTPases in reconstituted membrane tethering.

Kazuya Segawa1, Naoki Tamura1, Joji Mima2.   

Abstract

Membrane tethering is a highly regulated event occurring during the initial physical contact between membrane-bounded transport carriers and their target subcellular membrane compartments, thereby ensuring the spatiotemporal specificity of intracellular membrane trafficking. Although Rab-family small GTPases and specific Rab-interacting effectors, such as coiled-coil tethering proteins and multisubunit tethering complexes, are known to be involved in membrane tethering, how these protein components directly act upon the tethering event remains enigmatic. Here, using a chemically defined reconstitution system, we investigated the molecular basis of membrane tethering by comprehensively and quantitatively evaluating the intrinsic capacities of 10 representative human Rab-family proteins (Rab1a, -3a, -4a, -5a, -6a, -7a, -9a, -11a, -27a, and -33b) to physically tether two distinct membranes via homotypic and heterotypic Rab-Rab assembly. All of the Rabs tested, except Rab27a, specifically caused homotypic membrane tethering at physiologically relevant Rab densities on membrane surfaces (e.g. Rab/lipid molar ratios of 1:100-1:3,000). Notably, endosomal Rab5a retained its intrinsic potency to drive efficient homotypic tethering even at concentrations below the Rab/lipid ratio of 1:3,000. Comprehensive reconstitution experiments further uncovered that heterotypic combinations of human Rab-family isoforms, including Rab1a/6a, Rab1a/9a, and Rab1a/33b, can directly and selectively mediate membrane tethering. Rab1a and Rab9a in particular synergistically triggered very rapid and efficient membrane tethering reactions through their heterotypic trans-assembly on two opposing membranes. In conclusion, our findings establish that, in the physiological context, homotypic and heterotypic trans-assemblies of Rab-family small GTPases can provide the essential molecular machinery necessary to drive membrane tethering in eukaryotic endomembrane systems.
© 2019 Segawa et al.

Entities:  

Keywords:  RAB member RAS oncogene family; Rab; Ras superfamily; endomembrane system; liposome; membrane reconstitution; membrane tethering; membrane trafficking; small GTPase; transport vesicle

Mesh:

Substances:

Year:  2019        PMID: 30910814      PMCID: PMC6514636          DOI: 10.1074/jbc.RA119.007947

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  44 in total

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Journal:  Structure       Date:  2013-08-06       Impact factor: 5.006

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8.  Human Rab small GTPase- and class V myosin-mediated membrane tethering in a chemically defined reconstitution system.

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Journal:  J Biol Chem       Date:  2017-09-22       Impact factor: 5.157

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Journal:  Nucleic Acids Res       Date:  2016-11-29       Impact factor: 16.971

10.  An endosomal tether undergoes an entropic collapse to bring vesicles together.

Authors:  David H Murray; Marcus Jahnel; Janelle Lauer; Mario J Avellaneda; Nicolas Brouilly; Alice Cezanne; Hernán Morales-Navarrete; Enrico D Perini; Charles Ferguson; Andrei N Lupas; Yannis Kalaidzidis; Robert G Parton; Stephan W Grill; Marino Zerial
Journal:  Nature       Date:  2016-08-24       Impact factor: 49.962
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Review 5.  Rab family of small GTPases: an updated view on their regulation and functions.

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Journal:  FEBS J       Date:  2020-07-01       Impact factor: 5.542
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