Distinct role of TGN-resident clathrin adaptors for Vps21p activation in the TGN–endosome trafficking pathway

Author:

Nagano Makoto1,Aoshima Kaito1,Shimamura Hiroki1,Siekhaus Daria Elisabeth2ORCID,Toshima Junko Y.3ORCID,Toshima Jiro1ORCID

Affiliation:

1. Tokyo University of Science 1 Department of Biological Science and Technology , , 6-3-1 Niijuku, Katsushika-ku, Tokyo 125-8585 , Japan

2. Institute of Science and Technology Austria 2 , Am Campus 1, A-3400 Klosterneuburg , Austria

3. School of Health Science, Tokyo University of Technology 3 , 5-23-22 Nishikamada, Ota-ku, Tokyo 144-8535 , Japan

Abstract

ABSTRACT Clathrin-mediated vesicle trafficking plays central roles in post-Golgi transport. In yeast (Saccharomyces cerevisiae), the AP-1 complex and GGA adaptors are predicted to generate distinct transport vesicles at the trans-Golgi network (TGN), and the epsin-related proteins Ent3p and Ent5p (collectively Ent3p/5p) act as accessories for these adaptors. Recently, we showed that vesicle transport from the TGN is crucial for yeast Rab5 (Vps21p)-mediated endosome formation, and that Ent3p/5p are crucial for this process, whereas AP-1 and GGA adaptors are dispensable. However, these observations were incompatible with previous studies showing that these adaptors are required for Ent3p/5p recruitment to the TGN, and thus the overall mechanism responsible for regulation of Vps21p activity remains ambiguous. Here, we investigated the functional relationships between clathrin adaptors in post-Golgi-mediated Vps21p activation. We show that AP-1 disruption in the ent3Δ5Δ mutant impaired transport of the Vps21p guanine nucleotide exchange factor Vps9p transport to the Vps21p compartment and severely reduced Vps21p activity. Additionally, GGA adaptors, the phosphatidylinositol-4-kinase Pik1p and Rab11 GTPases Ypt31p and Ypt32p were found to have partially overlapping functions for recruitment of AP-1 and Ent3p/5p to the TGN. These findings suggest a distinct role of clathrin adaptors for Vps21p activation in the TGN–endosome trafficking pathway.

Funder

Japan Society for the Promotion of Science

Takeda Science Foundation

Life Science Foundation of Japan

Publisher

The Company of Biologists

Subject

Cell Biology

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