Fast-evolving cofactors regulate the role of HEATR5 complexes in intra-Golgi trafficking

Author:

Marmorale Lucas J.1ORCID,Jin Huan1ORCID,Reidy Thomas G.1ORCID,Palomino-Alonso Brandon1ORCID,Zysnarski Christopher J.1ORCID,Jordan-Javed Fatima1ORCID,Lahiri Sagar1ORCID,Duncan Mara C.1ORCID

Affiliation:

1. University of Michigan, Ann Arbor 1 Department of Cell and Developmental Biology, , Ann Arbor, MI, USA

Abstract

The highly conserved HEATR5 proteins are best known for their roles in membrane traffic mediated by the adaptor protein complex-1 (AP1). HEATR5 proteins rely on fast-evolving cofactors to bind to AP1. However, how HEATR5 proteins interact with these cofactors is unknown. Here, we report that the budding yeast HEATR5 protein, Laa1, functions in two biochemically distinct complexes. These complexes are defined by a pair of mutually exclusive Laa1-binding proteins, Laa2 and the previously uncharacterized Lft1/Yml037c. Despite limited sequence similarity, biochemical analysis and structure predictions indicate that Lft1 and Laa2 bind Laa1 via structurally similar mechanisms. Both Laa1 complexes function in intra-Golgi recycling. However, only the Laa2–Laa1 complex binds to AP1 and contributes to its localization. Finally, structure predictions indicate that human HEATR5 proteins bind to a pair of fast-evolving interacting partners via a mechanism similar to that observed in yeast. These results reveal mechanistic insight into how HEATR5 proteins bind their cofactors and indicate that Laa1 performs functions besides recruiting AP1.

Funder

National Institutes of Health

Office of Cyber Infrastructure and Computational Biology, National Institute of Allergy and Infectious Diseases

Publisher

Rockefeller University Press

Subject

Cell Biology

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