Abstract
The guided entry of tail-anchored protein (GET) pathway, in which the Get3 ATPase delivers an essential class of tail-anchored membrane proteins (TAs) to the Get1/2 receptor at the endoplasmic reticulum, provides a conserved mechanism for TA biogenesis in eukaryotic cells. The membrane-associated events of this pathway remain poorly understood. Here we show that complex assembly between the cytosolic domains (CDs) of Get1 and Get2 strongly enhances the affinity of the individual subunits for Get3•TA, thus enabling efficient capture of the targeting complex. In addition to the known role of Get1CD in remodeling Get3 conformation, two molecular recognition features (MoRFs) in Get2CD induce Get3 opening, and both subunits are required for optimal TA release from Get3. Mutation of the MoRFs attenuates TA insertion into the ER in vivo. Our results demonstrate extensive cooperation between the Get1/2 receptor subunits in the capture and remodeling of the targeting complex, and emphasize the role of MoRFs in receptor function during membrane protein biogenesis.
Original language | English |
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Article number | e202103079 |
Journal | Journal of Cell Biology |
Volume | 220 |
Issue number | 11 |
DOIs | |
State | Published - 1 Nov 2021 |
Bibliographical note
Publisher Copyright:© 2021 Chio et al.
Funding
This work was supported by Dean Willard Chair funds to S. Weiss and National Institutes of Health grants R01 GM107368 and R35 GM136321 and the Gordon and Betty Moore Foundation grant GBMF2939 to S.-o. Shan. The authors declare no competing financial interests.
Funders | Funder number |
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National Institutes of Health | R01 GM107368 |
National Institute of General Medical Sciences | R35GM136321 |
Gordon and Betty Moore Foundation | GBMF2939 |