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Mechanistic Bases for Privileged Capture and Unidirectional Targeting of Tail-Anchored Proteins by the Get3 ATPase

CALIFORNIA INSTITUTE OF TECHNOLOGY. 2019; 
Chio, Un Seng
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Proteins, Expression, Isolation and Analysis Clarified lysates of the cells from the same cultures in (B) were diluted with SDS sample buffer and immunoblotted against an anti-FLAG antibody (GenScript; top) to determine the steady-state Get3 levels in the different yeast strains. Get A Quote

摘要

C-terminal tail-anchored membrane proteins (TAs) are targeted post-translationally to the endoplasmic reticulum (ER) in eukaryotic cells mainly through the Guided entry of tail-anchored protein (GET) pathway. Here we use biochemical and biophysical approaches to shed further mechanistic insight into how the central chaperone, the Get3 ATPase, is able to capture TA substrates in a privileged manner and provide unidirectional targeting to the ER. Specifically, we first show in Chapter 2 that Get3 dynamically samples open and closed conformations as a "protean clamp". Binding of TA substrates induces Get3 to sample more open conformations that causes Get3 to dissociate from the cytosolic regulatory Get4/5 complex,... More

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