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An ATP13A1-assisted topogenesis pathway for folding multi-spanning membrane proteins

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NIAID Data Ecosystem2026-05-01 收录
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Many multi-spanning membrane proteins contain poorly hydrophobic transmembrane domains (pTMDs) protected from phospholipid in mature structure. Nascent pTMDs are difficult for translocon to recognize and insert. How pTMDs are discerned and packed into mature, muti-spanning configuration remains unclear. Here, we report that pTMD elicits a post-translational topogenesis pathway for its recognition and integration. Using six-spanning membrane protein ABC transporter G2 (ABCG2) and cultured human cells as models, we show that its pTMD2 can pass through translocon into the ER lumen, yielding an intermediate with inserted yet mis-oriented downstream TMDs. After translation, the intermediate recruits P5A-ATPase ATP13A1, which facilitates TMD re-orientation, allowing further folding and the integration of the remaining lumen-exposed pTMD2. Depleting ATP13A1 or disrupting pTMD-characteristic residues arrests intermediates with mis-oriented and exposed TMDs. Our results explain how a “difficult” pTMD is co-translationally skipped for insertion and post-translationally buried into final correct structure at the late stage of folding to avoid excessive lipid-exposure.
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2024-04-29
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