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Structural insights into the activation of autoinhibited human lipid flippase ATP8B1 upon substrate binding

Meng‐Ting Cheng, Yu Chen, Zhipeng Chen, Xin Liu, Zhiyong Zhang, Yuxing Chen, Wen‐Tao Hou, Cong‐Zhao Zhou

2022Proceedings of the National Academy of Sciences34 citationsDOIOpen Access PDF

Abstract

SignificanceATP8B1 is a P4 ATPase that maintains membrane asymmetry by transporting phospholipids across the cell membrane. Disturbance of lipid asymmetry will lead to the imbalance of the cell membrane and eventually, cell death. Thus, defects in ATP8B1 are usually associated with severe human diseases, such as intrahepatic cholestasis. The present structures of ATP8B1 complexed with its auxiliary noncatalytic partners CDC50A and CDC50B reveal an autoinhibited state of ATP8B1 that could be released upon substrate binding. Moreover, release of this autoinhibition could be facilitated by the bile acids, which are key factors that alter the membrane asymmetry of hepatocytes. This enabled us to figure out a feedback loop of bile acids and lipids across the cell membrane.

Topics & Concepts

MembraneSubstrate (aquarium)ChemistryFlippaseCell membranePhospholipid scramblaseCell biologyCellATPaseBiochemistryBiophysicsEnzymeBiologyPhospholipidPhosphatidylserineEcologyATP Synthase and ATPases ResearchDrug Transport and Resistance MechanismsLipid Membrane Structure and Behavior
Structural insights into the activation of autoinhibited human lipid flippase ATP8B1 upon substrate binding | Litcius