4.8 Article

Autoinhibition and regulation by phosphoinositides of ATP8B1, a human lipid flippase associated with intrahepatic cholestatic disorders

ELIFE (2022)

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Journal

ELIFE
Volume 11, Issue -, Pages -

Publisher

eLIFE SCIENCES PUBL LTD
DOI: 10.7554/eLife.75272

Keywords

lipid flippase; autoinhibition; phosphoinositides; P4-ATPases; progressive familial intrahepatic cholestasis; Cryo-EM; S; cerevisiae

Categories

Biology

Funding

  1. EMBO [5072-00025B]
  2. French Infrastructure for Integrated Structural Biology [7881]
  3. French Ministry for Higher Education
  4. European Commission
  5. Agence Nationale de la Recherche [FRISBI ANR-10-INSB-05]
  6. Lundbeckfonden
  7. Deutsche Forschungsgemeinschaft [ANR-14-CE09-0022]
  8. Danish Agency for Science and Higher Education [GU 1133/11-1]
  9. Agence Nationale de la Recherche (ANR) [ANR-14-CE09-0022] Funding Source: Agence Nationale de la Recherche (ANR)

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Research reveals that the human lipid flippase ATP8B1-CDC50A is autoinhibited by its N- and C-terminal tails, and ATP hydrolysis is unleashed by truncation of the C-terminus. However, it also requires phosphoinositides for full activation. Restoring inhibition of ATP8B1 truncation constructs with a synthetic peptide suggests molecular communication between the N- and C-termini and interference with the regulatory mechanism by exogenous compounds.
P4-ATPases flip lipids from the exoplasmic to the cytosolic leaflet, thus maintaining lipid asymmetry in eukaryotic cell membranes. Mutations in several human P4-ATPase genes are associated with severe diseases, for example in ATP8B1 causing progressive familial intrahepatic cholestasis, a rare inherited disorder progressing toward liver failure. ATP8B1 forms a binary complex with CDC50A and displays a broad specificity to glycerophospholipids, but regulatory mechanisms are unknown. Here, we report functional studies and the cryo-EM structure of the human lipid flippase ATP8B1-CDC50A at 3.1 & ANGS; resolution. We find that ATP8B1 is autoinhibited by its N- and C-terminal tails, which form extensive interactions with the catalytic sites and flexible domain interfaces. Consistently, ATP hydrolysis is unleashed by truncation of the C-terminus, but also requires phosphoinositides, most markedly phosphatidylinositol-3,4,5-phosphate (PI(3,4,5)P-3), and removal of both N- and C-termini results in full activation. Restored inhibition of ATP8B1 truncation constructs with a synthetic peptide mimicking the C-terminal segment further suggests molecular communication between N- and C-termini in the autoinhibition and demonstrates that the regulatory mechanism can be interfered with by exogenous compounds. A recurring (G/A)(Y/F)AFS motif of the C-terminal segment suggests that this mechanism is employed widely across P4-ATPase lipid flippases in plasma membrane and endomembranes.

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