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Phosphorylation-dependent pseudokinase domain dimerization drives full-length MLKL oligomerization

Yanxiang Meng, Sarah E. Garnish, Katherine A. Davies, Katrina A. Black, Andrew Leis, Christopher R. Horne, Joanne M. Hildebrand, Hanadi Hoblos, Cheree Fitzgibbon, Samuel N. Young, Toby A. Dite, Laura F. Dagley, Aarya Venkat, Natarajan Kannan, Akiko Koide, Shohei Koide, Alisa Glukhova, Peter E. Czabotar, James M. Murphy

2023Nature Communications36 citationsDOIOpen Access PDF

Abstract

The necroptosis pathway is a lytic, pro-inflammatory mode of cell death that is widely implicated in human disease, including renal, pulmonary, gut and skin inflammatory pathologies. The precise mechanism of the terminal steps in the pathway, where the RIPK3 kinase phosphorylates and triggers a conformation change and oligomerization of the terminal pathway effector, MLKL, are only emerging. Here, we structurally identify RIPK3-mediated phosphorylation of the human MLKL activation loop as a cue for MLKL pseudokinase domain dimerization. MLKL pseudokinase domain dimerization subsequently drives formation of elongated homotetramers. Negative stain electron microscopy and modelling support nucleation of the MLKL tetramer assembly by a central coiled coil formed by the extended, ~80 Å brace helix that connects the pseudokinase and executioner four-helix bundle domains. Mutational data assert MLKL tetramerization as an essential prerequisite step to enable the release and reorganization of four-helix bundle domains for membrane permeabilization and cell death.

Topics & Concepts

Cell biologyBiologyPhosphorylationNecroptosisProgrammed cell deathTetramerEffectorBiochemistryApoptosisEnzymeCell death mechanisms and regulationHippo pathway signaling and YAP/TAZEndoplasmic Reticulum Stress and Disease
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