Your search keyword '"Phoebe P. C. Smith"' showing total 3 results

1. Conformational interconversion of MLKL and disengagement from RIPK3 precede cell death by necroptosis

Author

Sarah E. Garnish, Yanxiang Meng, Akiko Koide, Jarrod J. Sandow, Eric Denbaum, Annette V. Jacobsen, Wayland Yeung, Andre L. Samson, Christopher R. Horne, Cheree Fitzgibbon, Samuel N. Young, Phoebe P. C. Smith, Andrew I. Webb, Emma J. Petrie, Joanne M. Hildebrand, Natarajan Kannan, Peter E. Czabotar, Shohei Koide, and James M. Murphy

Subjects

Science

Abstract

Mixed Lineage Kinase Domain-Like (MLKL) pseudokinase is phosphorylated by RIPK3 kinase prior to cell death by necroptosis. Here, the authors use monobodies that bind to the MLKL pseudokinase domain as tools, which allowed them to determine the crystal structures of the MLKL pseudokinase domain in two distinct conformations. By combining their structural data with cell signalling assays and MD simulations they provide evidence that endogenous MLKL preassociates with its upstream regulator RIPK3, and that MLKL disengages from RIPK3 following the induction of necroptosis.

Published

2021

2. Conformational interconversion of MLKL and disengagement from RIPK3 precede cell death by necroptosis

Author

Joanne M Hildebrand, Sarah E Garnish, Phoebe P. C. Smith, Annette V. Jacobsen, Yanxiang Meng, Eric Denbaum, Wayland Yeung, Andre L. Samson, Akiko Koide, Andrew I. Webb, Peter E. Czabotar, Natarajan Kannan, Samuel N. Young, Christopher R Horne, Emma J. Petrie, Jarrod J. Sandow, Shohei Koide, Cheree Fitzgibbon, and James M. Murphy

Subjects

0301 basic medicine, Conformational change, Protein Conformation, Necroptosis, Science, Molecular Conformation, General Physics and Astronomy, Kinases, Molecular Dynamics Simulation, Crystallography, X-Ray, DNA-binding protein, General Biochemistry, Genetics and Molecular Biology, Article, Cell membrane, 03 medical and health sciences, Mice, 0302 clinical medicine, Protein structure, medicine, Animals, Humans, Binding site, Phosphorylation, X-ray crystallography, Multidisciplinary, Binding Sites, Cell Death, Chemistry, Kinase, Cell Membrane, General Chemistry, U937 Cells, Recombinant Proteins, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Receptor-Interacting Protein Serine-Threonine Kinases, Mutation, HT29 Cells, Protein Kinases, Sequence Alignment, 030217 neurology & neurosurgery

Abstract

Phosphorylation of the MLKL pseudokinase by the RIPK3 kinase leads to MLKL oligomerization, translocation to, and permeabilization of, the plasma membrane to induce necroptotic cell death. The precise choreography of MLKL activation remains incompletely understood. Here, we report Monobodies, synthetic binding proteins, that bind the pseudokinase domain of MLKL within human cells and their crystal structures in complex with the human MLKL pseudokinase domain. While Monobody-32 constitutively binds the MLKL hinge region, Monobody-27 binds MLKL via an epitope that overlaps the RIPK3 binding site and is only exposed after phosphorylated MLKL disengages from RIPK3 following necroptotic stimulation. The crystal structures identified two distinct conformations of the MLKL pseudokinase domain, supporting the idea that a conformational transition accompanies MLKL disengagement from RIPK3. These studies provide further evidence that MLKL undergoes a large conformational change upon activation, and identify MLKL disengagement from RIPK3 as a key regulatory step in the necroptosis pathway., Mixed Lineage Kinase Domain-Like (MLKL) pseudokinase is phosphorylated by RIPK3 kinase prior to cell death by necroptosis. Here, the authors use monobodies that bind to the MLKL pseudokinase domain as tools, which allowed them to determine the crystal structures of the MLKL pseudokinase domain in two distinct conformations. By combining their structural data with cell signalling assays and MD simulations they provide evidence that endogenous MLKL preassociates with its upstream regulator RIPK3, and that MLKL disengages from RIPK3 following the induction of necroptosis.

Published

2021

3. Identification of MLKL membrane translocation as a checkpoint in necroptotic cell death using Monobodies

Author

Samuel N. Young, Patrick J. Hennessy, Andre L. Samson, Phoebe P. C. Smith, Richard W Birkinshaw, Katherine A Davies, Cheree Fitzgibbon, Emma J. Petrie, Peter E. Czabotar, Andrew I. Webb, Akiko Koide, James M. Murphy, Jarrod J. Sandow, Shohei Koide, Joanne M Hildebrand, Sarah E Garnish, Xavier J Gavin, and Eric Denbaum

Subjects

Protein Conformation, Fibronectin Type III Domain, Necroptosis, Crystallography, X-Ray, DNA-binding protein, Cell membrane, Necrosis, Biomimetic Materials, medicine, Humans, Phosphorylation, Protein kinase A, Multidisciplinary, Chemistry, Effector, Cell Membrane, Signal transducing adaptor protein, Biological Sciences, Transport protein, Cell biology, Protein Transport, medicine.anatomical_structure, Receptor-Interacting Protein Serine-Threonine Kinases, Protein Multimerization, Oligopeptides, Protein Kinases

Abstract

The necroptosis cell death pathway has been implicated in host defense and in the pathology of inflammatory diseases. While phosphorylation of the necroptotic effector pseudokinase Mixed Lineage Kinase Domain-Like (MLKL) by the upstream protein kinase RIPK3 is a hallmark of pathway activation, the precise checkpoints in necroptosis signaling are still unclear. Here we have developed monobodies, synthetic binding proteins, that bind the N-terminal four-helix bundle (4HB) “killer” domain and neighboring first brace helix of human MLKL with nanomolar affinity. When expressed as genetically encoded reagents in cells, these monobodies potently block necroptotic cell death. However, they did not prevent MLKL recruitment to the “necrosome” and phosphorylation by RIPK3, nor the assembly of MLKL into oligomers, but did block MLKL translocation to membranes where activated MLKL normally disrupts membranes to kill cells. An X-ray crystal structure revealed a monobody-binding site centered on the α4 helix of the MLKL 4HB domain, which mutational analyses showed was crucial for reconstitution of necroptosis signaling. These data implicate the α4 helix of its 4HB domain as a crucial site for recruitment of adaptor proteins that mediate membrane translocation, distinct from known phospholipid binding sites.

Published

2020