Architecture of the MKK6-p38α complex defines the basis of MAPK specificity and activation.
Pauline JuyouxIoannis GaldadasDorothea GobboJill von VelsenMartin PelosseMark D TullyOscar VadasFrancesco Luigi GervasioErika PellegriniMatthew W BowlerPublished in: Science (New York, N.Y.) (2023)
The mitogen-activated protein kinase (MAPK) p38α is a central component of signaling in inflammation and the immune response and is, therefore, an important drug target. Little is known about the molecular mechanism of its activation by double phosphorylation from MAPK kinases (MAP2Ks), because of the challenge of trapping a transient and dynamic heterokinase complex. We applied a multidisciplinary approach to generate a structural model of p38α in complex with its MAP2K, MKK6, and to understand the activation mechanism. Integrating cryo-electron microscopy with molecular dynamics simulations, hydrogen-deuterium exchange mass spectrometry, and experiments in cells, we demonstrate a dynamic, multistep phosphorylation mechanism, identify catalytically relevant interactions, and show that MAP2K-disordered amino termini determine pathway specificity. Our work captures a fundamental step of cell signaling: a kinase phosphorylating its downstream target kinase.
Keyphrases
- protein kinase
- molecular dynamics simulations
- electron microscopy
- oxidative stress
- signaling pathway
- immune response
- mass spectrometry
- induced apoptosis
- pi k akt
- tyrosine kinase
- high resolution
- cell cycle arrest
- high density
- single cell
- liquid chromatography
- emergency department
- stem cells
- molecular docking
- toll like receptor
- cerebral ischemia
- mesenchymal stem cells
- dendritic cells
- ms ms
- drug induced
- capillary electrophoresis