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Structural basis for ALK2/BMPR2 receptor complex signaling through kinase domain oligomerization

https://doi.org/10.1038/s41467-021-25248-5

Agnew, Christopher ; Ayaz, Pelin ; Kashima, Risa ; Loving, Hanna S. ; Ghatpande, Prajakta ; Kung, Jennifer E. ; Underbakke, Eric S. ; Shan, Yibing ; Shaw, David E. ; Hata, Akiko ; et al ( December 2021 , Nature Communications)

Abstract Upon ligand binding, bone morphogenetic protein (BMP) receptors form active tetrameric complexes, comprised of two type I and two type II receptors, which then transmit signals to SMAD proteins. The link between receptor tetramerization and the mechanism of kinase activation, however, has not been elucidated. Here, using hydrogen deuterium exchange mass spectrometry (HDX-MS), small angle X-ray scattering (SAXS) and molecular dynamics (MD) simulations, combined with analysis of SMAD signaling, we show that the kinase domain of the type I receptor ALK2 and type II receptor BMPR2 form a heterodimeric complex via their C-terminal lobes. Formation of this dimer is essential for ligand-induced receptor signaling and is targeted by mutations in BMPR2 in patients with pulmonary arterial hypertension (PAH). We further show that the type I/type II kinase domain heterodimer serves as the scaffold for assembly of the active tetrameric receptor complexes to enable phosphorylation of the GS domain and activation of SMADs.
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How IGF-1 activates its receptor

https://doi.org/10.7554/eLife.03772

Kavran, Jennifer M ; McCabe, Jacqueline M ; Byrne, Patrick O ; Connacher, Mary Katherine ; Wang, Zhihong ; Ramek, Alexander ; Sarabipour, Sarvenaz ; Shan, Yibing ; Shaw, David E ; Hristova, Kalina ; et al ( September 2014 , eLife)

The type I insulin-like growth factor receptor (IGF1R) is involved in growth and survival of normal and neoplastic cells. A ligand-dependent conformational change is thought to regulate IGF1R activity, but the nature of this change is unclear. We point out an underappreciated dimer in the crystal structure of the related Insulin Receptor (IR) with Insulin bound that allows direct comparison with unliganded IR and suggests a mechanism by which ligand regulates IR/IGF1R activity. We test this mechanism in a series of biochemical and biophysical assays and find the IGF1R ectodomain maintains an autoinhibited state in which the TMs are held apart. Ligand binding releases this constraint, allowing TM association and unleashing an intrinsic propensity of the intracellular regions to autophosphorylate. Enzymatic studies of full-length and kinase-containing fragments show phosphorylated IGF1R is fully active independent of ligand and the extracellular-TM regions. The key step triggered by ligand binding is thus autophosphorylation.

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