Snapshots of a hybrid transcription factor in the Hippo pathway

Luo, Xuelian

doi:10.1007/s13238-010-0105-z

Cited by 13 publications

(10 citation statements)

References 63 publications

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“…In this study, we found NHERF1 A190D mutation also appears to affect YAP function. The phosphorylation of YAP at serine 127 residue promotes its binding to 14-3-3 and impairs the nuclear import of YAP (37)(38)(39). NHERF1 A190D mutation led to a decrease in YAP phosphorylation.…”

Section: Discussionmentioning

confidence: 99%

A Novel NHERF1 Mutation in Human Breast Cancer and Effects on Malignant Progression

Yang

et al. 2017

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Section: Discussionmentioning

confidence: 99%

A Novel NHERF1 Mutation in Human Breast Cancer and Effects on Malignant Progression

Yang

et al. 2017

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“…Although YAP does not contain a DNA-binding domain, it binds to the TEAD family of transcription factors (which contains a sequence-specific DNA-binding domain) to form a functional hybrid transcription factor (Luo, 2010; Sudol et al, 2012; Zhao et al, 2008). The YAP–TEAD hybrid then activates the transcription of Hippo-responsive genes that promote cell growth and proliferation and inhibit apoptosis.…”

Section: Introductionmentioning

confidence: 99%

Structural Basis for Autoactivation of Human Mst2 Kinase and Its Regulation by RASSF5

et al. 2013

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SUMMARY The tumor-suppressive Hippo pathway controls tissue homeostasis through balancing cell proliferation and apoptosis. Activation of the kinases Mst1/2 is a key upstream event in this pathway and remains poorly understood. Mst1/2 and their critical regulators RASSFs contain SARAH domains that can homo- and hetero-dimerize. Here, we report the crystal structures of human Mst2 alone and bound to RASSF5. Mst2 undergoes activation through trans-autophosphorylation at its activation loop, which requires SARAH-mediated homodimerization. RASSF5 disrupts Mst2 homodimer and blocks Mst2 autoactivation. Binding of RASSF5 to already activated Mst2, however, does not inhibit its kinase activity. Thus, RASSF5 can act as an inhibitor or a potential positive regulator of Mst2, depending on whether it binds to Mst2 before or after activation-loop phosphorylation. We propose that these temporally sensitive functions of RASSFs enable the Hippo pathway to respond to and integrate diverse cellular signals.

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“…YAP is a major downstream effector of the Hippo pathway. It associates with the TEAD family of transcription factors to stimulate the transcription of Hippo-responsive genes that promote cell proliferation and inhibit apoptosis (Zhao et al 2008b;Luo 2010;Sudol et al 2012). Lats1/2-mediated phosphorylation inhibits YAP by promoting its cytoplasmic sequestration (Dong et al 2007;Zhao et al 2007;Hao et al 2008) and ubiquitination-dependent degradation (Zhao et al 2010b), thereby inhibiting the expression of Hippo-responsive genes, halting proliferation, and promoting apoptosis.…”

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confidence: 99%

Structural basis for Mob1-dependent activation of the core Mst–Lats kinase cascade in Hippo signaling

et al. 2015

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The Mst-Lats kinase cascade is central to the Hippo tumor-suppressive pathway that controls organ size and tissue homeostasis. The adaptor protein Mob1 promotes Lats activation by Mst, but the mechanism remains unknown. Here, we show that human Mob1 binds to autophosphorylated docking motifs in active Mst2. This binding enables Mob1 phosphorylation by Mst2. Phosphorylated Mob1 undergoes conformational activation and binds to Lats1. We determine the crystal structures of phospho-Mst2-Mob1 and phospho-Mob1-Lats1 complexes, revealing the structural basis of both phosphorylation-dependent binding events. Further biochemical and functional analyses demonstrate that Mob1 mediates Lats1 activation through dynamic scaffolding and allosteric mechanisms. Thus, Mob1 acts as a phosphorylation-regulated coupler of kinase activation by virtue of its ability to engage multiple ligands. We propose that stepwise, phosphorylation-triggered docking interactions of nonkinase elements enhance the specificity and robustness of kinase signaling cascades.

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Snapshots of a hybrid transcription factor in the Hippo pathway

Cited by 13 publications

References 63 publications

A Novel NHERF1 Mutation in Human Breast Cancer and Effects on Malignant Progression

A Novel NHERF1 Mutation in Human Breast Cancer and Effects on Malignant Progression

Structural Basis for Autoactivation of Human Mst2 Kinase and Its Regulation by RASSF5

Structural basis for Mob1-dependent activation of the core Mst–Lats kinase cascade in Hippo signaling

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