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4 záznamů v Medvik

Článek

Mutations in GRK2 cause Jeune syndrome by impairing Hedgehog and canonical Wnt signaling

Bosakova, Michaela
Autor Bosakova, Michaela Department of Biology, Faculty of Medicine, Masaryk University, Brno, Czech Republic International Clinical Research Center, St. Anne's University Hospital, Brno, Czech Republic Institute of Animal Physiology and Genetics of the CAS, Brno, Czech Republic
Abraham, Sara P
Autor Abraham, Sara P Department of Biology, Faculty of Medicine, Masaryk University, Brno, Czech Republic
Nita, Alexandru
Autor Nita, Alexandru Department of Biology, Faculty of Medicine, Masaryk University, Brno, Czech Republic
Hruba, Eva
Autor Hruba, Eva Institute of Animal Physiology and Genetics of the CAS, Brno, Czech Republic
Buchtova, Marcela
Autor Buchtova, Marcela Institute of Animal Physiology and Genetics of the CAS, Brno, Czech Republic
Taylor, S Paige
Autor Taylor, S Paige Department of Orthopaedic Surgery, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA
Duran, Ivan
Autor Duran, Ivan Department of Orthopaedic Surgery, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA
Martin, Jorge
Autor Martin, Jorge Department of Orthopaedic Surgery, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA
Svozilova, Katerina
Autor Svozilova, Katerina Department of Biology, Faculty of Medicine, Masaryk University, Brno, Czech Republic Institute of Animal Physiology and Genetics of the CAS, Brno, Czech Republic
Barta, Tomas
Autor Barta, Tomas Department of Histology and Embryology, Faculty of Medicine, Masaryk University, Brno, Czech Republic

EMBO molecular medicine. 2020 ; 12 (11) : e11739. [pub] 20201014

EMBO Mol Med
ISSN 1757-4684
Medvik
Zdroj

Mutations in genes affecting primary cilia cause ciliopathies, a diverse group of disorders often affecting skeletal development. This includes Jeune syndrome or asphyxiating thoracic dystrophy (ATD), an autosomal recessive skeletal disorder. Unraveling the responsible molecular pathology helps illuminate mechanisms responsible for functional primary cilia. We identified two families with ATD caused by loss-of-function mutations in the gene encoding adrenergic receptor kinase 1 (ADRBK1 or GRK2). GRK2 cells from an affected individual homozygous for the p.R158* mutation resulted in loss of GRK2, and disrupted chondrocyte growth and differentiation in the cartilage growth plate. GRK2 null cells displayed normal cilia morphology, yet loss of GRK2 compromised cilia-based signaling of Hedgehog (Hh) pathway. Canonical Wnt signaling was also impaired, manifested as a failure to respond to Wnt ligand due to impaired phosphorylation of the Wnt co-receptor LRP6. We have identified GRK2 as an essential regulator of skeletogenesis and demonstrate how both Hh and Wnt signaling mechanistically contribute to skeletal ciliopathies.

MeSH
Ellisův-van Creveldův syndrom * MeSH
kinasa 2 receptorů spřažených s G-proteiny genetika MeSH
lidé MeSH
mutace MeSH
proteiny hedgehog * genetika MeSH
signální dráha Wnt MeSH
Check Tag
lidé MeSH
Publikační typ
časopisecké články MeSH
práce podpořená grantem MeSH
Research Support, N.I.H., Extramural MeSH

Článek

Fibroblast growth factor receptor influences primary cilium length through an interaction with intestinal cell kinase

Proceedings of the National Academy of Sciences of the United States of America. 2019 ; 116 (10) : 4316-4325. [pub] 20190219

Proc Natl Acad Sci U S A
ISSN 1091-6490
Medvik
Zdroj

Vertebrate primary cilium is a Hedgehog signaling center but the extent of its involvement in other signaling systems is less well understood. This report delineates a mechanism by which fibroblast growth factor (FGF) controls primary cilia. Employing proteomic approaches to characterize proteins associated with the FGF-receptor, FGFR3, we identified the serine/threonine kinase intestinal cell kinase (ICK) as an FGFR interactor. ICK is involved in ciliogenesis and participates in control of ciliary length. FGF signaling partially abolished ICK's kinase activity, through FGFR-mediated ICK phosphorylation at conserved residue Tyr15, which interfered with optimal ATP binding. Activation of the FGF signaling pathway affected both primary cilia length and function in a manner consistent with cilia effects caused by inhibition of ICK activity. Moreover, knockdown and knockout of ICK rescued the FGF-mediated effect on cilia. We provide conclusive evidence that FGF signaling controls cilia via interaction with ICK.

Článek

The PTH/PTHrP-SIK3 pathway affects skeletogenesis through altered mTOR signaling

Science translational medicine. 2018 ; 10 (459) : . [pub] 20180919

Sci Transl Med
ISSN 1946-6242
Medvik
Zdroj

Studies have suggested a role for the mammalian (or mechanistic) target of rapamycin (mTOR) in skeletal development and homeostasis, yet there is no evidence connecting mTOR with the key signaling pathways that regulate skeletogenesis. We identified a parathyroid hormone (PTH)/PTH-related peptide (PTHrP)-salt-inducible kinase 3 (SIK3)-mTOR signaling cascade essential for skeletogenesis. While investigating a new skeletal dysplasia caused by a homozygous mutation in the catalytic domain of SIK3, we observed decreased activity of mTOR complex 1 (mTORC1) and mTORC2 due to accumulation of DEPTOR, a negative regulator of both mTOR complexes. This SIK3 syndrome shared skeletal features with Jansen metaphyseal chondrodysplasia (JMC), a disorder caused by constitutive activation of the PTH/PTHrP receptor. JMC-derived chondrocytes showed reduced SIK3 activity, elevated DEPTOR, and decreased mTORC1 and mTORC2 activity, indicating a common mechanism of disease. The data demonstrate that SIK3 is an essential positive regulator of mTOR signaling that functions by triggering DEPTOR degradation in response to PTH/PTHrP signaling during skeletogenesis.

Článek

The inositol phosphatase SHIP2 enables sustained ERK activation downstream of FGF receptors by recruiting Src kinases

Science signaling. 2018 ; 11 (548) : . [pub] 20180918

Sci Signal
ISSN 1937-9145
Medvik
Zdroj

Sustained activation of extracellular signal-regulated kinase (ERK) drives pathologies caused by mutations in fibroblast growth factor receptors (FGFRs). We previously identified the inositol phosphatase SHIP2 (also known as INPPL1) as an FGFR-interacting protein and a target of the tyrosine kinase activities of FGFR1, FGFR3, and FGFR4. We report that loss of SHIP2 converted FGF-mediated sustained ERK activation into a transient signal and rescued cell phenotypes triggered by pathologic FGFR-ERK signaling. Mutant forms of SHIP2 lacking phosphoinositide phosphatase activity still associated with FGFRs and did not prevent FGF-induced sustained ERK activation, demonstrating that the adaptor rather than the catalytic activity of SHIP2 was required. SHIP2 recruited Src family kinases to the FGFRs, which promoted FGFR-mediated phosphorylation and assembly of protein complexes that relayed signaling to ERK. SHIP2 interacted with FGFRs, was phosphorylated by active FGFRs, and promoted FGFR-ERK signaling at the level of phosphorylation of the adaptor FRS2 and recruitment of the tyrosine phosphatase PTPN11. Thus, SHIP2 is an essential component of canonical FGF-FGFR signal transduction and a potential therapeutic target in FGFR-related disorders.

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