Overexpression of Spry1 in chondrocytes causes attenuated FGFR ubiquitination and sustained ERK activation resulting in chondrodysplasia

Yang, Xuehui; Harkins, Lauren K.; Zubanova, Olga; Harrington, Anne; Коваленко, Д. В.; Nadeau, Robert J.; Chen, Pei-Yu; Toher, Jessica L.; Lindner, Volkhard; Liaw, Lucy; Friesel, Robert

doi:10.1016/j.ydbio.2008.05.555

Cited by 31 publications

(45 citation statements)

References 54 publications

(70 reference statements)

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“…This is surprising because loss of Spry1 function in several other contexts results in enhanced signaling downstream of RTKs [25], [26]. However, previous studies have also shown that Spry1 and Spry2 can interfere with ubiquitination and degradation of FGFR1 [27] and EGFR [28], [29], which leads to enhanced RTK signaling. By binding to c-Cbl, Spry2 prevents c-Cbl mediated ubiquitination and degradation of EGFR.…”

Section: Discussionmentioning

confidence: 99%

Spry1 and Spry4 Differentially Regulate Human Aortic Smooth Muscle Cell Phenotype via Akt/FoxO/Myocardin Signaling

et al. 2013

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BackgroundChanges in the vascular smooth muscle cell (VSMC) contractile phenotype occur in pathological states such as restenosis and atherosclerosis. Multiple cytokines, signaling through receptor tyrosine kinases (RTK) and PI3K/Akt and MAPK/ERK pathways, regulate these phenotypic transitions. The Spry proteins are feedback modulators of RTK signaling, but their specific roles in VSMC have not been established.Methodology/Principal FindingsHere, we report for the first time that Spry1, but not Spry4, is required for maintaining the differentiated state of human VSMC in vitro. While Spry1 is a known MAPK/ERK inhibitor in many cell types, we found that Spry1 has little effect on MAPK/ERK signaling but increases and maintains Akt activation in VSMC. Sustained Akt signaling is required for VSMC marker expression in vitro, while ERK signaling negatively modulates Akt activation and VSMC marker gene expression. Spry4, which antagonizes both MAPK/ERK and Akt signaling, suppresses VSMC differentiation marker gene expression. We show using siRNA knockdown and ChIP assays that FoxO3a, a downstream target of PI3K/Akt signaling, represses myocardin promoter activity, and that Spry1 increases, while Spry4 decreases myocardin mRNA levels.ConclusionsTogether, these data indicate that Spry1 and Spry4 have opposing roles in VSMC phenotypic modulation, and Spry1 maintains the VSMC differentiation phenotype in vitro in part through an Akt/FoxO/myocardin pathway.

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Section: Discussionmentioning

confidence: 99%

Spry1 and Spry4 Differentially Regulate Human Aortic Smooth Muscle Cell Phenotype via Akt/FoxO/Myocardin Signaling

et al. 2013

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“…Wild type C57BL/6J mice were obtained from National Institute on Aging; Pax7 CreERT2 (017763), Rosa26 mTmG (007576), Rosa26 nTnG (023035) and Rosa26 DTA (009669) mice were obtained from Jackson Laboratories (Bar Harbor, Maine); mice carrying a transgene encoding a Cre-inducible expression construct for Spry1 controlled by a chicken β-actin gene (CAG) promoter were used for Spry1-overexpression studies (Chakkalakal et al, 2012; Yang et al, 2008). Rosa26 mTmG , Rosa26 nTnG , Rosa26 DTA and CAG Spry1 mice were crossed with Pax7 CreERT2 mice to generate Pax7 CreER/+ ; Rosa26 mTmG/+ (P7mTmG), Pax7 CreER/+ ; Rosa26 nTnG/+ (P7nTnG), Pax7 CreER/+ ; Rosa26 DTA/+ (P7DTA), Pax7 CreER/+ ; CAG Spry1/+ (Spry1OX) mice and control CreER negative (Ctrl) littermates.…”

Section: Methodsmentioning

confidence: 99%

Loss of adult skeletal muscle stem cells drives age-related neuromuscular junction degeneration

Liu

Klose

Forman

et al. 2017

eLife

140

175

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Neuromuscular junction degeneration is a prominent aspect of sarcopenia, the age-associated loss of skeletal muscle integrity. Previously, we showed that muscle stem cells activate and contribute to mouse neuromuscular junction regeneration in response to denervation (Liu et al., 2015). Here, we examined gene expression profiles and neuromuscular junction integrity in aged mouse muscles, and unexpectedly found limited denervation despite a high level of degenerated neuromuscular junctions. Instead, degenerated neuromuscular junctions were associated with reduced contribution from muscle stem cells. Indeed, muscle stem cell depletion was sufficient to induce neuromuscular junction degeneration at a younger age. Conversely, prevention of muscle stem cell and derived myonuclei loss was associated with attenuation of age-related neuromuscular junction degeneration, muscle atrophy, and the promotion of aged muscle force generation. Our observations demonstrate that deficiencies in muscle stem cell fate and post-synaptic myogenesis provide a cellular basis for age-related neuromuscular junction degeneration and associated skeletal muscle decline.DOI: http://dx.doi.org/10.7554/eLife.26464.001

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“…Stability of proteins is essential for the maintenance of protein function. Overexpression of Sprouty 1 in chondrocytes results in decreased FGFR2 ubiquitination, increased FGFR2 stability, and sustained ERK activation (Yang et al 2008). The detailed mechanisms underlying the degradation of FGFRs after ligand binding are poorly known.…”

Section: Perspectivesmentioning

confidence: 99%

RECENT RESEARCH ON THE GROWTH PLATE: Advances in fibroblast growth factor signaling in growth plate development and disorders

Xie

Zhou

Chen

et al. 2014

Journal of Molecular Endocrinology

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Skeletons are formed through two distinct developmental actions, intramembranous ossification and endochondral ossification. During embryonic development, most bone is formed by endochondral ossification. The growth plate is the developmental center for endochondral ossification. Multiple signaling pathways participate in the regulation of endochondral ossification. Fibroblast growth factor (FGF)/FGF receptor (FGFR) signaling has been found to play a vital role in the development and maintenance of growth plates. Missense mutations in FGFs and FGFRs can cause multiple genetic skeletal diseases with disordered endochondral ossification. Clarifying the molecular mechanisms of FGFs/FGFRs signaling in skeletal development and genetic skeletal diseases will have implications for the development of therapies for FGF-signaling-related skeletal dysplasias and growth plate injuries. In this review, we summarize the recent advances in elucidating the role of FGFs/FGFRs signaling in growth plate development, genetic skeletal disorders, and the promising therapies for those genetic skeletal diseases resulting from FGFs/FGFRs dysfunction. Finally, we also examine the potential important research in this field in the future.

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Overexpression of Spry1 in chondrocytes causes attenuated FGFR ubiquitination and sustained ERK activation resulting in chondrodysplasia

Cited by 31 publications

References 54 publications

Spry1 and Spry4 Differentially Regulate Human Aortic Smooth Muscle Cell Phenotype via Akt/FoxO/Myocardin Signaling

Spry1 and Spry4 Differentially Regulate Human Aortic Smooth Muscle Cell Phenotype via Akt/FoxO/Myocardin Signaling

Loss of adult skeletal muscle stem cells drives age-related neuromuscular junction degeneration

RECENT RESEARCH ON THE GROWTH PLATE: Advances in fibroblast growth factor signaling in growth plate development and disorders

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