Phosphoproteomics-Mediated Identification of Fer Kinase as a Target of Mutant Shp2 in Noonan and LEOPARD Syndrome
摘要:
Noonan syndrome (NS) and LEOPARD syndrome (LS) cause congenital afflictions such as short stature, hypertelorism and heart defects. More than 50% of NS and almost all of LS cases are caused by activating and inactivating mutations of the phosphatase Shp2, respectively. How these biochemically opposing mutations lead to similar clinical outcomes is not clear. Using zebrafish models of NS and LS and mass spectrometry-based phosphotyrosine proteomics, we identified a down-regulated peptide of Fer kinase in both NS and LS. Further investigation showed a role for Fer during development, where morpholino-based knockdown caused craniofacial defects, heart edema and short stature. During gastrulation, loss of Fer caused convergence and extension defects without affecting cell fate. Moreover, Fer knockdown cooperated with NS and LS, but not wild type Shp2 to induce developmental defects, suggesting a role for Fer in the pathogenesis of both NS and LS.
展开
DOI:
10.1371/journal.pone.0106682
被引量:
年份:
2014
EBSCO
Semantic Scholar
掌桥科研
万方医学
dx.doi.org
查看更多
NCBI
NCBI
(全网免费下载)
Europe PMC
NCBI
Europe PMC
(全网免费下载)
plosone.org
adsabs.harvard.edu
ResearchGate
(全网免费下载)
ResearchGate
ProQuest
EBSCO
EBSCO
学术范
onAcademic
www.socolar.com
journals.plos.org
(全网免费下载)
学术范
(全网免费下载)
science-open.com
paperity.org
narcis.nl
scienceopen.com
dx.plos.org
通过文献互助平台发起求助,成功后即可免费获取论文全文。
相似文献
参考文献
引证文献
辅助模式
引用
文献可以批量引用啦~
欢迎点我试用!
