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HRAS mutants identified in Costello syndrome patients can induce cellular senescence: possible implications for the pathogenesis of Costello syndrome

Authors :
Toju Tanaka
Isaku Omori
Kiyoshi Kikuchi
Masaru Miura
Hiroshi Kawame
Erika Okano
Kenji Ihara
Johji Inazawa
Toshihiro Ohura
Yoichi Matsubara
Hiroyo Mabe
Akira Ohtake
Shin Nabatame
Kenji Kurosawa
Hironao Numabe
Kyoko Watanabe
Seiji Mizuno
Tetsuya Niihori
Hirofumi Ohashi
Yoko Aoki
Yoshikazu Kuroki
Shinichi Niijima
Nobuhiko Okamoto
Hiroshi Arai
Source :
Journal of Human Genetics. 56:707-715
Publication Year :
2011
Publisher :
Springer Science and Business Media LLC, 2011.

Abstract

Costello syndrome (CS) is a congenital disease that is characterized by a distinctive facial appearance, failure to thrive, mental retardation and cardiomyopathy. In 2005, we discovered that heterozygous germline mutations in HRAS caused CS. Several studies have shown that CS-associated HRAS mutations are clustered in codons 12 and 13, and mutations in other codons have also been identified. However, a comprehensive comparison of the substitutions identified in patients with CS has not been conducted. In the current study, we identified four mutations (p.G12S, p.G12A, p.G12C and p.G12D) in 21 patients and analyzed the associated clinical manifestations of CS in these individuals. To examine functional differences among the identified mutations, we characterized a total of nine HRAS mutants, including seven distinct substitutions in codons 12 and 13, p.K117R and p.A146T. The p.A146T mutant demonstrated the weakest Raf-binding activity, and the p.K117R and p.A146T mutants had weaker effects on downstream c-Jun N-terminal kinase signaling than did codon 12 or 13 mutants. We demonstrated that these mutant HRAS proteins induced senescence when overexpressed in human fibroblasts. Oncogene-induced senescence is a cellular reaction that controls cell proliferation in response to oncogenic mutation and it has been considered one of the tumor suppression mechanisms in vivo. Our findings suggest that the HRAS mutations identified in CS are sufficient to cause oncogene-induced senescence and that cellular senescence might therefore contribute to the pathogenesis of CS.

Details

ISSN :
1435232X and 14345161
Volume :
56
Database :
OpenAIRE
Journal :
Journal of Human Genetics
Accession number :
edsair.doi.dedup.....b9fc9aeb1143f53a79764a5fe3ebaf13
Full Text :
https://doi.org/10.1038/jhg.2011.85