Genotype-phenotype correlation in Costello syndrome: HRAS mutation analysis in 43 cases

Kerr, Bronwyn; Delrue, Marie‐Ange; Sigaudy, Sabine; Perveen, Rahat; Marche, Michèle; Burgelin, Ingrid; Stef, Marianne; Tang, Ben Zhong; Eden, O. B.; O’Sullivan, James; Sandre-Giovannoli, Annachiara De; Reardon, William; Brewer, Carole; Bennett, Christopher; Quarell, O.; M'Cann, E.; Donnai, Dian; Stewart, Fiona; Hennekam, Raoul C. M.; Cavé, Hélène; Verloes, Alain; Philip, Nicole; Lacombe, Didier; Levy, Nicolas; Arveiler, Benoı̂t; Black, Graeme C M

doi:10.1136/jmg.2005.040352

Cited by 214 publications

(220 citation statements)

References 19 publications

(21 reference statements)

Supporting

Mentioning

204

Contrasting

Unclassified

Order By: Relevance

“…Phenotypic features of Costello syndrome include polyhydramnios, increased birth weight, feeding problems, failure to thrive, short stature, developmental delay, pleasant personality, characteristic facial appearance, soft skin, papillomata, spatulate fingerpads, deep palmar creases, joint and skin laxity, kyphoscoliosis, pectus, and splayed fingers with ulnar deviation. Since the discovery that HRAS gene mutations cause Costello syndrome [Aoki et al, 2005], at least 150 genotyped patients have been studied [reviews by Estep et al, 2006;Gripp et al, 2006;Kerr et al, 2006;Zampino et al, 2007]. Consensus expert opinion recommends that Costello syndrome be defined solely by HRAS mutations , which differs from the molecular heterogeneity of CFC syndrome and Noonan syndrome.…”

Section: Introductionmentioning

confidence: 99%

Clinical, pathological, and molecular analyses of cardiovascular abnormalities in Costello syndrome: A Ras/MAPK pathway syndrome

Lin

Alexander

Colan

et al. 2011

American J of Med Genetics Pt A

114

106

View full text Add to dashboard Cite

Cardiovascular abnormalities are important features of Costello syndrome and other Ras/MAPK pathway syndromes (“RASopathies”). We conducted clinical, pathological and molecular analyses of 146 patients with an HRAS mutation including 61 enrolled in an ongoing longitudinal study and 85 from the literature. In our study, the most common (84%) HRAS mutation was p.G12S. A congenital heart defect (CHD) was present in 27 of 61 patients (44%), usually non‐progressive valvar pulmonary stenosis. Hypertrophic cardiomyopathy (HCM), typically subaortic septal hypertrophy, was noted in 37 (61%), and 5 also had a CHD (14% of those with HCM). HCM was chronic or progressive in 14 (37%), stabilized in 10 (27%), and resolved in 5 (15%) patients with HCM; follow‐up data was not available in 8 (22%). Atrial tachycardia occurred in 29 (48%). Valvar pulmonary stenosis rarely progressed and atrial septal defect was uncommon. Among those with HCM, the likelihood of progressing or remaining stable was similar (37%, 41% respectively). The observation of myocardial fiber disarray in 7 of 10 (70%) genotyped specimens with Costello syndrome is consistent with sarcomeric dysfunction. Multifocal atrial tachycardia may be distinctive for Costello syndrome. Potentially serious atrial tachycardia may present in the fetus, and may continue or worsen in about one‐fourth of those with arrhythmia, but is generally self‐limited in the remaining three‐fourths of patients. Physicians should be aware of the potential for rapid development of severe HCM in infants with Costello syndrome, and the need for cardiovascular surveillance into adulthood as the natural history continues to be delineated. © 2011 Wiley‐Liss, Inc.

show abstract

Section: Introductionmentioning

confidence: 99%

Clinical, pathological, and molecular analyses of cardiovascular abnormalities in Costello syndrome: A Ras/MAPK pathway syndrome

Lin

Alexander

Colan

et al. 2011

American J of Med Genetics Pt A

114

106

View full text Add to dashboard Cite

show abstract

“…Of two CS patients with a p.K117R mutation, one patient had an atypical phenotype such as microretrognatism and slightly less-pronounced plantar and palmar creases. 7 The other patient had mild craniofacial manifestations of CS. 13 One patient with the p.A146V mutation showed a mildly coarse face and did not have deep palmar creases.…”

Section: Discussionmentioning

confidence: 98%

“…The number of fatal cases was 5/138 patients with p.G12S, 4/6 with p.G12C, 3/17 with p.G12A, 3/4 with p.G12D, 2/2 with p.G12V, 1/1 with p.G12E and 1/1 with p.E63K. 3,[5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20][21][22][23] The mortality of patients with p.G12C or p.G12D was significantly higher than that of the patients with the more common p.G12S (P¼0.026 by Fisher's exact test). Previous studies have shown that the p.G12V substitution has the highest transformative potential (p.G12V4p.G12A, p.G12S, p.G12C, p.G12D4p.G13D) and is the most frequently found mutation in human tumors.…”

Section: Discussionmentioning

confidence: 99%

“…Previous studies have also suggested that CS patients with the p.G12A mutation may have an increased risk of malignancy, compared with patients with p.G12S. 7 Patients with the p.G12C mutation had a more severe CS phenotype; these individuals developed severe hypertrophic cardiomyopathy and died in the neonatal period. Patients with p.K117R or p.A146V had a milder and more unusual CS phenotype, compared with patients with mutations in codon 12 or 13.…”

Section: Introductionmentioning

confidence: 96%

“…3 It has been suggested that the CS diagnosis should be applied only to patients with a mutation in HRAS because of the high risk of malignancies associated with HRAS mutations and the relative homogeneity of the CS phenotype. 4 A total of 14 HRAS missense mutations and one duplication mutation have been reported in 185 patients with CS 3,[5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20][21][22][23] or congenital myopathy with excess of muscle spindles. 24 Most of these mutations have previously been reported as somatic and oncogenic mutations in various tumors.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

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

et al. 2011

View full text Add to dashboard Cite

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.

show abstract

Molecular Genetics of Costello Syndrome

Wright

Kerr

2014

Encyclopedia of Life Sciences

View full text Add to dashboard Cite

The molecular basis of Costello syndrome (CS) is heterozygous germline mutations in HRAS . Over 95% of patients with CS have been found to have mutations in codon 12 or codon 13, with over 80% having the single mutation c.34G>A, p.(Gly12Ser). The mutational spectrum is similar, but not identical, to that observed for somatic HRAS mutations in cancer. These mutations result in constitutive activation of the HRAS protein. The function of HRAS as a molecular switch is therefore perturbed, resulting in increased downstream Ras‐MAPK pathway activity. The severity of clinical features of CS in any given individual may be influenced by which mutation is present, with mutations more commonly observed in cancer, such as p.(Gly12Val), which have more dramatic effects at the cellular level, tending to lead to a more severe presentation. As for other germline disorders, however, much variability is seen, which may be due to further genomic and other modifying factors. Key Concepts: Germline gain of function mutations in HRAS cause Costello syndrome (CS). Somatic gain‐of‐function HRAS mutations (often with more extreme biochemical effects) are also found in cancer. HRAS p.(Gly12Ser) is the cause of CS in 80% of patients diagnosed with this condition. CS is associated with advanced paternal age. Spermatogonia in the testes of older fathers may be enriched for mutations conferring a proliferative advantage, such as the HRAS mutations that underlie CS.

show abstract

Genotype-phenotype correlation in Costello syndrome: HRAS mutation analysis in 43 cases

Cited by 214 publications

References 19 publications

Clinical, pathological, and molecular analyses of cardiovascular abnormalities in Costello syndrome: A Ras/MAPK pathway syndrome

Clinical, pathological, and molecular analyses of cardiovascular abnormalities in Costello syndrome: A Ras/MAPK pathway syndrome

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

Molecular Genetics of Costello Syndrome

Contact Info

Product

Resources

About