Germline gain-of-function mutations in SOS1 cause Noonan syndrome

Roberts, Amy; Araki, Toshiyuki; Swanson, Kenneth D.; Montgomery, Kate; Schiripo, Taryn A.; Joshi, Victoria A.; Li, Li; Yassin, Yosuf; Tamburino, Alex M; Neel, Benjamin G.; Kucherlapati, Raju

doi:10.1038/ng1926

Cited by 538 publications

(513 citation statements)

References 22 publications

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“…The analysis of SOS1 illustrates the individualized approach for each syndrome and mutation. Since Roberts et al [2007] listed each patient allowing complete analysis, and Zenker et al [2007b] provided a summary table useful for many data points, both references were used in a complementary fashion; a smaller series [Narumi et al, 2008] was omitted as per general methods. A condensed comparison is shown in Table VI based on study patient data only.…”

Section: Comparison With Rasopathiesmentioning

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

108

106

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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.

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Section: Comparison With Rasopathiesmentioning

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

108

106

View full text Add to dashboard Cite

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“…Phenotypically overlapping Costelo syndrome and cardio-facio-cutaneous syndrome are caused by gain-of-function HRAS mutation and KRAS/BRAF/MEK1/MEK2 mutation, respectively (Aoki et al, 2005;Niihori et al, 2006;RodriguezViciana et al, 2006). Some Noonan syndrome cases are also attributed to gain-of-function mutations in SOS1 that encodes the RAS guanine nucleotide exchange factor or KRAS (Schubbert et al, 2006;Roberts et al, 2007;Tartaglia et al, 2007). The observations collectively indicate that aberrant activation of the SHP-2-RAS-ERK pathway plays a key role in these overlapping developmental disorders (Gelb and Tartaglia, 2006).…”

Section: Introductionmentioning

confidence: 95%

Isolation of a distinct class of gain-of-function SHP-2 mutants with oncogenic RAS-like transforming activity from solid tumors

Miyamoto

Takahashi

et al. 2008

Oncogene

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“…17 We here show that the SOS1 c. M269R)) changes in exon 6 have been shown to be pathogenetic mutations. 13 The three affected members of the NS family here described did not show any mutation in the known NS genes other than the c.755T4C SOS1 variant. Our proband's phenotype resembles that of SOS1-mutated individuals, being associated with relative macrocephaly, ptosis and absence of short stature, whereas her cutaneous findings -lentigines, cafè-au-lait spots -are similar to those of NS-like with lentigines rather than those found in Cardio-facio-cutaneous syndrome and patients with SOS1 gene mutations, 8 that is, hyperkeratotic skin, sparse eyebrows, sparse slow growing curly hair.…”

Section: Discussionmentioning

confidence: 64%

“…At this purpose we transfected HEK293 cells with the mutant Sos-p.I252T plasmid, the wild-type human SOS1 or the mutant isoform SOS1 c.806T 4 C (p.(M269R)), previously reported to activate the RAS-ERK pathway 13 as a positive control and compared the ERK1 phosphorylation levels of each SOS1 isoform before and after EGF stimulation. We found that the Sos-p.I252T substitution significantly increased ERK1 phosphorylation level, with a level comparable to the c.806T 4 C (p.(M269R)) mutant-positive control (Figure 2a and b).…”

Section: Functional Study Of Sos1 C755t4c (P(i252t))mentioning

confidence: 99%

Differential allelic expression of SOS1 and hyperexpression of the activating SOS1 c.755C variant in a Noonan syndrome family

et al. 2015

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Noonan syndrome (NS) is a genetic condition characterized by congenital heart defects, short stature and characteristic facial features. We here present the case of a girl with moderate learning disabilities, delayed language development, craniofacial features and skin anomalies reminiscent of NS. After a mutation screening of the known NS genes PTPN11, SOS1, RAF1, KRAS, GRB2, BRAF and SHOC2 we found the heterozygous c.755T4C variant in SOS1 causing the p.I252T amino-acid substitution, which was considered possibly pathogenetic by bioinformatic predictions. The same variant was present in the proband's mother, displaying some NS features, and maternal grandfather showing no NS traits, but also by a healthy subject in 1000 genomes project database without phenotype informations. The functional analysis revealed that SOS1 c.755C activated the RAS-ERK intracellular pathway, whereas no effects on RAC-JNK cascade have been detected. After a comparison between the sequence of SOS1 cDNA from peripheral blood and SOS1 genomic DNA, we showed for the first time a differential allelic expression of the SOS1 gene in healthy individuals, thus occurring as a physiologic condition. Interestingly, we found that the mutated allele C was 50% more expressed than the wild-type allele T in all familial carriers. The comparable amount of SOS1 mRNA between mutated individuals and the controls indicates that the variant does not affect SOS1 expression. The present study provides a first evidence of allelic imbalance of SOS1 and pinpoints this condition as a possible mechanism underlying a different penetrance of some SOS1-mutated alleles in unrelated carriers.

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Germline gain-of-function mutations in SOS1 cause Noonan syndrome

Cited by 538 publications

References 22 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

Isolation of a distinct class of gain-of-function SHP-2 mutants with oncogenic RAS-like transforming activity from solid tumors

Differential allelic expression of SOS1 and hyperexpression of the activating SOS1 c.755C variant in a Noonan syndrome family

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