SMARCA4 inactivating mutations cause concomitant Coffin-Siris syndrome, microphthalmia and small-cell carcinoma of the ovary hypercalcaemic type
Articolo
Data di Pubblicazione:
2017
Citazione:
SMARCA4 inactivating mutations cause concomitant Coffin-Siris syndrome, microphthalmia and small-cell carcinoma of the ovary hypercalcaemic type / Errichiello, Edoardo; Mustafa, Noor; Vetro, Annalisa; Notarangelo, Lucia Dora; De Jonge, Hugo; Rinaldi, Berardo; Vergani, Debora; Giglio, Sabrina Rita; Morbini, Patrizia; Zuffardi, Orsetta. - In: JOURNAL OF PATHOLOGY. - ISSN 0022-3417. - 243:1(2017), pp. 9-15. [10.1002/path.4926]
Abstract:
SMARCA4 chromatin remodelling factor is mutated in 11% of Coffin-Siris syndrome (CSS) patients and in almost all small-cell carcinoma of the ovary hypercalcaemic type (SCCOHT) tumours. Missense mutations with gain-of-function or dominant-negative effects are associated with CSS, whereas inactivating mutations, leading to loss of SMARCA4 expression, have been exclusively found in SCCOHT. We applied whole-exome sequencing to study a 15-year-old patient with mild CSS who concomitantly developed SCCOHT at age 13 years. Interestingly, our patient also showed congenital microphthalmia, which has never previously been reported in CSS patients. We detected a de novo germline heterozygous nonsense mutation in exon 19 of SMARCA4 (c.2935C > T;p.Arg979*), and a somatic frameshift mutation in exon 6 (c.1236_1236delC;p.Gln413Argfs*88), causing complete loss of SMARCA4 immunostaining in the tumour. The immunohistochemical findings are supported by the observation that the c.2935C > T mutant transcript was detected by reverse transcription polymerase chain reaction at a much lower level than the wild-type allele in whole blood and the lymphoblastoid cell line of the proband, confirming nonsense-mediated mRNA decay. Accordingly, immunoblotting demonstrated that there was approximately half the amount of SMARCA4 protein in the proband's cells as in controls. This study suggests that SMARCA4 constitutional mutations associated with CSS are not necessarily non-truncating, and that haploinsufficiency may explain milder CSS phenotypes, as previously reported for haploinsufficient ARID1B. In addition, our case supports the dual role of chromatin remodellers in developmental disorders and cancer, as well as the involvement of SMARCA4 in microphthalmia, confirming previous findings in mouse models and the DECIPHER database. Finally, we speculate that mild CSS might be under-recognized in a proportion of SCCOHT patients harbouring SMARCA4 mutations.
Tipologia CRIS:
1.1 Articolo in rivista
Keywords:
2734; chromatin remodelling factors; Coffinâ Siris syndrome (CSS); haploinsufficiency; intellectual disability; microphthalmia; nonsense-mediated mRNA decay (NMD); small-cell carcinoma of the ovary hypercalcaemic type (SCCOHT); SMARCA4/BRG1; SWI/SNF complex; whole-exome sequencing (WES); Abnormalities; Multiple; Adolescent; Biomarkers; Tumor; Blotting; Western; Carcinoma; Small Cell; DNA Helicases; DNA Mutational Analysis; Face; Female; Genetic Predisposition to Disease; Hand Deformities; Congenital; Heterozygote; Humans; Hypercalcemia; Immunohistochemistry; Intellectual Disability; Male; Micrognathism; Microphthalmos; Middle Aged; Neck; Nuclear Proteins; Ovarian Neoplasms; Pedigree; Phenotype; RNA; Messenger; Reverse Transcriptase Polymerase Chain Reaction; Transcription Factors; Codon; Nonsense; Frameshift Mutation
Elenco autori:
Errichiello, Edoardo; Mustafa, Noor; Vetro, Annalisa; Notarangelo, Lucia Dora; De Jonge, Hugo; Rinaldi, Berardo; Vergani, Debora; Giglio, Sabrina Rita; Morbini, Patrizia; Zuffardi, Orsetta
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