| Literature DB >> 31147515 |
Casey A Gifford1,2, Sanjeev S Ranade1,2, Ryan Samarakoon1,2, Hazel T Salunga1,2, T Yvanka de Soysa1,2, Yu Huang1, Ping Zhou1, Aryé Elfenbein1,2, Stacia K Wyman1, Yen Kim Bui1,2, Kimberly R Cordes Metzler1,2, Philip Ursell3, Kathryn N Ivey1,2,4, Deepak Srivastava5,2,4,6.
Abstract
Complex genetic mechanisms are thought to underlie many human diseases, yet experimental proof of this model has been elusive. Here, we show that a human cardiac anomaly can be caused by a combination of rare, inherited heterozygous mutations. Whole-exome sequencing of a nuclear family revealed that three offspring with childhood-onset cardiomyopathy had inherited three missense single-nucleotide variants in the MKL2, MYH7, and NKX2-5 genes. The MYH7 and MKL2 variants were inherited from the affected, asymptomatic father and the rare NKX2-5 variant (minor allele frequency, 0.0012) from the unaffected mother. We used CRISPR-Cas9 to generate mice encoding the orthologous variants and found that compound heterozygosity for all three variants recapitulated the human disease phenotype. Analysis of murine hearts and human induced pluripotent stem cell-derived cardiomyocytes provided histologic and molecular evidence for the NKX2-5 variant's contribution as a genetic modifier.Entities:
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Year: 2019 PMID: 31147515 PMCID: PMC6557373 DOI: 10.1126/science.aat5056
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728