| Literature DB >> 33258288 |
Caio Robledo D'Angioli Costa Quaio1,2, Caroline Monaco Moreira1, Gil Monteiro Novo-Filho1, Patricia Rossi Sacramento-Bobotis1, Michele Groenner Penna1, Sandro Felix Perazzio1,3, Aurelio Pimenta Dutra1, Rafael Alves da Silva1,4, Monize Nakamoto Provisor Santos1, Vanessa Yurie Nozaki de Arruda1, Vanessa Galdeno Freitas1,5, Vinícius Ceola Pereira1, Maria Carolina Pintao1, Alexandre Ricardo Dos Santos Fornari1, Ana Lígia Buzolin1, Andre Yuji Oku1, Matheus Burger1, Rodrigo Fernandes Ramalho1, David Santos Marco Antonio1, Elisa Napolitano E Ferreira1, Otavio Jose Eulalio Pereira1, Vanessa Dionisio Cantagalli1, Ana Carolina Gomes Trindade1, Rafaela Rogerio Floriano de Sousa1, Cintia Reys Furuzawa1, Fernanda Verzini1, Shirley Dezan Matalhana1, Naiade Romano1, Daniele Paixão1, Caroline Olivati1, Gustavo Marquezani Spolador1, Gustavo Arantes Rosa Maciel1,6, Viviane Zorzanelli Rocha1,7, Javier Miguelez1, Mario Henrique Burlacchini de Carvalho1,8, Alexandre Wagner Silva de Souza1,3, Luis Eduardo Coelho Andrade1,3, Maria de Lourdes Chauffaille1, Aline Dos Santos Borgo Perazzio1, Ana Lucia Pereira Monteiro Catelani1, Miguel Mitne-Neto1, Chong Ae Kim2, Wagner Antonio da Rosa Baratela1.
Abstract
Rare diseases comprise a diverse group of conditions, most of which involve genetic causes. We describe the variable spectrum of findings and clinical impacts of exome sequencing (ES) in a cohort of 500 patients with rare diseases. In total, 164 primary findings were reported in 158 patients, representing an overall diagnostic yield of 31.6%. Most of the findings (61.6%) corresponded to autosomal dominant conditions, followed by autosomal recessive (25.6%) and X-linked (12.8%) conditions. These patients harbored 195 variants, among which 43.6% are novel in the literature. The rate of molecular diagnosis was considerably higher for prenatal samples (67%; 4/6), younger children (44%; 24/55), consanguinity (50%; 3/6), gastrointestinal/liver disease (44%; 16/36) and syndromic/malformative conditions (41%; 72/175). For 15.6% of the cohort patients, we observed a direct potential for the redirection of care with targeted therapy, tumor screening, medication adjustment and monitoring for disease-specific complications. Secondary findings were reported in 37 patients (7.4%). Based on cost-effectiveness studies in the literature, we speculate that the reports of secondary findings may influence an increase of 123.2 years in the life expectancy for our cohort, or 0.246 years/cohort patient. ES is a powerful method to identify the molecular bases of monogenic disorders and redirect clinical care.Entities:
Keywords: diagnostic yield; exome sequencing; incidental findings; rare diseases; secondary findings
Year: 2020 PMID: 33258288 DOI: 10.1002/ajmg.c.31860
Source DB: PubMed Journal: Am J Med Genet C Semin Med Genet ISSN: 1552-4868 Impact factor: 3.908