| Literature DB >> 28185376 |
Kristin D Kernohan1, David A Dyment1,2, Mihaela Pupavac3, Zvi Cramer3, Arran McBride1, Genevieve Bernard3, Isabella Straub3, Martine Tetreault4, Taila Hartley1, Lijia Huang1, Erick Sell5, Jacek Majewski3,4, David S Rosenblatt3, Eric Shoubridge3, Aziz Mhanni6, Tara Myers7, Virginia Proud8, Samanta Vergano8, Brooke Spangler8, Emily Farrow9,10, Jennifer Kussman7, Nicole Safina7, Carol Saunders9,10, Kym M Boycott1,2, Isabelle Thiffault9,10.
Abstract
Deleterious variants in the same gene present in two or more families with overlapping clinical features provide convincing evidence of a disease-gene association; this can be a challenge in the study of ultrarare diseases. To facilitate the identification of additional families, several groups have created "matching" platforms. We describe four individuals from three unrelated families "matched" by GeneMatcher and MatchMakerExchange. Individuals had microcephaly, developmental delay, epilepsy, and recessive mutations in TRIT1. A single homozygous mutation in TRIT1 associated with similar features had previously been reported in one family. The identification of these individuals provides additional evidence to support TRIT1 as the disease-causing gene and interprets the variants as "pathogenic." TRIT1 functions to modify mitochondrial tRNAs and is necessary for protein translation. We show that dysfunctional TRIT1 results in decreased levels of select mitochondrial proteins. Our findings confirm the TRIT1 disease association and advance the phenotypic and molecular understanding of this disorder.Entities:
Keywords: TRIT1; brain anomalies; developmental disorders; epilepsy; intellectual disability; tRNA
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Year: 2017 PMID: 28185376 DOI: 10.1002/humu.23196
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878