| Literature DB >> 30140198 |
Yoshiro Maezawa1, Hisaya Kato1, Minoru Takemoto1,2, Aki Watanabe1, Masaya Koshizaka1, Takahiro Ishikawa1, Forough Sargolzaeiaval3, Masafumi Kuzuya4, Hiroshi Wakabayashi5, Takashi Kusaka6, Koutaro Yokote1, Junko Oshima1,3.
Abstract
Werner syndrome (WS) is a rare autosomal recessive disorder characterized by systemic accelerated aging. It is caused by pathogenic variants of the WRN gene that encodes a nuclear helicase. In this report, we describe 4 newly identified WS cases among those referred to the Japanese Werner Consortium, Chiba University, Japan. All 4 cases were compound heterozygotes of the Japanese founder mutation, c.3139-1G>C, and a novel null pathogenic variant, c.1587G>A, c.2448+1G>A, or c.3233+1G>T, or an amino acid substitution variant, c.1720G>A, p.Gly574Arg. These 3 null pathogenic variants were not previously described. The p. Gly574Arg was previously reported in a European patient, and the identification of the second p. Gly574Arg case, with classical WS features, further confirmed the pathogenic nature of this variant. For the case with c.3233+1G>T, we determined the phase of 2 disease-causing mutations and demonstrated that they are on different chromosomes. This assay would be particularly important for those cases with ambiguous clinical diagnosis.Entities:
Keywords: Mendelian disorder; Progeroid syndrome; WRN; Werner syndrome
Year: 2018 PMID: 30140198 PMCID: PMC6103371 DOI: 10.1159/000489055
Source DB: PubMed Journal: Mol Syndromol ISSN: 1661-8769