<P>We performed targeted re-sequencing to identify the genetic etiology of early-onset postlingual deafness and encountered a frequent <I>TMPRSS3</I> allele harboring two variants in a cis configuration. We aimed to evaluate the path...
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https://www.riss.kr/link?id=A107739175
2017
-
SCOPUS,SCIE
학술저널
2246
0
상세조회0
다운로드다국어 초록 (Multilingual Abstract)
<P>We performed targeted re-sequencing to identify the genetic etiology of early-onset postlingual deafness and encountered a frequent <I>TMPRSS3</I> allele harboring two variants in a cis configuration. We aimed to evaluate the path...
<P>We performed targeted re-sequencing to identify the genetic etiology of early-onset postlingual deafness and encountered a frequent <I>TMPRSS3</I> allele harboring two variants in a cis configuration. We aimed to evaluate the pathogenicity of the allele. Among 88 cochlear implantees with autosomal recessive non-syndromic hearing loss, subjects with <I>GJB2</I> and <I>SLC26A4</I> mutations were excluded. Thirty-one probands manifesting early-onset postlingual deafness were sorted. Through targeted re-sequencing, we detected two families with a <I>TMPRSS3</I> mutant allele containing p.V116M and p.V291L in a cis configuration, p.[p.V116M; p.V291L]. A minor allele frequency was calculated and proteolytic activity was measured. A p.[p.V116M; p.V291L] allele demonstrated a significantly higher frequency compared to normal controls and merited attention due to its high frequency (4.84%, 3/62). The first family showed a novel deleterious splice site variant—c.783-1G>A—in a trans allele, while the other showed homozygosity. The progression to deafness was noted within the first decade, suggesting DFNB10. The proteolytic activity was significantly reduced, confirming the severe pathogenicity. This frequent mutant allele significantly contributes to early-onset postlingual deafness in Koreans. For clinical implication and proper auditory rehabilitation, it is important to pay attention to this allele with a severe pathogenic potential.</P>
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