Pathological variants in genes associated with disorders of sex development and central causes of hypogonadism in a whole-genome reference panel of 8380 Japanese individuals.

IF 1 Q4 GENETICS & HEREDITY Human Genome Variation Pub Date : 2022-09-28 DOI:10.1038/s41439-022-00213-w
Naomi Shiga, Yumi Yamaguchi-Kabata, Saori Igeta, Jun Yasuda, Shu Tadaka, Takamichi Minato, Zen Watanabe, Junko Kanno, Gen Tamiya, Nobuo Fuse, Kengo Kinoshita, Shigeo Kure, Akiko Kondo, Masahito Tachibana, Masayuki Yamamoto, Nobuo Yaegashi, Junichi Sugawara
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Abstract

Disorders of sex development (DSD) comprises a congenital condition in which chromosomal, gonadal, or anatomical sex development is atypical. In this study, we screened for pathogenic variants in 32 genes associated with DSDs and central causes of hypogonadism (CHG) in a whole-genome reference panel including 8380 Japanese individuals constructed by Tohoku Medical Megabank Organization. Candidate pathogenic (P) or likely pathogenic (LP) variants were extracted from the ClinVar, InterVar, and Human Gene Mutation databases. Ninety-one candidate pathological variants were found in 25 genes; 28 novel candidate variants were identified. Nearly 1 in 40 (either ClinVar or InterVar P or LP) to 157 (both ClinVar and InterVar P or LP) individuals were found to be carriers of recessive DSD and CHG alleles. In these data, genes implicated in gonadal dysfunction did not show loss-of-function variants, with a relatively high tendency of intolerance for haploinsufficiency based on pLI and Episcore, both of which can be used for estimating haploinsufficiency. We report the types and frequencies of causative variants for DSD and CHG in the general Japanese population. This study furthers our understanding of the genetic causes and helps to refine genetic counseling of DSD and CHG.

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在8380名日本人的全基因组参考小组中,与性发育障碍和性腺功能减退的主要原因相关的基因病理变异。
性发育障碍(DSD)包括染色体、性腺或解剖性发育不典型的先天性疾病。在这项研究中,我们筛选了32个与dsd和性腺功能减退(CHG)中心原因相关的基因的致病变异,其中包括由东北医学大银行组织构建的8380名日本人的全基因组参考小组。候选致病性(P)或可能致病性(LP)变异从ClinVar、InterVar和Human Gene Mutation数据库中提取。在25个基因中发现91个候选病理变异;鉴定出28种新的候选变异。近1 / 40 (ClinVar或InterVar P或LP)至157 (ClinVar和InterVar P或LP)个体被发现是隐性DSD和CHG等位基因的携带者。在这些数据中,与性腺功能障碍有关的基因没有显示出功能丧失变异,基于pLI和Episcore的单倍功能不全的不耐受倾向相对较高,两者都可以用于估计单倍功能不全。我们报告了日本普通人群中DSD和CHG致病变异的类型和频率。本研究进一步加深了我们对遗传原因的认识,有助于完善DSD和CHG的遗传咨询。
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来源期刊
Human Genome Variation
Human Genome Variation Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
2.30
自引率
0.00%
发文量
39
审稿时长
13 weeks
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