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‘Isolated’ germline mosaicism in the phenotypically normal father of a girl with X-linked hypophosphatemic rickets

苯丙氨酸 桑格测序 先证者 嵌合体 生殖系 遗传学 复合杂合度 生物 低磷血症性佝偻病 遗传咨询 佝偻病 等位基因 身材矮小 突变 内分泌学 基因 维生素D与神经学
作者
Yunting Lin,Yanna Cai,Jianan Xu,Chunhua Zeng,Huiying Sheng,Yu Yang,Xiuzhen Li,Li Liu
出处
期刊:European journal of endocrinology [Oxford University Press]
卷期号:182 (1): K1-K6 被引量:10
标识
DOI:10.1530/eje-19-0472
摘要

X-linked hypophosphatemic rickets (XLHR) is the most common form of inherited rickets caused by pathogenic variants of PHEX gene with an X-linked dominant inheritance pattern. Precise molecular diagnosis of pathogenic variant will benefit the genetic counseling and prenatal diagnosis for the family with XLHR. Here, we presented an 'isolated' germline mosaicism in the phenotypically normal father of a girl with XLHR.For the initial molecular screen of PHEX gene, DNA samples of the proband and her parents were extracted from their peripheral blood samples respectively. Sanger sequencing found a 'de novo' novel heterozygous variant, c.1666C>T(p.Q556X), at the PHEX gene in the proband, but not in her phenotypically healthy parents. Due to an occasional abnormality of his serum phosphate previously, further examinations for the father were taken to exclude the possibility of paternal mosaicism. Eight samples from different tissues were analyzed for PHEX gene by Sanger sequencing. Surprisingly, one 'isolated' germline mosaicism was detected only in his sperm with an estimated frequency of 26.67%. The mosaic allele was identical to the c.1666C>T(p.Q556X) variant in the proband.This is the first case of 'isolated' germline mosaicism with pathogenic PHEX variant. Our study provides accurate diagnosis and valuable counseling for this family. This report also alerts clinicians and geneticists to exclude the possibility of the isolated germline mosaicism and prevent intrafamilial recurrences of inherited diseases.

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