Two novel TMEM67 variations in a Chinese family with recurrent pregnancy loss: a case report

Author:

Pang Jialun1,Kong Fanjuan2,Tang Wanglan1,Xi Hui1,Ma Na1,Sheng Xiaoqi3,Peng Ying1,Liu Zhiyu2

Affiliation:

1. Department of Medical Genetics, Maternal and Child Health Hospital of Hunan Province

2. Department of Information Management, Maternal and Child Health Hospital of Hunan Province

3. NHC Key Laboratory of Birth Defect for Research and Prevention, Maternal and Child Health Hospital of Hunan Province

Abstract

Abstract Background:Recurrent pregnancy loss (RPL) is a common pregnancy complication that brings great pain to pregnant women and their families. Genetic factors are an important cause reason of RPL. However, clinical research on monogenic diseases with recurrent miscarriage is insufficient. Case presentation: Here we reported a Chinese family with RPL and genetic analysis of the abortion and parents. A paternally inherited heterozygous missense variant c.1415T>G (p.V472G) and a maternally inherited heterozygous nonsense variant c.2314del (p.M772*) in TMEM67gene were identified by trio-exome sequencing. c.2314del (p.M772*) generated a premature stop codon and truncated protein, was classified as “pathogenic”. c.1415T>G (p.V472G) located in extra-cellular region, was classified as “likely pathogenic”. Biallelic variants in TMEM67 gene cause lethal Meckel syndrome 3, consistent with the proband’s prenatal phenotype. Conclusion: The current study of the Chinese family expands the pathogenic variant spectrum of TMEM67and emphasizes the necessity of exome sequencing in RPL condition.

Publisher

Research Square Platform LLC

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