| Literature DB >> 30628060 |
Zhihua Zhang1, Jian Mu1, Junli Zhao2, Zhou Zhou1, Biaobang Chen1, Ling Wu3, Zheng Yan3, Wenjing Wang1, Lin Zhao1, Jie Dong1, Xiaoxi Sun4, Yanping Kuang3, Bin Li3, Lei Wang5, Qing Sang1.
Abstract
Successful fertilization is fundamental for sexual reproduction. After undergoing a series of molecular and morphological changes, the haploid sperm fuses with the haploid oocyte to create a diploid zygote. Defects in this process might lead to human fertilization failure. We have previously found homozygous mutations in WEE2 that are responsible for human fertilization failure, but the genetic basis of human fertilization failure requires further investigation. In the present study, we screened for WEE2 mutations in a new cohort of patients with fertilization failure. Through Sanger sequencing of WEE2 exons, we identified seven novel mutations and two reported mutations in WEE2 from six affected individuals. Morphologically normal PB1 oocytes can be retrieved from all patients. However, most of the oocytes cannot be fertilized successfully. These findings confirmed our previous research and expanded the mutational spectrum of WEE2, making it a potential genetic diagnostic marker for those suffering from human fertilization failure.Entities:
Keywords: WEE2; human fertilization failure; mutation
Mesh:
Substances:
Year: 2019 PMID: 30628060 DOI: 10.1111/cge.13505
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438