| Literature DB >> 30918116 |
Qing Sang1, Zhihua Zhang2, Juanzi Shi3, Xiaoxi Sun4, Bin Li5, Zheng Yan5, Songguo Xue6, Ai Ai5, Qifeng Lyu5, Wei Li7, Jilin Zhang7, Ling Wu5, Xiaoyan Mao5, Biaobang Chen2, Jian Mu2, Qiaoli Li2, Jing Du8, Qiang Sun7, Li Jin2, Lin He9, Shujia Zhu7, Yanping Kuang10, Lei Wang1,11.
Abstract
Connexins and pannexins are two protein families that play an important role in cellular communication. Pannexin 1 (PANX1), one of the members of pannexin family, is a channel protein. It is glycosylated and forms three species, GLY0, GLY1, and GLY2. Here, we describe four independent families in which mutations in PANX1 cause familial or sporadic female infertility via a phenotype that we term "oocyte death." The mutations, which are associated with oocyte death, alter the PANX1 glycosylation pattern, influence the subcellular localization of PANX1 in cultured cells, and result in aberrant PANX1 channel activity, ATP release in oocytes, and mutant PANX1 GLY1. Overexpression of a patient-derived mutation in mice causes infertility, recapitulating the human oocyte death phenotype. Our findings demonstrate the critical role of PANX1 in human oocyte development, provide a genetic explanation for a subtype of infertility, and suggest a potential target for therapeutic intervention for this disease.Entities:
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Year: 2019 PMID: 30918116 DOI: 10.1126/scitranslmed.aav8731
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956