Abstract

Oocyte maturation and fertilization are fundamental processes for successful human reproduction, and abnormalities in these processes will cause infertility. Recently, we identified biallelic mutations in <i>CDC20</i> that are responsible for human oocyte maturation arrest, fertilization failure, and early embryonic development arrest. In this study, we screened for further <i>CDC20</i> mutations in a new cohort of patients with abnormalities in oocyte maturation, fertilization, and early embryonic development. Through whole-exome sequencing, we identified the four novel mutations c.887G > A (p. Arg296Gln), c.964C > T (p.Arg322^∗), c.1155G > C (p.Trp385Cys), and c.330 + 1G > A (p. Glu111Ilefs^∗36) and one previously reported mutation c.965G > A (p.Arg322Gln) in <i>CDC20</i> in four infertile individuals from three independent families. The patients had different phenotypes of oocyte maturation arrest and fertilization failure resulting from the different mutations. This study confirms our previous research and expands the spectrum of known mutations in <i>CDC20</i>, providing new evidence supporting the function of <i>CDC20</i> in the genetic etiology of female infertility characterized by oocyte maturation arrest and fertilization failure.