Bi-allelic missense variants in MEI4 cause preimplantation embryonic arrest and female infertility

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Abstract

Preimplantation embryonic arrest is an important pathogenesis of female infertility, but little is known about the genetic factors behind this phenotype. MEI4 is an essential protein for DNA double-strand break formation during meiosis, and Mei4 knock-out female mice are viable but sterile, indicating that MEI4 plays a crucial role in reproduction. To date, MEI4 has not been found to be associated with any human reproductive diseases. Here, we identified six compound heterozygous and homozygous MEI4 variants—namely, c.293C > T (p.Ser98Leu), c.401C > G (p.Pro134Arg), c.391C > G (p.Pro131Ala), c.914A > T (p.Tyr305Phe), c.908C > G (p.Ala303Gly), and c.899A > T (p.Gln300Leu)—in four independent families that were responsible for female infertility mainly characterized by preimplantation embryonic arrest. In vitro , we found that these variants reduced the interaction between MEI4 and DNA. In vivo , we generated a knock-in mouse model and demonstrated that female mice were infertile and were characterized by developmental defects during oogenesis. Our findings reveal the important roles of MEI4 in human reproduction and provide a new diagnostic marker for genetic counseling of clinical infertility patients.

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infertility

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europepmc
last seen: 2026-05-19T01:45:01.086888+00:00