Biallelic variants in MAD2L1BP ( p31 ^comet ) cause female infertility characterized by oocyte maturation arrest.

Publisher: eLife Sciences Publications, Ltd Country of Publication: England NLM ID: 101579614 Publication Model: Electronic Cited Medium: Internet ISSN: 2050-084X (Electronic) Linking ISSN: 2050084X NLM ISO Abbreviation: Elife Subsets: MEDLINE

Original Publication: Cambridge, UK : eLife Sciences Publications, Ltd., 2012-

Adaptor Proteins, Signal Transducing*/genetics ; Cell Cycle Proteins*/genetics ; Infertility, Female*/genetics ; Nuclear Proteins*/genetics; Animals ; Female ; Humans ; Mice ; Cell Cycle Checkpoints ; Exome Sequencing ; Mad2 Proteins ; Oocytes/cytology ; Young Adult ; Adult ; Meiosis

Human oocyte maturation arrest represents one of the severe conditions for female patients with primary infertility. However, the genetic factors underlying this human disease remain largely unknown. The spindle assembly checkpoint (SAC) is an intricate surveillance mechanism that ensures accurate segregation of chromosomes throughout cell cycles. Once the kinetochores of chromosomes are correctly attached to bipolar spindles and the SAC is satisfied, the MAD2L1BP, best known as p31 ^comet , binds mitosis arrest deficient 2 (MAD2) and recruits the AAA+-ATPase TRIP13 to disassemble the mitotic checkpoint complex (MCC), leading to the cell-cycle progression. In this study, by whole-exome sequencing (WES), we identified homozygous and compound heterozygous MAD2L1BP variants in three families with female patients diagnosed with primary infertility owing to oocyte metaphase I (MI) arrest. Functional studies revealed that the protein variants resulting from the C-terminal truncation of MAD2L1BP lost their binding ability to MAD2. cRNA microinjection of full-length or truncated MAD2L1BP uncovered their discordant roles in driving the extrusion of polar body 1 (PB1) in mouse oocytes. Furthermore, the patient's oocytes carrying the mutated MAD2L1BP resumed polar body extrusion (PBE) when rescued by microinjection of full-length MAD2L1BP cRNAs. Together, our studies identified and characterized novel biallelic variants in MAD2L1BP responsible for human oocyte maturation arrest at MI, and thus prompted new therapeutic avenues for curing female primary infertility.
Competing Interests: LH, WL, XD, SZ, BX, FW, RJ, LL, LW, XJ, YC, JZ, CX, XT, HF, HZ, JB No competing interests declared
(© 2023, Huang, Li, Dai et al.)

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Keywords: MAD2L1BP; developmental biology; genetics; genomics; human; meiosis; mouse; oocyte; oocyte maturation arrest

GEO GSE232488

0 (Adaptor Proteins, Signal Transducing)
0 (Cell Cycle Proteins)
0 (Mad2 Proteins)
0 (MAD2L1BP protein, human)
0 (Nuclear Proteins)

Date Created: 20230619 Date Completed: 20230822 Latest Revision: 20230822

20230823

PMC10319434

10.7554/eLife.85649

37334967