AI Article Synopsis

  • Multiple morphological anomalies of the sperm flagella (MMAF syndrome) is a serious cause of male infertility linked to mutations in several genes that affect sperm flagellum structure.
  • Research identified significant homozygous mutations in the QRICH2 gene, crucial for sperm flagellum development, in patients from two Chinese families and further analyzed a wider cohort to link QRICH2 to MMAF.
  • Out of 167 affected individuals, 1% had homozygous loss-of-function variants confirming QRICH2's role, while 9.6% had heterozygous variants, suggesting these variants are common and not specifically linked to MMAF syndrome.

Article Abstract

Multiple morphological anomalies of the sperm flagella (MMAF syndrome) is a severe male infertility phenotype which has so far been formally linked to the presence of biallelic mutations in nine genes mainly coding for axonemal proteins overexpressed in the sperm flagellum. Homozygous mutations in QRICH2, a gene coding for a protein known to be required for stabilizing proteins involved in sperm flagellum biogenesis, have recently been identified in MMAF patients from two Chinese consanguineous families. Here, in order to better assess the contribution of QRICH2 in the etiology of the MMAF phenotype, we analyzed all QRICH2 variants from whole exome sequencing data of a cohort of 167 MMAF-affected subjects originating from North Africa, Iran, and Europe. We identified a total of 14 potentially deleterious variants in 18 unrelated individuals. Two unrelated subjects, representing 1% of the cohort, carried a homozygous loss-of-function variant: c.3501C>G [p.Tyr1167Ter] and c.4614C>G [p.Tyr1538Ter], thus confirming the implication of QRICH2 in the MMAF phenotype and human male infertility. Sixteen MMAF patients (9.6%) carried a heterozygous QRICH2 potentially deleterious variant. This rate was comparable to what was observed in a control group (15.5%) suggesting that the presence of QRICH2 heterozygous variants is not associated with MMAF syndrome.

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Source
http://dx.doi.org/10.1111/cge.13604DOI Listing

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