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Merck

Mutations in eIF4ENIF1 are associated with primary ovarian insufficiency.

The Journal of clinical endocrinology and metabolism (2013-08-02)
Thushiga Kasippillai, Daniel G MacArthur, Andrew Kirby, Brett Thomas, Cornelius B Lambalk, Mark J Daly, Corrine K Welt
ABSTRAKT

Primary ovarian insufficiency (POI), or premature ovarian failure, results from ovarian follicle depletion with a consequent elevation of FSH levels before age 40 years. We identified a family in which 9 women in 3 consecutive generations developed menopause at approximately age 30 years. We hypothesized a genetic cause with a dominant mode of inheritance. This was a family-based genetic study and a replicate group of women with POI. The study was conducted at an academic medical center. Seven affected women and an obligate carrier and 7 unaffected family members were genotyped. The genes of interest were also sequenced in 38 unrelated women with POI. The DNA from 7 family members was subjected to whole-exome sequencing. The genotypes of interest were confirmed and genotypes of additional family members and unrelated women with POI were determined using Sanger sequencing. A high-impact, deleterious variant that segregated appropriately with POI in the family was required. A heterozygous stop codon (Ser429X) was identified in the eukaryotic translation initiation factor 4E nuclear import factor 1 (eIF4ENIF1) in the proband and all affected women but not in the unaffected family members. The chance that such a high-impact, deleterious variant would segregate appropriately among the affected and unaffected relatives by chance is very low (P < .05). There were no additional mutations identified in eIF4ENIF1 or eIF4E in 38 unrelated women with POI. Data demonstrate a new gene associated with dominantly inherited POI. These results highlight the importance of translation initiation factors and their regulators in ovarian function.