A homozygous donor splice-site mutation in the meiotic gene MSH4 causes primary ovarian insufficiency

Premature ovarian insufficiency (POI) is a frequent pathology that affects women under 40 years of age, characterized by an early cessation of menses and high FSH levels. Despite recent progresses in molecular diagnosis, the etiology of POI remains idiopathic in most cases. Whole-exome sequencing of...

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Bibliographic Details
Published in:Human molecular genetics 2017-08, Vol.26 (16), p.3161
Main Authors: Carlosama, Carolina, Elzaiat, Maëva, Patiño, Liliana C, Mateus, Heidi E, Veitia, Reiner A, Laissue, Paul
Format: Article
Language:English
Subjects:
Adult
Cell Cycle Proteins - chemistry
Cell Cycle Proteins - genetics
Cell Cycle Proteins - metabolism
Cohort Studies
Exons
Female
Homozygote
Humans
Menopause, Premature - genetics
Mutation
Pedigree
Primary Ovarian Insufficiency - genetics
RNA Splice Sites
Whole Exome Sequencing
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Summary:Premature ovarian insufficiency (POI) is a frequent pathology that affects women under 40 years of age, characterized by an early cessation of menses and high FSH levels. Despite recent progresses in molecular diagnosis, the etiology of POI remains idiopathic in most cases. Whole-exome sequencing of members of a Colombian family affected by POI allowed us to identify a novel homozygous donor splice-site mutation in the meiotic gene MSH4 (MutS Homolog 4). The variant followed a strict mendelian segregation within the family and was absent in a cohort of 135 women over 50 years of age without history of infertility, from the same geographical region as the affected family. Exon trapping experiments showed that the splice-site mutation induced skipping of exon 17. At the protein level, the mutation p.Ile743_Lys785del is predicted to lead to the ablation of the highly conserved Walker B motif of the ATP-binding domain, thus inactivating MSH4. Our study describes the first MSH4 mutation associated with POI and increases the number of meiotic/DNA repair genes formally implicated as being responsible for this condition.
ISSN:0964-6906
1460-2083
DOI:10.1093/hmg/ddx199