Novel NOBOX Loss-of-function Mutations Account for 6.2% of Cases in a Large Primary Ovarian Insufficiency Cohort

Overview

Journal Hum Mutat

Specialty Genetics

Date 2011 Aug 13

PMID 21837770

Citations 40

Authors

Justine Bouilly

Anne Bachelot

Isabelle Broutin

Philippe Touraine

Nadine Binart

Affiliations

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Abstract

Primary ovarian insufficiency (POI) is a disorder associated with female infertility, which affects approximately 1% of women under 40 years of age. A genetic component has been suggested as one possible cause of the majority of cases of nonsyndromic forms. Newborn Ovary Homeobox (NOBOX) is an ovary-specific gene, playing a critical role in ovary in mice, as its absence leads to sterility mimicking a POI. In this study, we sequenced NOBOX in a cohort of 178 women with idiopathic POI. Among 19 identified variations, we described one nonsense (c.907C>T/p.R303X) and four missense (c.271G>T/p.G91W, c.349C>T/p.R117W, c.1025G>C/p.S342T, and c.1048G>T/p.V350L) NOBOX heterozygous mutations in 12 patients. We reproduced each of the five mutations and tested their effects on the signaling activity in transfected cells. We demonstrated that these mutations compromised the ability of the proteins to bind to and transactivate the well-known growth differentiation factor 9 (GDF9) promoter. The pattern of our findings suggests that the genetic mechanism in humans responsible for POI in women involves haploinsufficiency rather than dominant negative gene action. The identification, characterization, and the very high 6.2% prevalence of these new mutations in POI patients suggest considering NOBOX as the first autosomal candidate gene involved in this syndrome.

Citing Articles

Oocyte/zygote/embryo maturation arrest: a clinical study expanding the phenotype of NOBOX variants.

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Primary ovarian insufficiency: update on clinical and genetic findings.

Federici S, Rossetti R, Moleri S, Munari E, Frixou M, Bonomi M Front Endocrinol (Lausanne). 2024; 15:1464803.

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Whole-genome de novo sequencing reveals genomic variants associated with differences of sex development in SRY negative pigs.

Wu J, Tan S, Feng Z, Zhao H, Yu C, Yang Y Biol Sex Differ. 2024; 15(1):68.

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Screening of premature ovarian insufficiency associated genes in Hungarian patients with next generation sequencing.

Illes A, Piko H, Arvai K, Donka V, Szepesi O, Kosa J BMC Med Genomics. 2024; 17(1):98.

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HNF1A gene mutations and premature ovarian failure (POF): evidence from a clinical paradigm combining MODY 3 and POF.

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