Disruption of HDX gene in premature ovarian failure.

We present a case of a 19-year-old phenotypically normal girl with premature ovarian failure. Cytogenetic analysis using G banding and fluorescence in situ hybridization (FISH) from cultured peripheral blood lymphocytes of the patient and the family revealed a de novo X;15 translocation and the imbalance to be 46,X,t(X;15)(Xpter → Xq21::15q11 → 15qter;15pter → 15q11::Xq21 → Xqter). ish (CEPX+, wep15+, ISNRPN+, PML+, D15S10+, wcp15-, SNRRN-, PML-)[20]. The X chromosome inactivation (XCI) assay revealed a completely skewed XCI pattern in which selective pressure favors an active maternal allele. The Affymetrix 2.7 M cytogenetics whole-Genome array confirmed the chromosomal imbalance and identified disruption of the HDX gene at Xq21, the translocation breakpoint. PMID: 23441923 [PubMed - as supplied by publisher]

http://www.ncbi.nlm.nih.gov/pubmed/23441923?dopt=Abstract

Source: Systems Biology in Reproductive Medicine - February 26, 2013 Category: Reproduction Medicine Authors: Okten G, Gunes S, Onat OE, Tukun A, Ozcelik T, Kocak I Tags: Syst Biol Reprod Med Source Type: research