Most X;autosome translocations associated with premature ovarian failure do not interrupt X-linked genes

Prueitt, Robyn L.; Chen, H.; Barnes, R. Bowling; Zinn, Andrew R.

doi:10.1159/000064052

Cited by 66 publications

(47 citation statements)

References 22 publications

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“…Only the DIAPH2 gene, a human homolog of the Drosophila melanogaster diaphanous gene affecting spermatogenesis and oogenesis, was found disrupted by a breakpoint in a family with POI, but no mutation demonstrated its role in ovarian function nor that of the others candidates. However, most breakpoints described in POI patients were frequently mapped in Xq21, outside of genic regions, consistent with models for POI associated with X to autosome translocations that involve extra X chromosome effects (Mumm et al 2001, Prueitt et al 2002. These observations suggest the hypothesis that chromosomal rearrangements due to an epigenetic effect of the active X chromosome may account for a position effect on promoters of autosomal genes when involved in balanced translocations (Rizzolio et al 2007).…”

Section: Syndromic Poisupporting

confidence: 76%

Genes involved in human premature ovarian failure

Persani

Rossetti

Cacciatore

2010

Journal of Molecular Endocrinology

211

108

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Premature ovarian failure (POF) is an ovarian defect characterized by the premature depletion of ovarian follicles before the age of 40 years, representing one major cause of female infertility. POF relevance is continuously growing because women tend to conceive ever more frequently in their thirties and forties. POF can present very early with a pubertal defect. More frequently, it is the end stage of an occult process (primary ovarian insufficiency, POI) affecting w1-2% of under-40 women. POI is a heterogeneous disease caused by a variety of mechanisms. Though the underlying cause remains unexplained in the majority of cases, various data indicate that POI has a strong genetic component. These data include the existence of several causal genetic defects in humans, experimental and natural models, as well as the frequent familiarity. The variable expressivity of POI defect in women of the same family may indicate that, in addition to some monogenic forms, POI may frequently be considered as a multifactorial defect resulting from the contribution of several predisposing alleles. The X chromosome-linked defects play a major role among the presently known causal defects. Here, we review the principal X-linked and autosomal genes involved in syndromic and nonsyndromic forms of POI with the wish that this list will soon become upgraded because of the discovery of novel contributing mechanisms. A better understanding of POI pathogenesis will indeed allow the construction of tests able to predict the age of menopause in women at higher risk of POI.

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Section: Syndromic Poisupporting

confidence: 76%

Genes involved in human premature ovarian failure

Persani

Rossetti

Cacciatore

2010

Journal of Molecular Endocrinology

211

108

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“…32 Molecular mapping of several of these breakpoints have shown that they are scattered over the entire critical region, supporting the idea that integrity of a specific chromosomal domain may be important for the development of female germ cells. 33 Since the chromosome 1 breakpoints in male infertility do not seem to be associated with any specific chromosomal region(s), either at the cytogenetic or at the molecular level, we suggest that chromosome 1 harbours a large chromosomal domain, the integrity of which is important for normal spermatogenesis.…”

Section: Discussionmentioning

confidence: 81%

An excess of chromosome 1 breakpoints in male infertility

et al. 2004

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3 -48 Full affiliations can be seen as electronic supplementIn a search for potential infertility loci, which might be revealed by clustering of chromosomal breakpoints, we compiled 464 infertile males with a balanced rearrangement from Mendelian Cytogenetics Network database (MCNdb) and compared their karyotypes with those of a Danish nation-wide cohort. We excluded Robertsonian translocations, rearrangements involving sex chromosomes and common variants. We identified 10 autosomal bands, five of which were on chromosome 1, with a large excess of breakpoints in the infertility group. Some of these could potentially harbour a male-specific infertility locus. However, a general excess of breakpoints almost everywhere on chromosome 1 was observed among the infertile males: 26.5 versus 14.5% in the cohort. This excess was observed both for translocation and inversion carriers, especially pericentric inversions, both for published and unpublished cases, and was significantly associated with azoospermia. The largest number of breakpoints was reported in 1q21; FISH mapping of four of these breakpoints revealed that they did not involve the same region at the molecular level. We suggest that chromosome 1 harbours a critical domain whose integrity is essential for male fertility.

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“…[Cremers et al 1990], and DIAPH2 (MIM * 300108) in Xq22 [Bione et al 1998]. However, most of the breakpoints mapped in the Xq region described in POF patients are intergenic [Mumm et al 2001;Prueitt et al 2002]. Only the DIAPH2 gene was disrupted by translocation in a family with POF affecting oogenesis [Bione et al 1998].…”

Section: Resultsmentioning

confidence: 99%

Disruption ofHDXgene in premature ovarian failure

Ökten

Güneş

Onat

et al. 2013

Systems Biology in Reproductive Medicine

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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.

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Most X;autosome translocations associated with premature ovarian failure do not interrupt X-linked genes

Cited by 66 publications

References 22 publications

Genes involved in human premature ovarian failure

Genes involved in human premature ovarian failure

An excess of chromosome 1 breakpoints in male infertility

Disruption ofHDXgene in premature ovarian failure

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