Three patients with 9p deletions including DMRT1 and DMRT2: A girl with XY complement, bilateral ovotestes, and extreme growth retardation, and two XX females with normal pubertal development

Õunap, Katrin; Uibo, Oivi; Žordania, Riina; Kiho, Liina; Ilus, Tiiu; Õiglane-Shlik, Eve; Bartsch, Oliver

doi:10.1002/ajmg.a.30269

Cited by 68 publications

(40 citation statements)

References 29 publications

(56 reference statements)

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“…It is not clear why one deletion (present case) is associated with ovotesticular DSD and the other deletion with XY gonadal dysgenesis. The size of the deletion does not explain the different phenotypes as Õ unap et al (23) reported on a patient with bilateral ovotestes and an unbalanced translocation 46,XY,der(9)t(7;9)(q32;p24) leading to a deletion of DMRT1/DMRT2.…”

Section: Discussionmentioning

confidence: 94%

Partial deletion of DMRT1 causes 46,XY ovotesticular disorder of sexual development

Ledig¹,

Hiort²,

Wünsch³

et al. 2012

European Journal of Endocrinology

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Objective: Ovotesticular disorder of sexual development (DSD) is an unusual form of DSD, characterized by the coexistence of testicular and ovarian tissue in the same individual. In a subset of patients, ovotesticular DSD is caused by 46,XX/46,XY chimerism or mosaicism. To date, only a few monogenetic causes are known to be associated with XX and XY ovotesticular DSD. Design and methods: Clinical, hormonal, and histopathological data, and results of high-resolution array-comparative genomic hybridization (CGH) were obtained from a female patient with 46,XY ovotesticular DSD with testicular tissue on one side and an ovary harboring germ cells on the other. Results obtained by array-CGH were confirmed by RT-quantitative PCR. Results: We detected a deletion of w35 kb affecting exons 3 and 4 of the DMRT1 gene in a female patient with 46,XY ovotesticular DSD. To the best of our knowledge, this is the smallest deletion affecting DMRT1 presented to this point in time. Conclusions: We suggest that haploinsufficiency of DMRT1 is sufficient for both XY gonadal dysgenesis and XY ovotesticular DSD. Furthermore, array-CGH is a very useful tool in the molecular diagnosis of DSD.

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Section: Discussionmentioning

confidence: 94%

Partial deletion of DMRT1 causes 46,XY ovotesticular disorder of sexual development

Ledig¹,

Hiort²,

Wünsch³

et al. 2012

European Journal of Endocrinology

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“…Second, DMRT1 was expressed exclusively in testes among 50 investigated human tissues. Further evidence for DMRT1 as a male sexual regulator came either from the later studies of its expression in human embryos (Moniot et al, 2000) or from additional reports describing sex-reversed patients with the monosomy of 9p (Raymond et al, 1999a;Muroya et al, 2000;Õunap et al, 2004;Privitera et al, 2005;Vinci et al, 2007). In the meantime, the group of Zarkower from the University of Minnesota (Raymond et al, 1999b) and the group of Sinclair from the University of Melbourne (Smith et al, 1999a) published very important data about DMRT1 expression during mouse, chicken and alligator embryogenesis.…”

Section: Dmrt -Vertebrate Dm Domain Gene Familymentioning

confidence: 99%

DM Domain Genes: Sexual and Somatic Development During Vertebrate Embryogenesis

Bratuś¹

2012

Embryogenesis

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“…1D). The deletion of human DM genes on chromosome 9p is associated with intersexual development (6,27,31,49,55,59,63). Although originally described in relation to sex-determining pathways (67), an extended family of DM genes is proposed to function in general aspects of developmental patterning in vertebrates (35).…”

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confidence: 99%

Regulation of Sexual Dimorphism: Mutational and Chemogenetic Analysis of the Doublesex DM Domain

Zhang

Singh

et al. 2006

Molecular and Cellular Biology

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Doublesex (dsx) is a transcription factor in Drosophila that regulates somatic sexual differentiation. Maleand female-specific splicing isoforms of DSX share a novel DNA-binding domain, designated the DM motif. Broadly conserved among metazoan sex-determining factors, the DM domain contains a nonclassical zinc module and binds in the DNA minor groove. Here, we characterize the DM motif by site-directed and random mutagenesis using a yeast one-hybrid (Y1H) system and extend this analysis by chemogenetic complementation in vitro. The Y1H system is based on a sex-specific Drosophila enhancer element and validated through studies of intersexual dsx mutations. We demonstrate that the eight motif-specific histidines and cysteines engaged in zinc coordination are each critical and cannot be interchanged; folding also requires conserved aliphatic side chains in the hydrophobic core. Mutations that impair DNA binding tend to occur at conserved positions, whereas neutral substitutions occur at nonconserved sites. Evidence for a specific salt bridge between a conserved lysine and the DNA backbone is obtained through the synthesis of nonstandard protein and DNA analogs. Together, these results provide molecular links between the structure of the DM domain and its function in the regulation of sexual dimorphism.Sexual dimorphism is regulated by diverse molecular mechanisms (18). In mammals, male development is initiated by a gene on the Y chromosome that is designated Sry (sex-determining region of the Y chromosome) (7,30,41,42). Alternative genetic mechanisms operate in Drosophila melanogaster (and Caenorhabditis elegans), wherein sex is determined by the X-to-autosome ratio, a process linked to X-dosage compensation (Fig. 1A) (19, 59). The sex-determining hierarchy of Drosophila defines an RNA-splicing cascade through the actions of Sex Lethal (SXL) and the TRA factors (18). Doublesex (dsx) functions downstream of this cascade to define one branch of a ramifying pathway (Fig. 1A) (29,59). The sex-specific isoforms of DSX (DSX M and DSX F ; Fig. 1B) regulate most aspects of somatic sexual dimorphism in D. melanogaster. These isoforms share an N-terminal DNA-binding domain, designated the DM motif (Fig. 1C). In this article, we present a mutational analysis of the DSX DM domain to identify key determinants of folding and DNA recognition.The Wilkins-Wolf hypothesis posits that sex-determining pathways have evolved in a reverse order from bottom (most broadly conserved) to top (least conserved) (65, 66). This viewpoint is supported by the ubiquity of DM genes among metazoan sex-determining pathways (35, 59). Such genes encode a newly recognized class of transcription factors (for a review, see reference 59). DM sequences are broadly conserved in metazoans, including nematodes, fish, reptiles, birds, and mammals (Fig. 1D). The deletion of human DM genes on chromosome 9p is associated with intersexual development (6,27,31,49,55,59,63). Although originally described in relation to sex-determining pathways (67), an extended family...

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Three patients with 9p deletions including DMRT1 and DMRT2: A girl with XY complement, bilateral ovotestes, and extreme growth retardation, and two XX females with normal pubertal development

Cited by 68 publications

References 29 publications

Partial deletion of DMRT1 causes 46,XY ovotesticular disorder of sexual development

Partial deletion of DMRT1 causes 46,XY ovotesticular disorder of sexual development

DM Domain Genes: Sexual and Somatic Development During Vertebrate Embryogenesis

Regulation of Sexual Dimorphism: Mutational and Chemogenetic Analysis of the Doublesex DM Domain

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