Search

Your search keyword '"xx male"' showing total 12 results
Start Over Descriptor "xx male" Database OpenAIRE
12 results on '"xx male"'

1. Multiscale analysis of SRY‐positive 46,XX testicular disorder of sex development: Presentation of nine cases

Author

Sezgin Gunes, Gonul Ogur, Omer Salih Akar, Onur Emre Onat, Tayfun Ozcelik, Ramazan Asci, Ummet Abur, Engin Altundag, Onat, Onur Emre, and Özçelik, Tayfun

Subjects
Male, medicine.medical_specialty, Array-CGH, Urology, Pseudoautosomal region, Biology, Y chromosome, Testicular Diseases, Translocation, Genetic, X-inactivation, Endocrinology, Hypergonadotropic hypogonadism, XX male, Internal medicine, medicine, Humans, Genes, sry, X chromosome, Azoospermia, Karyotype, General Medicine, medicine.disease, Phenotype, Testis determining factor, Karyotyping, Infertility, X chromosome inactivation, SRY-positive 46
Abstract

46,XX testicular disorder of sex development (46,XX TDSD) is a relatively rare condition characterised by the presence of testicular tissue with 46,XX karyotype. The present study aims to reveal the phenotype to genotype correlation in a series of sex-determining region Y (SRY)-positive 46,XX TDSD cases. We present the clinical findings, hormone profiles and genetic test results of six patients with SRY-positive 46,XX TDSD and give the details and follow-up findings of our three of previously published patients. All patients presented common characteristics such as azoospermia, hypergonadotropic hypogonadism and an SRY gene translocated on the terminal part of the short arm of one of the X chromosomes. Mean ± standard deviation (SD) height of the patients was 164.78 ± 8.0 cm. Five patients had decreased secondary sexual characteristics, and three patients had gynaecomastia with varying degrees. Five of the seven patients revealed a translocation between protein kinase X (PRKX) and inverted protein kinase Y (PRKY) genes, and the remaining two patients showed a translocation between the pseudoautosomal region 1 (PAR1) of X chromosome and the differential region of Y chromosome. X chromosome inactivation (XCI) analysis results demonstrated random and skewed XCI in 5 cases and 1 case, respectively. In brief, we delineate the phenotypic spectrum of patients with SRY-positive 46,XX TDSD and the underlying mechanisms of Xp;Yp translocations.

Published
2020

2. NR5A1 is a novel disease gene for 46,XX testicular and ovotesticular disorders of sex development

Author

Toon Rosseel, Anne-Laure Todeschini, Reiner A. Veitia, Leendert H. J. Looijenga, Frank Peelman, Dorien Baetens, Frauke Coppieters, Hans Stoop, Elfride De Baere, Martine Cools, and Pathology

Subjects
0301 basic medicine, Male, Models, Molecular, XX MALE, Steroidogenic Factor 1, OVARIAN INSUFFICIENCY, 0302 clinical medicine, STEROIDOGENIC FACTOR-1, Gene duplication, Testis, Medicine and Health Sciences, XX DSD, Missense mutation, RNA-SEQ, Disorders of sex development, Original Research Article, Genetics (clinical), Nuclear Proteins, Pedigree, Up-Regulation, DNA-Binding Proteins, medicine.anatomical_structure, Female, TRUE HERMAPHRODITISM, medicine.medical_specialty, endocrine system, Gonad, gonadal development, Testicular Disorder, Mutation, Missense, NR5A1, 030209 endocrinology & metabolism, Biology, 46,XX DSD, Polymorphism, Single Nucleotide, NUCLEAR RECEPTOR, Andrology, 03 medical and health sciences, Young Adult, Internal medicine, Exome Sequencing, medicine, True hermaphroditism, Humans, PARTIAL DUPLICATION, Genetic Predisposition to Disease, testicular DSD, MUTATIONS, Sequence Analysis, RNA, Gene Expression Profiling, Haplotype, Ovary, Biology and Life Sciences, medicine.disease, Ovotesticular Disorders of Sex Development, Gene expression profiling, 030104 developmental biology, Endocrinology, Haplotypes, ADRENAL INSUFFICIENCY, ovotesticular DSD, Transcription Factors
Abstract

Purpose: We aimed to identify the genetic cause in a cohort of 11 unrelated cases and two sisters with 46,XX SRY-negative (ovo)testicular disorders of sex development (DSD). Methods: Whole-exome sequencing (n = 9), targeted resequencing (n = 4), and haplotyping were performed. Immunohistochemistry of sex-specific markers was performed on patients' gonads. The consequences of mutation were investigated using luciferase assays, localization studies, and RNA-seq. Results: We identified a novel heterozygous NR5A1 mutation, c.274C>T p.(Arg92Trp), in three unrelated patients. The Arg92 residue is highly conserved and located in the Ftz-F1 region, probably involved in DNA-binding specificity and stability. There were no consistent changes in transcriptional activation or subcellular localization. Transcriptomics in patient-derived lymphocytes showed upregulation of MAMLD1, a direct NR5A1 target previously associated with 46,XY DSD. In gonads of affected individuals, ovarian FOXL2 and testicular SRY-independent SOX9 expression observed. Conclusions: We propose NR5A1, previously associated with 46,XY DSD and 46,XX primary ovarian insufficiency, as a novel gene for 46,XX (ovo)testicular DSD. We hypothesize that p.(Arg92Trp) results in decreased inhibition of the male developmental pathway through downregulation of female antitestis genes, thereby tipping the balance toward testicular differentiation in 46,XX individuals. In conclusion, our study supports a role for NR5A1 in testis differentiation in the XX gonad. Genet Med 19 4, 367–376.

Published
2017

4. La gestione clinica dei maschi 46,XX

Author

Francesco Lombardo, Francesco Pallotti, and Andrea Sansone

Subjects
XX male, business.industry, testosterone, Medicine, terapia, 46,XX male, business, Humanities
Published
2018

5. Disorders of sexual development: understanding the basics

Author

Abdulkadir A

Subjects
ambiguous genitalia, Medicine (General), intersex, RK1-715, hermaphroditism, xy female, R5-920, Dentistry, disorder of sexual differentiation, Pathophysiology, management, intersex, disorder of sexual differentiation, hermaphroditism, pseudohermaphroditism, ambiguous genitalia, XX male, XY female, pseudohermaphroditism, xx male, pathophysiology, management
Abstract

The enthusiasms on 'intersex' have been with humanity since antique. Inadequacies in the management of the condition backwash in Psychosocial and medical morbidities with occasional mortality. The upsurge in the knowledge of its pathophysiology over generations has incredibly improved the management outcome. This study aims to present the fundamentals of the Pathophysiology and Management of DSD. The information provided is intended to guide in the basic evaluation and care of individuals with the disorder. Material and Method:Search from PubMed, EMBASE and AJOL for Literature on Disorders of Sexual development was reviewed. The search words were; intersex, the disorder of sexual differentiation (DSD), Pseudohermaphroditism, Hermaphroditism and Ambiguous genitalia. The literature on the Pathophysiology and the managementwas appraised and summarized. Conclusion:Genetic inquest and advances in molecular biology had provided cognizance on the pathophysiology of DSD. Patient's advocacy groups and denovo medical ethics necessitated the transformations in the approach to the management.

Published
2016

6. 46,XX, der(15),t(Y;15)(q12;p11) karyotype in an azoospermic male

Author

Serap Tutgun Onrat, Muhsin Elmas, and Zafer Söylemez

Subjects
Azoospermia, Genetics, Proband, congenital, hereditary, and neonatal diseases and abnormalities, medicine.diagnostic_test, Derivative chromosome, azoospermia, Chromosomal translocation, Karyotype, Case Report, Fluorescence In Situ Hybridization, Biology, medicine.disease, Molecular biology, Yq, 15p translocation, Hypergonadotropic hypogonadism, XX male, medicine, Klinefelter syndrome, infertility, Genetics (clinical), Fluorescence in situ hybridization
Abstract

We report on a Yq/15p translocation in a 23-year-old infertile male referred for Klinefelter Syndrome testing, who had azoospermia and bilateral small testes. Hormonal studies revealed hypergonadotropic hypogonadism. Conventional cytogenetic procedures giemsa trypsin giemsa (GTG) and high resolution banding (HRB) and molecular cytogenetic techniques Fluorescence In Situ Hybridization (FISH) performed on high-resolution lymphocyte chromosomes revealed the karyotype 46,XX, t(Y;15)(q12;p11). SRY-gene was confirmed to be present by classical Polymerase Chain Reaction (PCR) methods. His father carried de novo derivative chromosome 15 [45,X, t(Y;15)(q12;p11)] and was fertile; the karyotype of the father using G-band technique confirmed a reciprocal balanced translocation between chromosome Y and 15. In the proband, the der (15) has been inherited from the father because the mother had a normal karyotype (46,XX). In the proband, the der (15) could have produced genetic imbalance leading to unbalanced robertson translocation between chromosome Y and 15, which might have resulted in azoospermia and infertility in the proband. The paternal translocation might have lead to formation of imbalanced ova, which might be resulted infertility in the proband. Sister's karyotypes was normal (46,XX) while his brother was not analyzed.

Published
2012

7. Identification of SOX3 as an XX male sex reversal gene in mice and humans

Author

Dale McAninch, Vincent R. Harley, Valerie A. Arboleda, Paul Q. Thomas, Henrik Bengtsson, Eric Vilain, Jennie Slee, Karine Rizzoti, Ryohei Sekido, João Gonçalves, Edwina Sutton, Jacqueline Tan, Helen J. Eyre, Robin Lovell-Badge, D L Bruno, James N. Hughes, Erin Turbitt, Kevin Christopher Knower, Stefan J. White, L. Rowley, Nicholas Rogers, and Andrew H. Sinclair

Subjects
Male, 46, XX Testicular Disorders of Sex Development, Male sex determination, Reversão Sexual, Regulatory Sequences, Nucleic Acid, Mice, 0302 clinical medicine, Pregnancy, Testis, Gene Rearrangement, Regulation of gene expression, Genetics, 0303 health sciences, Sex Reversal, Gene Expression Regulation, Developmental, SOX9 Transcription Factor, General Medicine, Sex reversal, Doença Genéticas, Up-Regulation, medicine.anatomical_structure, Testis determining factor, SOX3, Female, SOX9, Research Article, Homem XX, Adult, Gonad, Transgene, Mice, Transgenic, Biology, Y chromosome, Aldehyde Dehydrogenase 1 Family, 03 medical and health sciences, SRY, medicine, Animals, Humans, DNA Primers, 030304 developmental biology, Sertoli Cells, Base Sequence, SOXB1 Transcription Factors, Infant, Retinal Dehydrogenase, Sex Determination, Gene rearrangement, Aldehyde Dehydrogenase, XX Male, Mice, Inbred C57BL, Disease Models, Animal, Mice, Inbred CBA, Determinação do Sexo, 030217 neurology & neurosurgery
Abstract

Sex in mammals is genetically determined and is defined at the cellular level by sex chromosome complement (XY males and XX females). The Y chromosome-linked gene sex-determining region Y (SRY) is believed to be the master initiator of male sex determination in almost all eutherian and metatherian mammals, functioning to upregulate expression of its direct target gene Sry-related HMG box-containing gene 9 (SOX9). Data suggest that SRY evolved from SOX3, although there is no direct functional evidence to support this hypothesis. Indeed, loss-of-function mutations in SOX3 do not affect sex determination in mice or humans. To further investigate Sox3 function in vivo, we generated transgenic mice overexpressing Sox3. Here, we report that in one of these transgenic lines, Sox3 was ectopically expressed in the bipotential gonad and that this led to frequent complete XX male sex reversal. Further analysis indicated that Sox3 induced testis differentiation in this particular line of mice by upregulating expression of Sox9 via a similar mechanism to Sry. Importantly, we also identified genomic rearrangements within the SOX3 regulatory region in three patients with XX male sex reversal. Together, these data suggest that SOX3 and SRY are functionally interchangeable in sex determination and support the notion that SRY evolved from SOX3 via a regulatory mutation that led to its de novo expression in the early gonad.

Published
2011

8. Testis development in the absence of SRY: chromosomal rearrangements at SOX9 and SOX3

Author

Gianni Russo, Pietro Palumbo, Maurizio Merico, Alexis Parada-Bustamante, Emmanouil Manolakos, M. Chaabouni, Silvana Beri, Orsetta Zuffardi, Mohammadreza Dehghani, Leopoldo Zelante, Paola Grammatico, Roberto Giorda, Massimo Carella, Laura Cardarelli, Lilia Kraoua, Maria Clara Bonaglia, Annalisa Vetro, Alfredo Brusco, Orietta Radi, Francesca Forzano, Orazio Palumbo, Marjan Sabaghian, Andrea Castro, Savino Calvano, Mohamed Basly, Sabrina Giglio, Giovanna Camerino, and Crystalena Sofocleous

Subjects
Adult, Male, sex reversal, XX male, sox3, sox9, 46, XX Disorders of Sex Development, Context (language use), Chromosomal translocation, Biology, Article, Translocation, Genetic, Chromosome Breakpoints, Gene duplication, Testis, Genetics, medicine, Humans, Disorders of sex development, Genetics (clinical), X chromosome, Chromosomes, Human, X, SOXB1 Transcription Factors, Breakpoint, Infant, Newborn, Chromosome, SOX9 Transcription Factor, medicine.disease, Testis determining factor, Testis development, SOX9, SOX3, Female, Chromosomes, Human, Pair 17
Abstract

Duplications in the ~2 Mb desert region upstream of SOX9 at 17q24.3 may result in familial 46,XX disorders of sex development (DSD) without any effects on the XY background. A balanced translocation with its breakpoint falling within the same region has also been described in one XX DSD subject. We analyzed, by conventional and molecular cytogenetics, 19 novel SRY-negative unrelated 46,XX subjects both familial and sporadic, with isolated DSD. One of them had a de novo reciprocal t(11;17) translocation. Two cases carried partially overlapping 17q24.3 duplications ~500 kb upstream of SOX9, both inherited from their normal fathers. Breakpoints cloning showed that both duplications were in tandem, whereas the 17q in the reciprocal translocation was broken at ~800 kb upstream of SOX9, which is not only close to a previously described 46,XX DSD translocation, but also to translocations without any effects on the gonadal development. A further XX male, ascertained because of intellectual disability, carried a de novo cryptic duplication at Xq27.1, involving SOX3. CNVs involving SOX3 or its flanking regions have been reported in four XX DSD subjects. Collectively in our cohort of 19 novel cases of SRY-negative 46,XX DSD, the duplications upstream of SOX9 account for ~10.5% of the cases, and are responsible for the disease phenotype, even when inherited from a normal father. Translocations interrupting this region may also affect the gonadal development, possibly depending on the chromatin context of the recipient chromosome. SOX3 duplications may substitute SRY in some XX subjects.

Published
2015

9. 46,XX Male Disorder of Sexual Development: A Case Report

Author

Ahmet Anık, Ece Böber, Ayhan Abaci, and Gönül Çatlı

Subjects
Male, Infertility, Gonad, 46, XX Disorders of Sex Development, Adolescent, Endocrinology, Diabetes and Metabolism, Karyotype, Case Report, Disorder of sexual development, Biology, Y chromosome, Translocation, Genetic, Andrology, XX male, Endocrinology, Testis, Male external genitalia, medicine, Humans, Genes, sry, In Situ Hybridization, Fluorescence, SRY gene, Chromosomes, Human, X, medicine.diagnostic_test, Embryo, Organ Size, medicine.disease, medicine.anatomical_structure, Testis determining factor, Karyotyping, Pediatrics, Perinatology and Child Health, Fluorescence in situ hybridization
Abstract

The main factor influencing sex determination of an embryo is the sex-determining region Y (SRY), a master regulatory gene located on the Y chromosome. The presence of SRY causes the bipotential gonad to differentiate into a testis. However, some individuals carry a Y chromosome but are phenotypically female (46,XY females) or have a female karyotype but are phenotypically male (46,XX males). 46, XX male is rare (1:20 000 in newborn males), and SRY positivity is responsible for this condition in approximately 90% of these subjects. External genitalia of 46,XX SRY-positive males appear as normal male external genitalia, and such cases are diagnosed when they present with small testes and/or infertility after puberty. Herein, we report an adolescent who presented with low testicular volume and who was diagnosed as a 46,XX male. SRY positivity was demonstrated in the patient by fluorescence in situ hybridization method. Key words: Disorder of sexual development, XX male, SRY gene

Published
2013

10. A CASE OF SEX REVERSAL SYNDROME WITH SEX-DETERMINING REGION (XX MALE)

Author

YAMAMOTO, MASANORI, YOKOI, KEISUKE, KATSUNO, SATOSHI, HIBI, HATSUKI, and MIYAKE, KOJI

Subjects
endocrine system, XX male, urogenital system, Infertility, Sex determining region
Abstract

We examined a 32-year-old man with a 4-year history of infertility. The man's sex life, male hair pattern, and penis were normal, and he had no history of erection problems. Left and right testicular volumes were 2 ml and 3 ml, respectively. Semen analysis showed no sperm. The endocrine panel revealed increased serum luteinizing hormone and follicle-stimulating hormone levels, and a normal serum testosterone level. A testicular biopsy demonstrated that both Leydig cell and Sertoli cell hyperplasia were present, and that no germ cells were found in the tubules. A chromosome analysis done on the peripheral blood lymphocytes revealed a karyotype of 46, XX. We identified the sex-determining region, Y, by polymerase chain reaction using Y-specific probes in this patient. The diagnosis was XX male.

Published
1995

11. Homem XX: relato de três casos na faixa etária pediátrica

Author

Damiani, Durval, Guedes, Dulce Rondina, Damiani, Daniel, Dichtchekenian, Vaê, Coelho Neto, José Rodrigues, Maciel-Guerra, Andréa Trevas, Guerra-Júnior, Gil, Mello, Maricilda Palandi de, and Setian, Nuvarte

Subjects
Diferenciação sexual, Homem XX, Testículo, XX male, Infertility, Intersex, Testes, Intersexo, Sexo reverso, Sex differentiation, Sex reversal, Infertilidade
Abstract

São apresentados três pacientes com a condição clínica conhecida como "homem XX", rara na faixa etária pediátrica, caracterizada por um fenótipo masculino (em geral não associado a ambigüidade genital), testículos, porém cariótipo 46,XX. O diagnóstico costuma ser feito no adulto devido à esterilidade; na faixa etária pediátrica, ele é feito nos casos com ambigüidade genital ou ginecomastia. Na maioria dos pacientes é detectado o gene SRY (Sex-determining Region of the Y chromosome), o que explica a diferenciação testicular, porém em 20% dos casos ele está ausente, o que torna evidente que a determinação gonadal é um processo dependente de múltiplos genes e fatores de transcrição. O diagnóstico de apenas 3 casos em dois serviços de referência num período de quase 30 anos indica sua raridade entre os casos de anomalias da diferenciação sexual. We report on three patients with the clinical condition known as "XX male", which is uncommon in the pediatric age group. Patients have a male phenotype (usually without ambiguous genitalia) and testes; however, the karyotype is 46,XX. The diagnosis is usually made in adult life due to infertility; it may also be done by the pediatrician when there is ambiguous genitalia or gynecomastia. The SRY gene (Sex-determining Region of the Y chromosome) is detected in most cases, thus explaining the origin of testicular development; however, it is absent in 20% of the cases, thus indicating that gonadal determination is a complex process which depends on the interaction of many genes and transcription factors. The finding of only 3 cases in two reference services in a 30-year period indicates the rarity of this disorder among intersex cases.

Published
2005

12. An Sry-Positive 46,XX Male

Author

S Virk, Anupam Kaur, Jai Rup Singh, Surbhi Mahajan, and K Sachdeva

Subjects
Testis determining factor, azoospermia, Genetics, infertile, QH426-470, Biology, xx male, Genetics (clinical)
Abstract

An Sry-Positive 46,XX MaleThe 46,XX karyotype in a male is a rare sex chromosomal disorder. It mostly results from unequal crossovers between the X and Y chromosomes during meiosis. We here report a 32-year-old infertile male in whom seminal analysis showed azoospermia. Chromosomal analysis revealed a 46,XX karyotype and fluorescentin situhybridization (FISH) showed the presence of the SRY gene. This report highlights the value of karyotyping and FISH analysis in cases of infertility.

Published
2007

Catalog

Books, media, physical & digital resources
See catalog results