Your search keyword '"Disgenesia gonadal"' showing total 25 results

1. Síndrome de Frasier: ¿Cómo diagnosticar una enfermedad rara en la consulta de Ginecología? Reporte de caso.

Author

Muñoz-Infante, Marina, Pineda-Mateo, María, Gallardo-Martínez, Jara, Hoffner, Karolina, and Morales-Bueno, Ángela

Subjects

GYNECOLOGY, OVARIAN cancer, GLOMERULONEPHRITIS, GONADAL dysgenesis, INTERSEXUALITY, NEPHROBLASTOMA, ADNEXA uteri, CHILDBIRTH

Abstract

Copyright of Ginecología y Obstetricia de México is the property of Federacion Mexicana de Ginecologia y Obstetricia and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

2. Disgenesia gonadal completa 46,XY o síndrome de Swyer: reporte de un caso.

Author

Añorve-Vargas, Alexis, Pérez-López, José del Carmen, MandujanoÁlvarez, Gabriel Juan, Domínguez-Morales, Ever, and Contreras-Albavera, Elfego Octavio

Subjects

GONADAL dysgenesis, AMENORRHEA, PHENOTYPES, GENOTYPES, KARYOTYPES, HYPOGONADISM, FETAL development

Abstract

Copyright of Ginecología y Obstetricia de México is the property of Federacion Mexicana de Ginecologia y Obstetricia and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

3. Nueva variante del gen STAG3 causante de insuficiencia ovárica prematura.

Author

Gómez-Rojas, Susana, Enrique Aristizábal-Duque, Jorge, Fernanda Muñoz-Fernández, Luisa, Paula Sarmiento-Ramón, María, and Pilar Pereira-Gómez, María del

Subjects

*PREMATURE ovarian failure, *GENETIC variation, *GONADAL dysgenesis, *AMENORRHEA, *HYPOTHYROIDISM, *PREMATURE menopause, GONADAL diseases

Abstract

Objectives: To describe a case of ovarian failure secondary to a homozygous pathogenic variant in the STAG3 gene not previously reported. Material and methods: A 16-year-old patient with primary amenorrhea and absence of secondary sexual characteristics, with documented autoimmune hypothyroidism, poor genital and gonadal streak development which prompted the performance of clinical exome sequencing. A homozygous pathogenic variant not previously reported in the STAG3 gene, which has been associated with premature ovarian insufficiency (POI), was identified. Conclusions: In this case, clinical exome sequencing was key for identifying a STAG gene abnormality, probably associated with POI and long term prognosis for the patient. A new pathogenic variant c.2773delT; p.Ser925Profs*6 of the STAG3 gene associated with POI was established. [ABSTRACT FROM AUTHOR]

Published

2022

4. Agenesia uterina y ovárica. Una combinación inusual causante de hipogonadismo hipergonadotropo (HH).

Author

Benítez Cardoza, María Clara and García Bermejo, Roberto

Abstract

Introduction: hypergonadotropic Hypogonadism (HH) is the cause of delayed puberty, characterized by an intrinsic gonadal condition that interrupts the action of the hypothalamic-pituitary-gonadal axis. With a varied etiology, including genetic or acquired alterations. The association of uterine and ovarian agenesis in the same patient as the cause of HH is unusual. There are cases described in the HH literature with agenesis, dysgenesis, ovarian hypoplasia, but without uterine alteration. Case description: 12-year-old patient who consults for short stature with absence of pubertal development. Hormonal studies suffering from HH. Pelvic ultrasound and pelvic magnetic resonance imaging are requested, confirming gonadal and uterine agenesis. Management is performed with calcium supplements, estrogens as hormonal replacement to induce secondary sexual characteristics and support in your bone health. Achieve a normal final size according to your average parental size and improvement in your quality of life. Discussion: short stature and absence of secondary sexual characteristics is a form of clinical presentation of HH. Ovarian agenesis as a cause of HH, associated with uterine agenesis in the same patient, is an unusual association, motivating the publication of the case. Conclusion: it is important to recognize HH early, in order to provide timely treatment, and thus improve quality of life. [ABSTRACT FROM AUTHOR]

Published

2021

5. Abordaje del recién nacido con alteraciones del desarrollo sexual.

Author

Acosta-Rodríguez, Ariana Liseth and Mendoza-Rojas, Víctor Clemente

Published

2019

6. Síndrome de Frasier en una adolescente: asociación con disgenesia gonadal y enfermedad renal crónica.

Author

Fernández Rodríguez, Yaribel, Sardinas Solís, Rosa María, and Aguilera Yumbet, Yania

Abstract

The case report of a 16 years adolescent with apparent good health state who had been attended approximately for 3 years in the Pediatrics service to present lack of puberal changes, primary amenorrhoea, as well as increase of volume in lower members is described. The pertinent and complementary examinations were carried out and taking into account the group of clinical elements she presented, including a significant proteinuria associated with corporal dysmorfisms and hypogenitalism, the case was exposed to a multidisciplinary team, formed by nephrologists, Endocrinology specialists, geneticists and psychologists. Frasier syndrome was diagnosed, associated to nephrotic syndrome and gonadal dysgenesis. [ABSTRACT FROM AUTHOR]

Published

2019

7. New STAG3 gene variant as a cause of premature ovarian insufficiency

Author

Gómez-Rojas, Susana, Aristizábal-Duque, Jorge Enrique, Muñoz-Fernández, Luisa Fernanda, Sarmiento-Ramón, María Paula, and Pereira-Gómez, María del Pilar

Subjects

hipogonadismo, gonadal dysgenesis, Hypogonadism, autoimmunity, disgenesia gonadal, autoinmunidad, complete exorne sequencing, insuficiencia ovárica primaria, secuenciación del exorna completo, primary ovarian insufficiency

Abstract

RESUMEN Objetivos: describir un caso de falla ovárica secundaria a una variante patogénica homocigota en el gen STAG3 no reportada previamente. Materiales y métodos: paciente de 16 años con amenorrea primaria y ausencia de características sexuales secundarias, en quien se documentó hipotiroidismo autoinmune, pobre desarrollo genital y cintilla gonadal, por lo cual se realizó secuenciación de exorna clínico. Se identificó una variante homocigota patogénica previamente no reportada en el gen STAG3, el cual ha sido relacionado con insuficiencia ovárica prematura (IOP). Conclusiones: en este caso, la realización de exorna clínico fue determinante para identificar una alteración del gen STAG, probablemente asociada a la IOP y el pronóstico a largo plazo de la paciente. Se establece una nueva variante patogénica c.2773delT; p.Ser925Profs*6 del gen STAG3 asociada a la IOP. ABSTRACT Objectives: To describe a case of ovarian failure secondary to a homozygous pathogenic variant in the STAG3 gene not previously reported. Material and methods: A 16-year-old patient with primary amenorrhea and absence of secondary sexual characteristics, with documented autoimmune hypothyroidism, poor genital and gonadal streak development which prompted the performance of clinical exorne sequencing. A homozygous pathogenic variant not previously reported in the STAG3 gene, which has been associated with premature ovarian insufficiency (POI), was identified. Conclusions: In this case, clinical exorne sequencing was key for identifying a STAG gene abnormality, probably associated with POI and long term prognosis for the patient. A new pathogenic variant c.2773delT; p.Ser925Profs*6 of the STAG3 gene associated with POI was established.

Published

2022

8. Estudo de microdeleções do cromossomo Y em indivíduos com disgenesia gonadal e linhagem celular 46,XY

Author

Dos Santos, Ana Paula, 1986, Maciel-Guerra, Andrea Trevas, 1960, Mello, Maricilda Palandi de, Marques-de-Faria, Antonia Paula, Melo, Mônica Barbosa de, Universidade Estadual de Campinas. Faculdade de Ciências Médicas, Programa de Pós-Graduação em Ciências Médicas, and UNIVERSIDADE ESTADUAL DE CAMPINAS

Subjects

Chromosome deletion, Deleção cromossômica, Mosaicism, Y Chromosome, Disgenesia gonadal, Mosaicismo, Cromossomo Y, Gonadal dysgenesis

Abstract

Orientadores: Andréa Trevas Maciel Guerra, Maricilda Palandi de Mello Dissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciências Médicas Resumo: As disgenesias gonadais parcial (DGP) e mista (DGM) caracterizam-se por ambiguidade genital e presença de gônada disgenética associada a testículo disgenético ou dois testículos disgenéticos. Na DGP o cariótipo é 46,XY; na DGM, há mosaico 45,X/46,XY ou suas variantes (mais de duas linhagens e (ou) anomalias estruturais do cromossomo Y). Esses mosaicos podem determinar, ainda, fenótipo feminino com síndrome de Turner (ST), distúrbio da diferenciação do sexo ovotesticular (DDS OT) e esterilidade em homens com genitais normais. Independentemente do fenótipo gonadal e genital, esses indivíduos apresentam outros sinais clínicos decorrentes da linhagem 45,X, como baixa estatura, dismorfismos, anomalias cardíacas e renais e diversas afecções adquiridas. Nos últimos anos surgiram evidências de ligação entre microdeleções do Y e o mosaicismo com linhagem 45,X. Há, ainda, indicações de que a instabilidade cromossômica trazida por essas deleções possa ser mais pronunciada nas gônadas. O objetivo deste trabalho foi investigar a presença de microdeleções do Y em indivíduos com DGP e naqueles com mosaico 45,X/46,XY ou suas variantes e diferentes fenótipos. A casuística constou de 15 indivíduos com DGP e 15 com mosaicismo, dos quais a maioria apresentava DGM (11 casos). Foram analisados 38 sequence tagged sites (STS) cobrindo a região específica masculina (MSY, male specific region) em Yp, centrômero e Yq por meio da técnica de reação em cadeia da polimerase (PCR) multiplex e individual. Todos os STS investigados nos indivíduos com DGP tiveram amplificação positiva, porém havia STS de Yq ausentes em seis indivíduos com mosaicismo e DGM, dos quais dois sem alterações estruturais de Y evidentes ao cariótipo. Essas deleções se localizavam em regiões contendo genes relacionados à espermatogênese (AZFb e AZFc - azoospermia factor). A ausência de deleções nos indivíduos com DGP não confirma a hipótese de que a instabilidade desse cromossomo nas gônadas seja uma das causas dessa afecção. Por outro lado, as deleções encontradas no segundo grupo indicam, em alguns casos, associação entre alterações estruturais do Y detectáveis somente a nível molecular e o surgimento de mosaicismo. Caso sejam criados no sexo masculino e busquem procedimentos de fertilização in vitro, há risco de que esses indivíduos transmitam cromossomos Y instáveis na divisão celular Abstract: Partial and mixed gonadal dysgenesis (PGD and MGD) are characterized by genital ambiguity and the finding of either a streak gonad and a dysgenetic testis or two dysgenetic testes. In PGD there is a 46,XY karyotype, whereas in MGD there is a 45,X/46,XY mosaic or its variants (more than two lineages and/or structural abnormalities of the Y chromosome). These mosaics are also compatible with a female phenotype and Turner syndrome, ovotesticular disorder of sex development, and infertility in men with normal external genitalia. Regardless of the gonadal and genital phenotypes, these individuals present other clinical features associated with the 45,X cell line, including short stature, dysmorphisms, cardiovascular and renal anomalies and various acquired diseases. During the last few years, evidences of a link between Y microdeletions and 45,X mosaicism have been reported. There are also indications that the instability caused by such deletions might be more significant in germ cells. The aim of this work was to investigate the presence of Y chromosome microdeletions in individuals with PGD and in those with 45,X/46,XY mosaicism or its variants and variable phenotypes. Our sample comprised 15 individuals with PGD and 15 with mosaicism, most of them with a MGD phenotype (n=11). Thirty-eight sequence tagged sites (STS) spanning the male specific region (MSY) on the Y chromosome (Yp, centromere and Yq) where analyzed by multiplex PCR and some individual reactions. All STS showed positive amplifications in the PGD group. Conversely, in the group with mosaicism, six individuals with MGD had been identified with Yq microdeletions, two of them did not have structural abnormalities of the Y chromosome recognized by routine cytogenetic analysis. The deleted STSs were located within AZFb and AZFc (Azoospermia Factor) regions, which harbor several genes responsible for spermatogenesis. Absence of deletions in individuals with PGD does not confirm the hypothesis that instability of the Y chromosome in the gonads could be one of the causes of such condition. However, deletions identified in the second group indicate that mosaicism may be associated with Y chromosome abnormalities detectable only at the molecular level. If patients with mosaicism and Y microdeletions reared as males decide to undergo in vitro fertilization, Y chromosomes which tend to be unstable during cell division may be transmitted to offspring Mestrado Ciências Biomédicas Mestra em Ciências Médicas

Published

2021

9. Prevalence of Y-chromosome sequences and gonadoblastoma in Turner syndrome.

Author

Trovó de Marqui, Alessandra Bernadete, da Silva-Grecco, Roseane Lopes, and Spadotto Balarin, Marly Aparecida

Subjects

*Y chromosome, *TURNER'S syndrome, *GONADAL dysgenesis

Abstract

Objective: To assess the prevalence of Y-chromosome sequences and gonadoblastoma in patients with Turner syndrome (TS) using molecular techniques. Data source: A literature search was performed in Pubmed, limiting the period of time to the years 2005-2014 and using the descriptors: TS and Y sequences (n=26), and TS and Y- chromosome material (n=27). The inclusion criteria were: articles directly related to the subject and published in English or Portuguese. Articles which did not meet these criteria and review articles were excluded. After applying these criteria, 14 papers were left. Data synthesis: The main results regarding the prevalence of Y-chromosome sequences in TS were: (1) about 60% of the studies were conducted by Brazilian researchers; (2) the prevalence varied from 4.6 to 60%; (3) the most frequently investigated genes were SRY, DYZ3 and TSPY; (4) seven studies used only polymerase chain reaction, while in the remaining seven it was associated with FISH. Nine of the 14 studies reported gonadectomy and gonadoblastoma. The highest prevalence of gonadoblastoma (33%) was found in two studies. In five out of the nine papers evaluated the prevalence of gonadoblastoma was 10-25%; in two of them it was zero. Conclusions: According to these data, molecular analysis to detect Y-chromosome sequences in TS patients is indicated, regardless of their karyotype. In patients who test positive for these sequences, gonadoblastoma needs to be investigated. [ABSTRACT FROM AUTHOR]

Published

2016

10. Estudo funcional de novas variações nucleotídicas no gene NR5A1 em pacientes 46,XY com distúrbios da diferenciação do sexo

Author

Fabbri-Scallet, Helena, 1987, Mello, Maricilda Palandi de, Hiort, Olaf, Werner, Ralf, Sonati, Maria de Fátima, Bertuzzo, Carmen Sílvia, Costa, Elaine Maria Frade, Gonçalves, Edmilson Ricardo, Universidade Estadual de Campinas. Instituto de Biologia, Programa de Pós-Graduação em Genética e Biologia Molecular, and UNIVERSIDADE ESTADUAL DE CAMPINAS

Subjects

Steroidogenic factor 1, Mutation, Fator esteroidogênico 1, Disgenesia gonadal, Mutação, Gonadal dysgenesis

Abstract

Orientadores: Maricilda Palandi de Mello, Olaf Hiort, Ralf Werner Tese (doutorado) - Universidade Estadual de Campinas, Instituto de Biologia Resumo: Os Distúrbios da Diferenciação do Sexo (DDS) caracterizam-se pelos desenvolvimentos gonadal e/ou genital incompletos ou desordenados , que levam a uma discordância entre o sexo genético, gonadal e fenotípico do indivíduo afetado. Entre os genes envolvidos na cascata de diferenciação e determinação sexual, encontra-se o NR5A1, que codifica a proteína SF-1, e que quando mutado, pode levar a diferentes fenótipos de DDS, como disgenesia gonadal pura e parcial, DDS ovário testicular 46,XX, DDS 46,XX testicular, anorquia bilateral e hipospádia, além de quadros de amenorréia primária, insuficiência ovariana primária, infertilidade masculina, entre outros ...Observação: O resumo, na íntegra, poderá ser visualizado no texto completo da tese digital Abstract: Disorders of Sex Development (DSD) are defined as congenital conditions in which development of chromosomal, gonadal or anatomical sex is atypical. Mutations in the NR5A1 gene, which encodes the transcription factor SF-1, are responsible for different phenotypes of DSD, such partial and complete gonadal dysgenesis, 46,XX testicular and ovotesticular DSD, bilateral anorchia, hypospadia, and also can be associated with primary amenorrhea, premature ovarian failure, male infertility, adrenal tumors and others...Note: The complete abstract is available with the full electronic document Doutorado Genética Animal e Evolução Doutor em Genética e Biologia Molecular FAPESP 2013/05603-5, 2013/24333-9 BEPE 2013/24333-9

Published

2021

11. Analises de mutações e de seus efeitos na expressão do gene SRY em casos de disgenesia gonadal XY

Author

Cunha Júnior, José Luiz Rosenberis, Mello, Maricilda Palandi de, Benedetti, Celso Eduardo, 1964, Soardi, Fernanda Caroline, Azzoni, Adriano Rodrigues, Paulino, Luciana Campos, Universidade Estadual de Campinas. Instituto de Biologia, Programa de Pós-Graduação em Genética e Biologia Molecular, and UNIVERSIDADE ESTADUAL DE CAMPINAS

Subjects

Diferenciação do sexo, gonadal dysgenesis, Functional analysis, Mutação (Biologia), Análise funcional, Disgenesia gonadal, SRY genes, Mutation (Biology), Sex differentiation, Genes sry

Abstract

Orientadores: Maricilda Palandi de Mello, Celso Eduardo Benedetti, Fernanda Caroline Soardi Dissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Biologia Resumo: A expressão do gene SRY (Sex Determining Region in chromosome Y) é responsável por desencadear a determinação testicular durante o desenvolvimento embrionário, a partir das gônadas ainda indiferenciadas. Mutações nesse gene são encontradas em muitos casos de anomalias do desenvolvimento gonadal. O projeto teve por objetivo principal a análise funcional do efeito de uma mutação na região promotora do gene SRY, sendo que essa mutação consiste em uma deleção de 3 pares de base em um dos sítios consenso de ligação do fator de transcrição Sp1 ao promotor do gene. O portador dessa mutação é um indivíduo com disgenesia gonadal pura 46,XY, sendo que outros membros da família apresentavam ambiguidade genital e o pai, também portador da mutação, possuía grave hipospadia ao nascimento. Para tentar esclarecer os efeitos desta mutação nos mecanismos moleculares de regulação da expressão do gene SRY, este trabalho primeiramente analisou a interação da proteína Sp1 com os sítios localizados na região promotora de SRY e o efeito da mutação nesta interação, através de ensaios de EMSA (Electrophoretic Mobility Shift Assay). Concluiu-se que os sítios Sp1A e Sp1B se ligam a duas moléculas de Sp1 e que a mutação no Sp1A praticamente abole esta ligação. Possivelmente a ausência dessa ligação impediu a formação de um complexo de transcrição, causando uma diminuição na expressão do gene SRY e levando à ausência de formação dos testículos e reversão sexual completa na paciente. Complementando, foi analisado o efeito dessa mutação na expressão através de ensaio de expressão com gene repórter, no qual o promotor normal se mostrou em média duas vezes mais eficiente na ativação da expressão da luciferase que o promotor mutante. Entretanto, mais experimentos de transfecção, inclusive com outras linhagens celulares, devem ser realizados para confirmação desse resultado. Além disso, foi analisado o efeito de uma nova mutação (localizada na região codificante do gene SRY) na ligação da proteína SRY com o DNA, através de ensaios de EMSA. Concluiu-se que a mutação E89K, associada com disgenesia gonadal pura 46,XY, reduziu em alto nível a atividade de ligação in vitro da proteína SRY mutante ao DNA, o que representa um forte indício de que atividade reduzida da proteína mutante não foi suficiente para desencadear o processo de determinação testicular. Paralelamente, foi feito o rastreamento de mutações no gene SRY e sua região promotora em novos casos de disgenesia gonadal, não tendo sido encontradas, porém, alterações nos pacientes analisados Abstract: The SRY (Sex Determining Region in chromosome Y) gene expression is responsible for testicular determination during embrionary development. Mutations in SRY are found in many cases of anomalies of gonadal development. This project analyzed the functional effect of a mutation in SRY promoter region; the mutation is a 3-bp deletion in a consensus binding site for Sp1 transcription factor. The patient presented 46,XY pure gonadal dysgenesis, and a family history of relatives with different levels of genital ambiguity. Her father shares the same mutation in the SRY promoter region. In order to investigate the effects of the mutation upon the molecular mechanisms that regulate SRY gene expression, the interaction of the Sp1 transcription factor with normal and mutant binding sites was analyzed by EMSA (Electrophoretic Mobility Shift Assay). Each of Sp1A and Sp1B normal sites binds to a single Sp1 molecule, whereas the 3-bp deletion in Sp1A abolishs the binding to this site. Probably, the lack of Sp1 binding to the Sp1A site prevented the formation of a stable transcription complex, reducing the level of SRY expression and leading to the absence of testicles and complete sex reversal in the patient. Parallely, the effect of the mutation was analyzed by a reporter gene assay, indicating that the normal promoter is almost two times more efficient than the mutant promoter in the activation of luciferase gene expression using HeLa cells. However, further transfection experiments with other cell lineages must be performed to confirm this result. In addition, the effect of a new mutation (E89K, located in the SRY gene coding region) was analyzed by testing the ability of the SRY mutant protein to bind its DNA consensus sequence. EMSA assays revealed that the E89K mutation, which is associated with 46,XY pure gonadal dysgenesis, strongtly reduced the SRY protein binding activity in vitro. This result is a strong evidence that the reduced activity of SRY mutant protein was not sufficient to trigger the testicular determination in the patient, leading to the pure gonadal dysgenesis phenotype. Screening of mutations in the SRY gene coding and promoter regions was also performed in six diferent patients with 46,XY gonadal dysgenesis. However, other mutations have not been identified Mestrado Genética Animal e Evolução Mestre em Genética e Biologia Molecular

Published

2021

12. Deleción 9p-. Disgenesia gonadal asociada a retraso mental e hipoplasia del cuerpo calloso. ¿Síndrome de genes contiguos?

Author

Climent Alcalá, F. J., Molina Rodríguez, M. A., Casado, I. González, Bris, L. Osona, Fresno, L. Salamanca, Guerrero-Fernández, J., Martínez-Frías, M. L., and Bouthelier, R. Gracia

Published

2010

13. Prevalência de sequências do Y e de gonadoblastoma em síndrome de Turner

Author

Alessandra Bernadete Trovó de Marqui, Marly Aparecida Spadotto Balarin, and Roseane Lopes da Silva-Grecco

Subjects

Gynecology, medicine.medical_specialty, Y chromosome, Turner syndrome, Reação em cadeia da polimerase, Gonadoblastoma, 030209 endocrinology & metabolism, Disgenesia gonadal, Biology, medicine.disease, Cromossomo Y, Polymerase chain reaction, 03 medical and health sciences, 0302 clinical medicine, Síndrome de Turner, 030220 oncology & carcinogenesis, Pediatrics, Perinatology and Child Health, Prevalence, medicine, Prevalência, Gonadal dysgenesis

Abstract

ResumoObjetivoApresentar a prevalência de sequências do cromossomo Y por técnicas moleculares e de gonadoblastoma em pacientes com síndrome de Turner.Fontes de dadosFoi feita uma pesquisa bibliográfica no Pubmed, com limite de período entre 2005 e 2014, com os descritores Turner syndrome and Y sequences (n=26) e Turner syndrome and Y chromosome material (n=27). Os critérios de inclusão foram artigos que tivessem relação direta com o tema e publicados no idioma inglês ou português. Foram excluídos aqueles que não cumpriram esses critérios e eram do tipo revisão. Após aplicação desses critérios, 14 foram selecionados.Síntese dos dadosOs principais resultados quanto à prevalência de sequências do cromossomo Y em síndrome de Turner foram: 1 – cerca de 60% dos estudos foram feitos por pesquisadores brasileiros; 2 – a frequência variou de 4,6 a 60%; 3 – os genes SRY, DYZ3 e TSPY foram os mais investigados; 4 – a técnica de PCR foi empregada exclusivamente em sete estudos e nos sete restantes, associada à FISH. Nove dos 14 estudos apresentaram informações sobre gonadectomia e gonadoblastoma. Dois estudos relataram a maior prevalência para gonadoblastoma (33%). Cinco dos nove estudos referiram prevalência de 10 a 25% e em dois esse valor foi nulo.ConclusõesDe acordo com os dados apresentados, é indicada a pesquisa molecular para sequências do cromossomo Y em pacientes com ST, independentemente do cariótipo. Naquelas com positividade para essas sequências, é necessária a investigação de gonadoblastoma.AbstractObjectiveTo assess the prevalence of Y‐chromosome sequences and gonadoblastoma in patients with Turner syndrome using molecular techniques.Data sourceA literature search was performed in Pubmed, limiting the period of time to the years 2005 to 2014 and using the descriptors: Turner syndrome and Y sequences (n=26), and Turner syndrome and Y‐chromosome material (n=27). The inclusion criteria were: articles directly related to the subject and published in English or Portuguese. Articles which did not meet these criteria and review articles were excluded. After applying these criteria, 14 papers were left.Data synthesisthe main results regarding the prevalence of Y‐chromosome sequences in Turner syndrome were: 1–about 60% of the studies were conducted by Brazilian researchers; 2–the prevalence varied from 4.6 to 60%; 3–the most frequently investigated genes were SRY, DYZ3 and TSPY; 4–seven studies used only PCR, while in the remaining seven it was associated with FISH. Nine of the 14 studies reported gonadectomy and gonadoblastoma. The highest prevalence of gonadoblastoma (33%) was found in two studies. In five out of the nine papers evaluated the prevalence of gonadoblastoma was 10 to 25%; in two of them it was zero.Conclusionsaccording to these data, molecular analysis to detect Y‐chromosome sequences in TS patients is indicated, regardless of their karyotype. In patients who test positive for these sequences, gonadoblastoma needs to be investigated.

Published

2016

14. Peripheral precocious puberty: 46,XY complete gonadal dysgenesis

Author

Helena Cardoso, Luzia Lucélia Saraiva Ribeiro, J.A. Cidade-Rodrigues, Cátia Peixoto, B. Amaral, Jorge Luis Gavina Pereira, M. João Oliveira, Teresa Borges, M. Santalha, and S. Figueiredo

Subjects

medicine.medical_specialty, Sexual differentiation, business.industry, Gonadal dysgenesis, Gonadoblastoma, Disgenesia gonadal, medicine.disease, Pediatrics, Pubertad precoz, RJ1-570, Testis determining factor, Endocrinology, Management of Technology and Innovation, Internal medicine, medicine, Dysgerminoma, Precocious puberty, Thelarche, business, Testosterone

Abstract

Despite standard clinical definitions and availability of diagnostic tests for precocious puberty, an intensive and structured investigation is needed in order to diagnose the aetiology in particular cases.A 4-year-old, phenotypically female child was referred to paediatric endocrinology consultation for premature pubarche and thelarche. There was an acceleration of growth velocity with high levels of oestradiol and testosterone, and prepubertal FSH and LH measurements. Investigation showed bilateral gonadoblastoma as the cause of the peripheral precocious puberty.Genetic studies revealed 46,XY karyotype with mutation c.89G>T (p.Arg30Ile) in exon 1 of the SRY gene, confirming the diagnosis of complete gonadal dysgenesis. Disorders of sexual differentiation must be considered in the approach and investigation of peripheral precocious puberty, especially in the presence of ovarian tumours, such as gonadoblastoma and dysgerminoma. Resumen: La pubertad precoz, a pesar de las definiciones clínicas estandarizadas y pruebas de diagnóstico disponibles, requiere, en ciertas situaciones una investigación exhaustiva y estructurada con el fin de conocer la causa.Niña de 4 años de edad, fenotípicamente de sexo femenino, enviada a la consulta de endocrinología pediátrica por pubarquia y telarquia. Se observó aceleración en la tasa de crecimiento con niveles altos de estradiol y testosterona, con determinaciones prepúberes de la hormona luteinizante y foliculoestimulante. El resto del estudio de pubertad precoz periférica mostró la presencia de gonadoblastoma bilateral. El estudio genético reveló cariotipo 46 XY con mutación c.89G> T (p.Arg30Ile) en el exón 1 del gen SRY, confirmando el diagnóstico de disgenesia gonadal completa.Los trastornos de la diferenciación sexual deben ser considerados en el abordaje y la investigación de las causas de la pubertad precoz periférica, especialmente en presencia de tumores de ovario, como gonadoblastoma y disgerminomas.

Published

2014

15. Gen SRY y ausencia de tejido testicular en una mujer 47XYY con disgenesia gonadal

Author

Rojas, John Jairo, Jubiz, William, and Isaza, Carolina

Subjects

47 XYY karyotype, Gen SRY, SRY gene, Primary hypogonadism, Disgenesia gonadal, Diferenciación sexual, Sex differentiation, Cariotipo 47XYY, Hipogonadismo primario, Gonadal dysgenesis

Abstract

Este artículo revisa conceptos actuales sobre determinación y diferenciación sexual con base en el estudio genético de una niña de 13 años que consultó por talla baja y aumento de peso. El examen físico mostró Tanner I en mamas y en vello púbico, sin signos de androgenización. Mientras el nivel de la hormona de crecimiento (GH) era normal, las hormonas folículoestimulante (FSH) y luteinizante (LH) estaban aumentadas. Mediante laparoscopia y posterior estudio patológico se demostró la presencia de gonadas rudimentarias con ausencia de tejido testicular. Aunque el cariotipo obtenido fue 47XYY y el análisis molecular identificó la presencia del gen SRY, su funcionalidad es incierta, lo que hace necesaria su secuenciación, con la finalidad de determinar posibles mutaciones. En respuesta a la terapia con estrógenos y progesterona se desarrollaron tanto los caracteres sexuales secundarios como una menstruación normal. Aunque es posible que en la paciente haya una doble alteración genética donde concurran la mutación de novo de un gen y una no disyunción en la meiosis paterna, el caso descrito es ilustrativo de la importancia del estudio genético en la evaluación de la disgenesia gonadal. This paper reviews current concepts about sex determination and differentiation in males and females. We also present a 13 year old girl, who consulted for short stature and weight gain. She was a Tanner I for breast and pubic hair. There were no signs of androgen excess. Lab showed a high FSH and LH with normal growth hormone. Laparoscopy revealed streak gonads without testicular tissue. Karyotype was 47XYY, with the SRY gene present. Functional studies of the gene to detect mutations were not performed. Patient responded to a combination of estradiol and medroxyprogesterone with normal menses and breast development. This patient is an example of the importance of performing genetic studies in the evaluation of gonadal dysgenesis cases. It is possible that a de novo mutation of the gene, rather than a paternal meiotic nondysjunction was present in our patient.

Published

2013

16. Spontaneous puberty in girls with early diagnosis of Turner syndrome

Author

Carpini, Stela, Carvalho, Annelise Barreto, Guerra-Júnior, Gil, Baptista, Maria Tereza Matias, Lemos-Marini, Sofia Helena Valente, and Maciel-Guerra, Andréa Trevas

Subjects

puberdade, puberty, gonadal dysgenesis, Turner syndrome, Síndrome de Turner, disgenesia gonadal, diagnóstico precoce, early diagnosis

Abstract

OBJECTIVE: To verify if the frequency of spontaneous pubertal development among girls with Turner syndrome (TS) diagnosed in infancy and childhood is greater than that of patients diagnosed later. SUBJECTS AND METHODS: Thirty three girls aged < 10 years at the time of diagnosis were evaluated regarding pubertal development. The frequency of spontaneous puberty was compared with that of girls aged > 13 years diagnosed at the same service. RESULTS: Sixteen of 32 informative patients had signs of spontaneous puberty, a frequency greater than that of patients diagnosed later. In six patients, there was no progression of puberty; menarche occurred in six, and one became pregnant, but the fetus was a stillborn. Spontaneous puberty was absent in all cases with 45,X karyotype. CONCLUSIONS: The greater prevalence of spontaneous puberty in girls whose diagnosis was not based on pubertal delay suggests that, among those diagnosed later, there is a bias towards patients with hypogonadism. Arq Bras Endocrinol Metab. 2012;56(9):653-7 OBJETIVO: Verificar se a frequência de puberdade espontânea em meninas com síndrome de Turner (ST) diagnosticadas na infância é superior a de pacientes diagnosticadas posteriormente. SUJEITOS E MÉTODOS: Foram avaliadas 33 meninas < 10 anos ao diagnóstico quanto ao desenvolvimento puberal. A frequência de puberdade espontânea foi comparada com a de pacientes com mais de 13 anos diagnosticadas no mesmo serviço. RESULTADOS: Dezesseis das 32 pacientes informativas tiveram sinais puberais espontâneos, frequência superior a daquelas diagnosticadas posteriormente. Em seis delas, não houve progressão da puberdade; a menarca ocorreu em seis casos e uma paciente ficou grávida, porém o feto foi natimorto. Em todos os casos com cariótipo 45,X não ocorreu puberdade espontânea. CONCLUSÕES: A maior prevalência de puberdade espontânea em meninas cujo diagnóstico não se baseou em atraso puberal sugere que naquelas detectadas posteriormente haja distorção em favor de pacientes com hipogonadismo. Arq Bras Endocrinol Metab. 2012;56(9):653-7

Published

2012

17. Growth, pubertal development and associated anomalies in patients with XY partial gonadal dysgenesis

Author

Juliana Gabriel Ribeiro de Andrade, Maciel-Guerra, Andrea Trevas, 1960, Castro, Ângela Maria Spínola, Baptista, Maria Tereza Matias, Universidade Estadual de Campinas. Faculdade de Ciências Médicas, Programa de Pós-Graduação em Saúde da Criança e do Adolescente, and UNIVERSIDADE ESTADUAL DE CAMPINAS

Subjects

Sex differentiation disorders, Crescimento, Distúrbios da diferenciação do sexo, Puberty, Disgenesia gonadal, Growth, Gonadal Dysgenesis, Puberdade

Abstract

Orientador: Andrea Trevas Maciel-Guerra Dissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas Resumo: Introdução: A disgenesia gonadal (DG) parcial XY, caracterizada por disgenesia testicular e genitais internos e externos ambíguos em indivíduos com cariótipo 46,XY, é uma causa rara de distúrbio da diferenciação do sexo, de prognóstico ainda não completamente elucidado e etiologia ainda desconhecida. No entanto, o conhecimento a respeito de sua evolução clínica, da ocorrência de puberdade espontânea e de anomalias associadas é fundamental para definição do sexo de criação e orientação das famílias. Além disso, como genes responsáveis pela diferenciação testicular agem como promotores do crescimento, é possível haver associação dessa afecção com distúrbios do crescimento pré e pós-natal. Objetivo: Avaliar características clínicas associadas a esse distúrbio da diferenciação gonadal: antecedentes gestacionais e familiares, crescimento, puberdade espontânea e anomalias associadas. Sujeitos e Métodos: Análise retrospectiva dos dados contidos nos prontuários de 11 pacientes com DG Parcial XY criados no sexo masculino e com ao menos um dos testículos situado na bolsa escrotal. Estes pacientes haviam sido objeto de extensa avaliação clínica, histopatológica e molecular entre 1996 e 1998. Resultados: A maioria dos pacientes atingiu altura final dentro do canal de crescimento, e todos tiveram puberdade espontânea, apesar de níveis elevados de LH em alguns casos; apenas um necessitou de reposição de andrógenos para completar o desenvolvimento puberal. Havia níveis elevados de FSH e grave oligospermia; deficiência mental foi observada em três casos e hipotireoidismo em dois. Discussão: Portadores de DG parcial XY criados no sexo masculino e que tenham ao menos um testículo tópico têm bom prognóstico quanto à puberdade espontânea, embora haja possibilidade de falência secundária das células de Leydig; já o prognóstico quanto á função reprodutora é reservado. Não há indicações de que haja distúrbios do crescimento pré e pós-natal associados à disgenesia testicular. Apesar do pequeno número amostral, a maior freqüência de déficit cognitivo e hipotireoidismo observada nesta amostra indica que é necessário haver especial atenção a estas possíveis anomalias associadas Abstract: Introduction: XY partial gonadal dysgenesis (GD), characterized by ambiguous internal and external genitália in 46,XY subjects, is a rare cause of disorder of sex development. Both prognosis and etiology are still unknown. However, knowledge regarding natural history, spontaneous puberty and associated anomalies is essential to define sex of rearing and to discuss the prognosis with the parents. In addition, as genes responsible for testicular differentiation act as growth promoters, there may be an association of this disorder with pre and postnatal growth deficiency. Aim: To evaluate the clinical features associated with this disorder of gonadal differentiation: gestational and family history, growth, spontaneous puberty and associated anomalies. Subjects and Methods: Retrospective analysis of data from the clinical files of 11 patients with XY partial GD reared as males and who had at least one testis located in the scrotum. These patients had been subject to careful clinical, histopathological and molecular evaluation between 1996 and 1998. Results: Most patients attained final height within the limits of their growth channel, and all had spontaneous pubertal development, though some had high levels of LH. Only one needed androgen replacement to complete puberty. There were high levels of FSH and severe oligospermia. Mental deficiency was observed in three cases and hypothyroidism in two. Discussion: Patients with XY partial GD with at least one topic testis have good prognosis regarding spontaneous puberty, though there is a possibility of secondary Leydig cells' failure; there is no good prognosis regarding reproductive function. There are no indications on pre or postnatal growth deficiency associated with testicular dysgenesis. Despite the small sample size, the higher frequency of cognitive deficit and hypothyroidism indicates that there must be special attention to these associated disorders Mestrado Saúde da Criança e do Adolescente Mestre em Saúde da Criança e do Adolescente

Published

2010

18. Amenorrea secundaria—mosaicismo 45, X/46, XX— fertilidad y reinicio menstrual

Author

Osuna Ceballos, Jesús A.

Subjects

Revistas, Medicina y Salud, Insuficiencia ovárica prematura, Revista Venezolana de Endocrinología y Metabolismo, Facultad de Medicina, Sociedad Venezolana de Endocrinología y Metabolismo, Disgenesia gonadal, Secondary amenorrhea, Premature ovarian failure, Casos Clínicos [Revista Venezolana de Endocrinología y Metabolismo], Gonadal dysgenesis, Amenorrea secundaria

Abstract

Objetivo: Presentación de una paciente de 17 años de edad, con un mosaicismo 45,X/46,XX que consultó por amenorrea secundaria, con posterior normalización del ciclo menstrual y fertilidad. Metodos: Historia clínica, estudios endocrinos, laparoscopia, biopsia de ovarios y estudio citogenético. Resultados: La paciente inició cambios puberales espontáneos a la edad de 11 años y menarca a los 13 años, seguida de ciclos regulares de 28 días, hasta el momento de su consulta por amenorrea secundaria de 10 meses de evolución. En el exámen físico se constató una talla de 1,48 m., peso corporal de 40 Kg, normal desarrollo de sus caractéres sexuales secundarios y ausencia de alteraciones somáticas particulares. La citología vaginal mostró predominio de células intermedias y ausencia de células superficiales. El estudio hormonal reveló una concentración sérica de LH y FSH en límites altos de la normalidad, estradiol bajo y valores normales de TSH, T4 libre, prolactina y cortisol. La prueba de estimulación con GnRH reveló una respuesta exagerada de ambas gonadotrofinas. El estudio citogenético reveló un mosaicismo 45,X/46,XX. Prueba progestacional: ausencia de sangrado por deprivación postratamienbto con medroxiprogesterona: 10 mg/día/7 días. negativa. Durante 34 meses presentó sangramientos inducidos con ciclos combinados de estrógenos + progesterona, después de lo cual presentó menstruaciones espontáneas hasta lograr embarazo a los 22 años de edad. A las 38 semanas de embarazo se realizó cesárea electiva de la cual se obtuvo un varón normal. Retorno menstrual a los 4 meses posparto con continuidad de ciclos regulares hasta su edad actual de 29 años. Conclusiones: El presente caso ilustra el amplio espectro clínico del mosaicismo 45,X/46,XX, en una paciente con diferentes grados de su función ovárica, la cual inició con una menarca normal, seguida de insuficiencia ovárica con amenorrea secundaria hipergonadotrópica y posterior reinicio de ciclos menstruales regulares y subsiguiente fertilidad. Objective: To present a 17-year-old patient with 10-months-secondary amenorrhea, and a 45,X /46,XX mosaicism, who subsequently normalized her menstrual cycles and had spontaneous pregnancy. Methods: Data from the clinical history; endocrinological studies, laparoscopy and ovarian biopsy, and cytogenetic analysis are presented. Results: This patient presented spontaneous pubertal changes at the age of 11 years, and her menarche at 13 years of age, with regular menses every 28 days, and then she developed secondary amenorrhea of 10 months duration at 17 years of age. On physical examination she presented a height of 1,48 m., and her weight was 40 Kg. Her secondary sexual characters were normal and no particular somatic malformation were present. Vaginal cytology smear showed predominance of intermediate cells. Laboratory tests showed low serum estradiol levels, high FSH and LH serum concentration. Prolactin, free thyroxine, TSH and cortisol serum concentration were within normal range. LH and FSH values gave an exagerated response to GnRH stimulus. Cytogenetic study showed a 45,X/46,XX mosaicism. Progestational test was negative. For 34 months she presented regular menses while on combined estrogen + progesterone therapy. Thereafter she resumed spontaneous regular menses, until she became pregnant at the age of 22 years. At 38 weeks of pregnancy, caesarean section was performed and a normal male baby was obtained. Regular menses were resumed four months after delivery, and continued normaly until her present 29 years of age. Conclusions: The present case shows the wide clinical spectrum of the 45,X/46,XX mosaicism, in a patient with different levels of ovarian function, starting with a normal menarche, followed by ovarian failure and hypergonadotropic amenorrhea, and subsequent restoration of regular menstrual cycles, and fertility. 27-29 osunacja@ula.ve

Published

2009

19. Factors associated to referral of patients with features of Turner Syndrome to a tertiary reference center

Author

Annelise Barreto de Carvalho, Maciel-Guerra, Andrea Trevas, 1960, Castro, Ângela Maria Spínola, Marmo, Denise Barbieri, Universidade Estadual de Campinas. Faculdade de Ciências Médicas, Programa de Pós-Graduação em Saúde da Criança e do Adolescente, and UNIVERSIDADE ESTADUAL DE CAMPINAS

Subjects

Pediatria, Disgenesia gonadal, Estatura, Gonadal Dysgenesis, Stature, Pediatrics, Aberrações cromossômicas, Chromossome aberrations

Abstract

Orientador: Andrea Trevas Maciel-Guerra Dissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas Resumo: A Síndrome de Turner (ST) caracteriza-se pela presença de um cromossomo X e perda parcial ou total do segundo cromossomo sexual. Suas características mais comuns são baixa estatura e disgenesia gonadal. O diagnóstico precoce é fundamental para que as pacientes possam se beneficiar de diversas condutas específicas a serem tomadas quando necessário. Objetivo: analisar uma ampla casuística de pacientes com ST e a forma do encaminhamento de pacientes com essa suspeita clínica a um serviço de referência. Sujeitos: 425 pacientes do sexo feminino encaminhadas ao Grupo Interdisciplinar de Estudos da Determinação e Diferenciação do Sexo da Faculdade de Ciências Médicas da Universidade de Campinas para investigação de ST, no período de janeiro de 1989 a outubro de 2006. Métodos: Foram analisados os seguintes dados obtidos dos prontuários clínicos: constituição cromossômica, idade, estatura (em escore z) e estadio puberal no momento do diagnóstico, origem do encaminhamento (interno ou externo ao HC) e especialidade do médico que encaminhou. Foi feita análise descritiva, comparação de pacientes com e sem ST e das pacientes com ST de acordo com a origem e a especialidade do médico, além de análise de correlação entre estatura e idade ao diagnóstico. Resultados: O diagnóstico de ST foi feito em 36,9% dos casos, com baixa freqüência de cariótipos 45,X e predominância de aberrações estruturais. A média de idade ao diagnóstico da ST foi 12,01 anos, o escore z da estatura -3,09 e havia atraso puberal em 71,4% das 63 pacientes com mais de 13 anos. Os médicos pediatras foram os que mais encaminharam pacientes com suspeita desta síndrome, e aquelas provenientes de serviços externos tiveram com maior freqüência diagnóstico confirmado de ST. Comparadas às demais, as pacientes com ST apresentavam maior déficit na estatura e maior freqüência de atraso puberal. Dentre os casos de ST, as encaminhadas do próprio HC tinham estatura mais baixa que as de origem externa, porém com idade e freqüência de atraso puberal semelhantes; as encaminhadas por pediatras eram mais jovens, porém com estatura e freqüência de atraso puberal semelhantes às daquelas encaminhadas por não pediatras. Foi encontrada correlação linear negativa significativa entre a idade ao diagnóstico e a estatura no total de pacientes com ST, porém a ausência dessa correlação nos casos encaminhados por não pediatras sugere que esse grupo de pacientes, de diagnóstico mais tardio, possa ter déficit estatural menos acentuado e atraso puberal nem sempre evidente Discussão: O presente trabalho mostrou alta freqüência de casos de ST em serviço de referência, porém com diagnóstico ainda tardio na maioria dos casos e independente de serem provenientes ou não de serviços terciários. É necessário, portanto, divulgar entre pediatras e não pediatras em todos os níveis de atenção os conhecimentos necessários ao encaminhamento e diagnóstico precoce da ST Abstract: Turner syndrome (TS) is characterized by the presence of one X chromosome and partial or total lack of the second sex chromosome. Short stature and gonadal dysgenesis are the most frequent features. The early diagnosis is essential to allow appropriate management and institution of various therapeutic measures. Aim: To analyze a large sample of TS patients and to evaluate the referral of patients with clinical suspicion of this chromosome aberration. Subjects: 425 female patients referred to the Interdisciplinary Group of Disorders of sex development of the Faculty of medical sciences of the University of Campinas to investigate TS between January 1989 and October 2006. Methods: The following data were obtained from the medical records: chromosome constitution; age, height (zscore) and pubertal stage at diagnosis; origin of referral (from the University Hospital - UH - or outside services) and specialty of the physician who referred the patient. Descriptive analysis, followed by comparison between patients with and without TS and, among patients with TS, comparison according to origin and specialty of the physician. Correlation between age and height at diagnosis was also analyzed. Results: The diagnosis of TS was made in 36.9% of the cases, with low frequency of the 45,X karyotype and predominance of structural aberrations. Mean age of diagnosis was 12.01 years, height z score -3.09, and pubertal delay was found in 71.4% of the 63 patients aged more than 13 years. Pediatricians referred most patients, and the frequency of TS was higher among cases referred from outside services. When compared to the other patients of the sample, TS girls had shorter stature and higher frequency of pubertal delay. Among patients with TS, those referred from the UH had shorter stature but similar age and frequency of pubertal delay; those referred by pediatricians were younger, but stature and frequency of pubertal delay were similar to those referred by non-pediatricians. There was negative linear correlation between age and stature in the whole sample of girls with TS at diagnosis; however, absence of a similar correlation among girls referred by non-pediatricians suggests that in this group of patients, whose diagnosis was even more delayed, growth deficiency and puberty delay may be less evident. Discussion: The present work shows high frequency of TS in a reference service, but age at diagnosis is delayed in most cases, independent from its origin. Information about TS and the need for early diagnosis must be spread among pediatricians and non-pediatricians in all levels of health attention Mestrado Pediatria Mestre em Saúde da Criança e do Adolescente

Published

2009

20. Gen SRY y ausencia de tejido testicular en una mujer 47XYY con disgenesia gonadal

Author

Rojas, John Jairo, Jubiz, William, and Isaza, Carolina

Subjects

SRY gene, 47 XYY karyotype, Primary hypogonadism, Gen SRY, Disgenesia gonadal, Diferenciación sexual, Sex differentiation, Cariotipo 47XYY, Hipogonadismo primario, Gonadal dysgenesis

Abstract

Este artículo revisa conceptos actuales sobre determinación y diferenciación sexual con base en el estudio genético de una niña de 13 años que consultó por talla baja y aumento de peso. El examen físico mostró Tanner I en mamas y en vello púbico, sin signos de androgenización. Mientras el nivel de la hormona de crecimiento (GH) era normal, las hormonas folículoestimulante (FSH) y luteinizante (LH) estaban aumentadas. Mediante laparoscopia y posterior estudio patológico se demostró la presencia de gonadas rudimentarias con ausencia de tejido testicular. Aunque el cariotipo obtenido fue 47XYY y el análisis molecular identificó la presencia del gen SRY, su funcionalidad es incierta, lo que hace necesaria su secuenciación, con la finalidad de determinar posibles mutaciones. En respuesta a la terapia con estrógenos y progesterona se desarrollaron tanto los caracteres sexuales secundarios como una menstruación normal. Aunque es posible que en la paciente haya una doble alteración genética donde concurran la mutación de novo de un gen y una no disyunción en la meiosis paterna, el caso descrito es ilustrativo de la importancia del estudio genético en la evaluación de la disgenesia gonadal. This paper reviews current concepts about sex determination and differentiation in males and females. We also present a 13 year old girl, who consulted for short stature and weight gain. She was a Tanner I for breast and pubic hair. There were no signs of androgen excess. Lab showed a high FSH and LH with normal growth hormone. Laparoscopy revealed streak gonads without testicular tissue. Karyotype was 47XYY, with the SRY gene present. Functional studies of the gene to detect mutations were not performed. Patient responded to a combination of estradiol and medroxyprogesterone with normal menses and breast development. This patient is an example of the importance of performing genetic studies in the evaluation of gonadal dysgenesis cases. It is possible that a de novo mutation of the gene, rather than a paternal meiotic nondysjunction was present in our patient.

Published

2005

21. Disgenesias gonadais e tumores: aspectos genéticos e clínicos

Author

Lipay, Mônica V. Nunes, Bianco, Bianca, and Verreschi, Ieda T.N.

Subjects

Diferenciação sexual, Sexual differentiation, Tumor gonadal, Gonadoblastoma, Disgenesia gonadal, Gonadal tumor, Gonadal dysgenesis

Abstract

As Disgenesias Gonadais compõem um espectro clínico de anomalias com fenótipo variável, de feminino a ambíguo ou masculino, em pacientes com desenvolvimento puberal comprometido ou ausente e cariótipo contendo ou não um cromossomo Y e/ou cromossomos marcadores. Embora as seqüências Y-específicas nem sempre sejam evidentes citogeneticamente, as gônadas disgenéticas de pacientes com estas seqüências do cromossomo Y apresentam potencialidade para o desenvolvimento de tumores gonadais. O gonadoblastoma, neoplasia de células germinativas misturadas com células de cordões sexuais, geralmente com calcificações focais, é o mais temido pela sua freqüência. Outras neoplasias de comportamento maligno ou não ocorrem nas disgenesias, sendo também relacionadas à presença de seqüências do cromossomo Y. A detecção destas seqüências por técnicas citogenéticas ou moleculares tem sido estimulada para nortear a indicação profilática de cirurgia para retirada das gônadas neste grupo de pacientes, uma vez que não são, em geral, tumores metastáticos e pela possibilidade de cura com a sua rescisão. Gonadal dysgenesis comprises a clinical spectrum of anomalies in patients with female, ambiguous or male phenotype, absent or impaired puberty and karyotype with or without Y chromosome and/or chromosome markers. Although Y-specific sequences are seldom cytogenetically evident, dysgenetic gonads are potentially prone to developing tumors. Gonadoblastoma, a mixed germ cell and sex-cord cells tumor with variable degree of focal calcification, is the most harmful due to its frequency. Other gonadal tumor, maligns or not, also occur in gonadal dysgenesis. As they are not metastatic tumors and may be eradicated by selective excisions, the importance of detecting Y-sequences by molecular sensitized techniques is stressed in order to indicate prophylactic gonadectomy.

Published

2005

22. Genes envolvidos na determinação e diferenciação do sexo

Author

Christine Hackel, Juliana Godoy Assumpção, and Maricilda Palandi de Mello

Subjects

Diferenciação gonadal, Endocrinology, Diabetes and Metabolism, Female development, Ovary, General Medicine, Disgenesia gonadal, Biology, Sexo, Chromosome, Y chromosome, Gene, Andrology, Testis determining factor, medicine.anatomical_structure, Cromossomo, External genitalia, SRY, medicine, Sex, Pathological, Gonadal dysgenesis, Gonadal differentiation, Hormone

Abstract

O sexo cromossômico é estabelecido na fertilização pela presença de um cromossomo X ou Y. O desenvolvimento dos sexos masculino e feminino passa, num primeiro momento, pela especialização das gônadas em testículos ou ovários; os demais processos decorrem de efeitos secundários provocados pelos hormônios por elas produzidos. As etapas de determinação e diferenciação das gônadas em testículos ou em ovários e a diferenciação dos genitais externos masculinos ou femininos envolvem a expressão específica de uma cascata de genes. Esses genes, seus respectivos padrões de expressão, bem como seus envolvimentos na manifestação de patologias ligadas ao desenvolvimento gonadal e dos genitais externos serão abordados nesta revisão. Chromosomal sex is established at fertilization by the presence of an X or Y chromosome. The first step of male and female development is gonadal specialization in testes or ovaries; all other processes that follow result from secondary effects produced by testis and ovary hormones. Gonadal determination and differentiation and the development of external genitalia involve time- and tissue-specific expression of genes forming a gene cascade. Those genes, their expression profile and their role in the pathological manifestations related to gonadal and external genitalia development will be discussed in this review.

Published

2005

23. Amenorrea secundaria-mosaicismo 45,X/46,XX fertilidad y reinicio de funcion menstrual

Author

Osuna C, Jesús A

Subjects

amenorrea secundaria, secondary amenorrhea, gonadal dysgenesis, disgenesia gonadal, insuficiencia ovárica prematura, premature ovarian failure

Abstract

Objetivo: Presentación de una paciente de 17 años de edad, con un mosaicismo 45,X/46,XX que consultó por amenorrea secundaria, con posterior normalización del ciclo menstrual y fertilidad. Metodos: Historia clínica, estudios endocrinos, laparoscopia, biopsia de ovarios y estudio citogenético. Resultados: La paciente inició cambios puberales espontáneos a la edad de 11 años y menarca a los 13 años, seguida de ciclos regulares de 28 días, hasta el momento de su consulta por amenorrea secundaria de 10 meses de evolución. En el exámen físico se constató una talla de 1,48 m., peso corporal de 40 Kg, normal desarrollo de sus caractéres sexuales secundarios y ausencia de alteraciones somáticas particulares. La citología vaginal mostró predominio de células intermedias y ausencia de células superficiales. El estudio hormonal reveló una concentración sérica de LH y FSH en límites altos de la normalidad, estradiol bajo y valores normales de TSH, T4 libre, prolactina y cortisol. La prueba de estimulación con GnRH reveló una respuesta exagerada de ambas gonadotrofinas. El estudio citogenético reveló un mosaicismo 45,X/46,XX. Prueba progestacional: ausencia de sangrado por deprivación postratamienbto con medroxiprogesterona: 10 mg/día/7 días. negativa. Durante 34 meses presentó sangramientos inducidos con ciclos combinados de estrógenos + progesterona, después de lo cual presentó menstruaciones espontáneas hasta lograr embarazo a los 22 años de edad. A las 38 semanas de embarazo se realizó cesárea electiva de la cual se obtuvo un varón normal. Retorno menstrual a los 4 meses posparto con continuidad de ciclos regulares hasta su edad actual de 29 años. Conclusiones: El presente caso ilustra el amplio espectro clínico del mosaicismo 45,X/46,XX, en una paciente con diferentes grados de su función ovárica, la cual inició con una menarca normal, seguida de insuficiencia ovárica con amenorrea secundaria hipergonadotrópica y posterior reinicio de ciclos menstruales regulares y subsiguiente fertilidad. Objective: To present a 17-year-old patient with 10-months-secondary amenorrhea, and a 45,X /46,XX mosaicism, who subsequently normalized her menstrual cycles and had spontaneous pregnancy. Methods: Data from the clinical history; endocrinological studies, laparoscopy and ovarian biopsy, and cytogenetic analysis are presented. Results: This patient presented spontaneous pubertal changes at the age of 11 years, and her menarche at 13 years of age, with regular menses every 28 days, and then she developed secondary amenorrhea of 10 months duration at 17 years of age. On physical examination she presented a height of 1,48 m., and her weight was 40 Kg. Her secondary sexual characters were normal and no particular somatic malformation were present. Vaginal cytology smear showed predominance of intermediate cells. Laboratory tests showed low serum estradiol levels, high FSH and LH serum concentration. Prolactin, free thyroxine, TSH and cortisol serum concentration were within normal range. LH and FSH values gave an exagerated response to GnRH stimulus. Cytogenetic study showed a 45,X/46,XX mosaicism. Progestational test was negative. For 34 months she presented regular menses while on combined estrogen + progesterone therapy. Thereafter she resumed spontaneous regular menses, until she became pregnant at the age of 22 years. At 38 weeks of pregnancy, caesarean section was performed and a normal male baby was obtained. Regular menses were resumed four months after delivery, and continued normaly until her present 29 years of age. Conclusions: The present case shows the wide clinical spectrum of the 45,X/46,XX mosaicism, in a patient with different levels of ovarian function, starting with a normal menarche, followed by ovarian failure and hypergonadotropic amenorrhea, and subsequent restoration of regular menstrual cycles, and fertility.

Published

2003

24. Prevalência de sequências do Y e de gonadoblastoma em síndrome de Turner

Author

Alessandra Bernadete Trovó de Marqui, Roseane Lopes da Silva-Grecco, and Marly Aparecida Spadotto Balarin

Subjects

Economics and Econometrics, medicine.medical_specialty, Turner syndrome, Reação em cadeia da polimerase, Gonadoblastoma, Gonadal dysgenesis, 030209 endocrinology & metabolism, Y chromosome, 03 medical and health sciences, 0302 clinical medicine, Síndrome de Turner, Materials Chemistry, Media Technology, Prevalence, Medicine, Humans, In patient, Prevalência, Review Articles, Gynecology, Data source, Ovarian Neoplasms, Chromosomes, Human, Y, business.industry, lcsh:RJ1-570, Forestry, Karyotype, lcsh:Pediatrics, Sequence Analysis, DNA, Disgenesia gonadal, medicine.disease, Cromossomo Y, Polymerase chain reaction, Testis determining factor, 030220 oncology & carcinogenesis, Karyotyping, Female, business

Abstract

Objective: To assess the prevalence of Y-chromosome sequences and gonadoblastoma in patients with Turner syndrome (TS) using molecular techniques. Data source: A literature search was performed in Pubmed, limiting the period of time to the years 2005–2014 and using the descriptors: TS and Y sequences (n=26), and TS and Y-chromosome material (n=27). The inclusion criteria were: articles directly related to the subject and published in English or Portuguese. Articles which did not meet these criteria and review articles were excluded. After applying these criteria, 14 papers were left. Data synthesis: The main results regarding the prevalence of Y-chromosome sequences in TS were: (1) about 60% of the studies were conducted by Brazilian researchers; (2) the prevalence varied from 4.6 to 60%; (3) the most frequently investigated genes were SRY, DYZ3 and TSPY; (4) seven studies used only polymerase chain reaction, while in the remaining seven it was associated with FISH. Nine of the 14 studies reported gonadectomy and gonadoblastoma. The highest prevalence of gonadoblastoma (33%) was found in two studies. In five out of the nine papers evaluated the prevalence of gonadoblastoma was 10–25%; in two of them it was zero. Conclusions: According to these data, molecular analysis to detect Y-chromosome sequences in TS patients is indicated, regardless of their karyotype. In patients who test positive for these sequences, gonadoblastoma needs to be investigated. RESUMO Objetivo: Apresentar a prevalência de sequências do cromossomo Y por técnicas moleculares e de gonadoblastoma em pacientes com síndrome de Turner. Fontes de dados: Foi feita uma pesquisa bibliográfica no Pubmed, com limite de período entre 2005 e 2014, com os descritores Turner syndrome and Y sequences (n=26) e Turner syndrome and Y chromosome material (n=27). Os critérios de inclusão foram artigos que tivessem relação direta com o tema e publicados no idioma inglês ou português. Foram excluídos aqueles que não cumpriram esses critérios e eram do tipo revisão. Após aplicação desses critérios, 14 foram selecionados. Síntese dos dados: Os principais resultados quanto à prevalência de sequências do cromossomo Y em síndrome de Turner foram: 1 – cerca de 60% dos estudos foram feitos por pesquisadores brasileiros; 2 – a frequência variou de 4,6 a 60%; 3 – os genes SRY, DYZ3 e TSPY foram os mais investigados; 4 – a técnica de PCR foi empregada exclusivamente em sete estudos e nos sete restantes, associada à FISH. Nove dos 14 estudos apresentaram informações sobre gonadectomia e gonadoblastoma. Dois estudos relataram a maior prevalência para gonadoblastoma (33%). Cinco dos nove estudos referiram prevalência de 10 a 25% e em dois esse valor foi nulo. Conclusões: De acordo com os dados apresentados, é indicada a pesquisa molecular para sequências do cromossomo Y em pacientes com ST, independentemente do cariótipo. Naquelas com positividade para essas sequências, é necessária a investigação de gonadoblastoma.

25. Disgenesia gonadal con cromatina positiva

Author

Aspillaga H, Manuel, Avendaño B, Isabel, Aguirre O, María Isabel, and Labraña T, Cecilia

Subjects

Chromatine positive, gonadal dysgenesis, mosaicism, cromosoma X en anillo, Cromatina positiva, isocromosoma Xq, disgenesia gonadal, Xring chromosome, mosaicismo, Xq isochiomosome

Published

1986