Your search keyword '"Gonadal Dysgenesis"' showing total 6,450 results

251. Researcher at Capital Medical University Zeroes in on Turner Syndrome (Improvement of Bone Metabolism in Prepubertal Girls with Turner Syndrome Following Long-term Pegylated Growth Hormone Treatment).

Abstract

A recent study conducted at Capital Medical University in Beijing, China, focused on the improvement of bone metabolism in prepubertal girls with Turner Syndrome (TS) following long-term polyethylene glycol recombinant human Growth Hormone (PEG-rhGH) treatment. The study involved 28 prepubertal girls with TS, with 18 receiving PEG-rhGH therapy and 10 not receiving it. Results showed that after 12 months of PEG-rhGH therapy, the treatment group exhibited significant increases in growth velocity and height standard deviation scores, along with enhanced bone formation markers. The research suggests that PEG-rhGH therapy in children with TS can significantly improve linear growth and benefit bone metabolism. [Extracted from the article]

Published

2024

252. Recent Studies from Capital Health Regional Medical Center Add New Data to Leydig Cell Tumor (12465 Unraveling The Enigma: A Multifaceted Presentation Of Hormonal Dysregulation In A 37-year-old Woman).

Subjects

ENDOCRINE cells, TESTICULAR diseases, ENDOCRINE diseases, LEYDIG cells, SKIN diseases, GONADAL dysgenesis

Abstract

A recent study from Capital Health Regional Medical Center focused on Leydig cell tumors, rare gonadal tumors known for producing androgens leading to symptoms like hirsutism. The study highlighted the importance of accurate diagnosis and multidisciplinary collaboration for optimal management of Leydig cell tumors. Surgical resection is the primary treatment, with long-term follow-up recommended for monitoring. The study emphasized the need to consider Leydig cell tumors in cases of hirsutism with elevated androgen levels. [Extracted from the article]

Published

2024

253. "Methods For Non-Invasive Prenatal Ploidy Calling" in Patent Application Approval Process (USPTO 20240331799).

Abstract

The patent application titled "Methods For Non-Invasive Prenatal Ploidy Calling" by inventors from Natera Inc. introduces a method for determining the ploidy status of chromosomes in a fetus using maternal and fetal DNA samples. The method aims to provide accurate prenatal genetic diagnosis without invasive procedures, such as amniocentesis, which carry risks. By analyzing cell-free fetal DNA and intact fetal cells in maternal blood, the method offers a non-invasive approach to detect chromosomal abnormalities, aiding in the early identification of conditions like Down syndrome and Turner syndrome. The patent application outlines detailed procedures for DNA preparation, enrichment, and analysis to determine the ploidy state of the fetus. [Extracted from the article]

Published

2024

254. Pirogov Russian National Research Medical University Researchers Detail Findings in Gonadal Dysgenesis (Swyer Syndrome: Clinical Case of Gonadal Dysgenesis in a 15-year-old Girl).

Abstract

Researchers from Pirogov Russian National Research Medical University have published a clinical case study on gonadal dysgenesis, specifically focusing on Swyer syndrome. Swyer syndrome is a rare genetic disorder characterized by gonadal dysgenesis and a karyotype of 46, XY. The syndrome is often asymptomatic until puberty, when underdevelopment of secondary sexual characteristics becomes apparent. The study highlights diagnostic criteria, treatment options including surgery and hormone replacement therapy, and emphasizes the importance of thorough examination to avoid complications. The research provides valuable insights for medical professionals managing patients with Swyer syndrome. [Extracted from the article]

Published

2024

255. New Findings from Peking Union Medical College Hospital in the Area of Turner Syndrome Published (Approach to the Patient: Diagnosis and Treatment with Growth Hormone of Turner Syndrome and its Variants).

Abstract

A recent study conducted at Peking Union Medical College Hospital explored Turner syndrome (TS) and its variants. TS is a genetic condition characterized by the partial or complete absence of the second X chromosome in females. The study focused on patients with Xp deletion caused by unbalanced X-autosome translocations, which were considered as TS variants. The researchers proposed a diagnosis workflow and a risk assessment tool for growth hormone (GH) treatment in TS variants. The study concluded that the diagnosis workflow and risk assessment tool are valuable for clinicians in managing complex cases of TS variants with GH treatment. [Extracted from the article]

Published

2024

256. All India Institute of Medical Sciences (AIIMS) Researcher Publishes New Studies and Findings in the Area of Clinical Anatomy (Clinical, Genetic, Biochemical, Hormonal, and Radiological Profile in Patients with Disorders of Sex Development...).

Subjects

SEX differentiation disorders, ADRENOGENITAL syndrome, MEDICAL genetics, PEDIATRIC surgeons, SEX differentiation (Embryology), GONADAL dysgenesis

Abstract

A recent study conducted at the All India Institute of Medical Sciences (AIIMS) in Chhattisgarh, India, focused on patients with disorders of sex development (DSD). The study examined the clinical, genetic, biochemical, hormonal, and radiological profiles of seven DSD patients who presented at the institute over a two-year period. The researchers found that patients with DSD require systematic management at a tertiary care center, and the assignment of sex should only be done after a proper diagnosis and workup. The study emphasizes the importance of counseling parents and following guidelines for individualized management. [Extracted from the article]

Published

2024

257. Researcher at Department of Endocrinology Has Published New Data on Enzymes and Coenzymes (A novel mutation in a case of XY DSD with progressive virilization at puberty).

Subjects

ANDROGEN-insensitivity syndrome, COENZYMES, CHORIONIC gonadotropins, MEDICAL sciences, NEWSPAPER editors, GONADAL dysgenesis

Abstract

A recent study conducted in Telangana, India, focused on a case of ambiguous genitalia in a patient who experienced progressive virilization during puberty. The researchers identified a novel mutation in the NR5A1 gene and a mutation in the DHX37 gene, which are associated with testicular dysgenesis and ambiguous genitalia, respectively. Despite testosterone therapy, the patient exhibited poor virilization and a high testosterone/dihydrotestosterone ratio. The study highlights the potential impact of these mutations on the conversion of testosterone to dihydrotestosterone. For more information, the full article can be accessed through the provided link. [Extracted from the article]

Published

2024

258. Department of Pediatric Surgery and Pediatric Urology Researcher Highlights Recent Research in Pediatrics (Short-Term Impact of Newly Imposed Legal Restriction on DSD Surgery in Children in Germany).

Subjects

ADRENOGENITAL syndrome, SEX differentiation disorders, SURGICAL technology, PEDIATRIC surgery, PEDIATRIC urology, GONADAL dysgenesis

Abstract

A recent study conducted in Germany examined the impact of newly imposed legal restrictions on surgery for children with Disorders of Sexual Development (DSD). The study included 35 patients, with 15 in the group operated on after the legislation and 20 in the control group operated on before the legislation. The research found that the introduction of the legislation led to a significant delay in surgery. The study suggests that further amendments to the law are needed to minimize potential harm, particularly for patients with severe hypospadias and 46,XX congenital adrenal hyperplasia. [Extracted from the article]

Published

2024

259. Studies from Jamia Millia Islamia University in the Area of Turner Syndrome Published (Turner Syndrome where are we?).

Abstract

A recent report from Jamia Millia Islamia University discusses the findings of research on Turner syndrome. Turner syndrome is a genetic condition that occurs when one X chromosome is missing in phenotypic females, leading to various complications such as short stature, cardiovascular issues, autoimmune disorders, and infertility. The research emphasizes the need for a comprehensive and multidisciplinary approach to diagnosis and management, with growth hormone therapy being a fundamental treatment. The study also highlights the importance of ongoing research to identify potential therapeutic interventions and improve the overall functioning and quality of life for individuals with Turner syndrome. [Extracted from the article]

Published

2024

260. University of Gothenburg Reports Findings in Turner Syndrome (Psychiatric disorders and comorbidity in women with Turner Syndrome: a retrospective national cohort study).

Subjects

MENTAL illness, SEX differentiation disorders, GONADAL diseases, ENDOCRINE diseases, MEDICAL research

Abstract

A recent study conducted by the University of Gothenburg in Sweden examined the occurrence of psychiatric disorders in women with Turner Syndrome (TS), a genetic condition characterized by partial or complete monosomy X. The study found that the most common psychiatric diagnoses in women with TS were mood and anxiety disorders. Interestingly, the frequency of psychiatric diagnoses in women with TS was lower than in the general population. The researchers concluded that further investigations are needed to better understand the mental health needs of women with TS. [Extracted from the article]

Published

2024

261. Gauhati Medical College and Hospital Researcher Reveals New Findings on Endocrinology and Metabolism (Variability in Sex Assignment at Birth and Etiological Diagnosis of Differences of Sex Development: A Ten-Year Institutional Experience from...).

Subjects

HYPERANDROGENISM, SEX differentiation disorders, SEX chromosomes, KLINEFELTER'S syndrome, REPORTERS & reporting, GONADAL dysgenesis

Abstract

A recent study conducted at Gauhati Medical College and Hospital in Assam, India, examined the variability in sex assignment at birth and the etiological diagnosis of differences of sex development (DSD). The study analyzed the records of individuals with DSD over a ten-year period, noting their age at presentation, sex assignment, gender identity, and relevant hormonal and radiological investigations. The most prevalent type of DSD was 46, XY DSD, followed by 46, XX DSD and sex chromosome DSD. The study highlights the importance of comprehensive approaches to DSD diagnosis and management, particularly in regions with limited resources. [Extracted from the article]

Published

2024

262. Researchers from University of Pittsburgh Describe Findings in Turner Syndrome (Rare Turner Syndrome and Lupus Coexistence With Insights From Dna Methylation Patterns).

Abstract

A recent study conducted by researchers from the University of Pittsburgh explores the coexistence of Turner Syndrome and lupus in a female patient. Turner Syndrome is a rare genetic disorder characterized by the absence or partial absence of one X chromosome in females. The study suggests a potential link between the gene-dose effect from the X-chromosome and the development of lupus. The researchers found higher levels of DNA methylation in interferon-regulated genes in the patient, which may provide a protective effect against lupus. This research was supported by the NIH National Institute of Allergy & Infectious Diseases. [Extracted from the article]

Published

2024

263. Heterozygous variant in NR5A1 gene as a monogenic form of gonadal dysgenesis: a case report

Author

Antonella Gambadauro, Giorgia Pepe, Celeste Casto, Angelo Tropeano, Carmelo Romeo, and Malgorzata Wasniewska

Subjects

gonadal dysgenesis, nr5a1 gene, dsd, disorders of sex development, Medicine, Biology (General), QH301-705.5

Abstract

NR5A1 gene mutations are associated principally to 46,XY DSD (Disorders of Sex Development), with an extensive range of phenotypic variability in patients, comprising gonadal dysgenesis and male infertility. NR5A1 gene plays a crucial role in reproduction, steroidogenesis, and sexual differentiation. The present case describes an Italian male adolescent with ambiguous genitalia at birth and a 46,XY karyotype who was investigated for DSD genetic panel conditions due to slow pubertal progression. A heterozygous variant in NR5A1 (NM_004959.4: c.937CT, p.Arg313Cys) was identified in this patient and in his father. The same variant was previously described in other studies showing the wide heterogeneity of genotype-phenotype correlation in DSD patients.

Published

2021

264. Clinico-hormonal Parameters as a Primary Step to Differentiate Normosmic Idiopathic Hypogonadotropic Hypogonadism and Kallmann Syndrome in a Tertiary Care Hospital in Eastern India

Author

Ram Chandra Bhadra, Dona Saha, and Arjun Baidya

Subjects

anosmia, gonadal dysgenesis, puberty, Medicine

Abstract

Introduction: Idiopathic hypogonadotropic hypogonadism is a rare gonadal dysgenesis in which puberty does not take place naturally. It occurs due to insufficient pulsatile secretion of Gonadotrophin-Releasing Hormone (GnRH) and the resulting Follicle-Stimulating Hormone (FSH) and Luteinising Hormone (LH) deficiency leads to absence of or delayed sexual maturation. Kallmann syndrome is an uncommon genetic disorder characterised by hypogonadotropic hypogonadism associated with anosmia or hyposmia. When anosmia is absent, the same is referred as normosmic Idiopathic Hypogonadotropic hypogonadism (nIHH). Aim: To find out the significant differences between Kallmann syndrome and nIHH based on clinical features and biochemical assessment as a primary measure to initiate the treatment early. Materials and Methods: This hospital based cross-sectional observational cohort study was conducted in Department of Endocrinology, Nilratan Sircar Medical College and Hospital, Kolkata, India. The study was done on 55 cases of IHH presenting to the department with delayed secondary sexual characteristics. Results: Out of these 55 cases, 45 (81.8%) were of nIHH and only 10 (18.2%) cases were of Kallmann Syndrome. It was found that both the conditions show male predominance. Smell abnormalities were present only in Kallmann group. The level of serum testosterone was significantly higher (p

Published

2021

265. Effects of genomic instability in populations of Drosophilae melanogaster from regions of Ukraine with different radiation impact factors

Author

A. P. Kravets, D. A. Sokolova, and N. L. Kovalchuk

Subjects

mobile elements, gonadal dysgenesis, genomic instability, dynamic effects of chronic exposure., Atomic physics. Constitution and properties of matter, QC170-197

Abstract

Differences in the gonadal dysgenesis frequency as an indicator of the activation of mobile elements were revealed in F1-descendants of natural populations of Drosophіla melanogaster, selected from regions of different radiation impact. Under conditions of additional low-rate chronic irradiation in laboratory conditions for 10 generations, significant differences in changes in the level and dynamics of this indicator were established depending on the accumulated dose of Drosophila populations from the city of Netishin (Khmelnytskyi NPP) and Magarach city.

Published

2021

266. Keratosis follicularis spinulosa decalvans in a woman with XY karyotype.

Author

Linares‐Navarro, Rubén, Castiñeiras‐González, Jose, and Rodríguez‐Prieto, Manuel Á.

Subjects

*KERATOSIS follicularis, *KARYOTYPES, *GONADAL dysgenesis, *THERAPEUTICS, *ECTODERMAL dysplasia

Published

2023

267. MAP3K1-related gonadal dysgenesis: Six new cases and review of the literature.

Author

Granados, Andrea, Alaniz, Veronica, Mohnach, Lauren, Barseghyan, Hayk, Vilain, Eric, Ostrer, Harry, Quint, Elisabeth, Chen, Ming, and Keegan, Catherine

Subjects

MAP3K1, 46, XY DSD, disorders of sex development, gonadal dysgenesis, Adolescent, Child, Child, Preschool, Disorder of Sex Development, 46, XY, Female, Gonadal Dysgenesis, Humans, MAP Kinase Kinase Kinase 1, Male, Mutation, Pedigree, Sex Differentiation

Abstract

Investigation of disorders of sex development (DSD) has resulted in the discovery of multiple sex-determining genes. MAP3K1 encodes a signal transduction regulator in the sex determination pathway and is emerging as one of the more common genes responsible for 46,XY DSD presenting as complete or partial gonadal dysgenesis. Clinical assessment, endocrine evaluation, and genetic analysis were performed in six individuals from four unrelated families with 46,XY DSD. All six individuals were found to have likely pathogenic MAP3K1 variants. Three of these individuals presented with complete gonadal dysgenesis, characterized by bilateral streak gonads with typical internal and external female genitalia, while the other three presented with partial gonadal dysgenesis, characterized by incomplete testicular development, resulting in clitoral hypertrophy with otherwise typical female external genitalia. Testing for MAP3K1 variants should be considered in patients with 46,XY complete or partial gonadal dysgenesis, particularly in families with multiple members affected with 46,XY DSD. Identification of a MAP3K1 variant should prompt an evaluation for DSD in female siblings of the proband.

Published

2017

268. Novel Genomic Variants, Atypical Phenotypes and Evidence of a Digenic/Oligogenic Contribution to Disorders/Differences of Sex Development in a Large North African Cohort

Author

Housna Zidoune, Asmahane Ladjouze, Djalila Chellat-Rezgoune, Asma Boukri, Scheher Aman Dib, Nassim Nouri, Meryem Tebibel, Karima Sifi, Noureddine Abadi, Dalila Satta, Yasmina Benelmadani, Joelle Bignon-Topalovic, Maeva El-Zaiat-Munsch, Anu Bashamboo, and Ken McElreavey

Subjects

disorders/differences in sex development (DSD), gonadal dysgenesis, genetic etiology, digenic/oligogenic, testis, ovary, Genetics, QH426-470

Abstract

In a majority of individuals with disorders/differences of sex development (DSD) a genetic etiology is often elusive. However, new genes causing DSD are routinely reported and using the unbiased genomic approaches, such as whole exome sequencing (WES) should result in an increased diagnostic yield. Here, we performed WES on a large cohort of 125 individuals all of Algerian origin, who presented with a wide range of DSD phenotypes. The study excluded individuals with congenital adrenal hypoplasia (CAH) or chromosomal DSD. Parental consanguinity was reported in 36% of individuals. The genetic etiology was established in 49.6% (62/125) individuals of the total cohort, which includes 42.2% (35/83) of 46, XY non-syndromic DSD and 69.2% (27/39) of 46, XY syndromic DSD. No pathogenic variants were identified in the 46, XX DSD cases (0/3). Variants in the AR, HSD17B3, NR5A1 and SRD5A2 genes were the most common causes of DSD. Other variants were identified in genes associated with congenital hypogonadotropic hypogonadism (CHH), including the CHD7 and PROKR2. Previously unreported pathogenic/likely pathogenic variants (n = 30) involving 25 different genes were identified in 22.4% of the cohort. Remarkably 11.5% of the 46, XY DSD group carried variants classified as pathogenic/likely pathogenic variant in more than one gene known to cause DSD. The data indicates that variants in PLXNA3, a candidate CHH gene, is unlikely to be involved in CHH. The data also suggest that NR2F2 variants may cause 46, XY DSD.

Published

2022

269. Early Bilateral Gonadoblastoma in a Patient with Mixed Gonadal Dysgenesis (Karyotype 45,X/46,XY): Case Report and Review of Literature

Author

Ignas Trainavičius, Darius Dasevičius, Birutė Burnytė, Robertas Kemežys, and Gilvydas Verkauskas

Subjects

Disorders of sex development, Gonadal dysgenesis, Mixed gonadal dysgenesis, 45,X/46,XY mosaicism, Gonadoblastoma, Gonadectomy, Medicine

Abstract

Background: Mixed gonadal dysgenesis is a rare congenital and challenging condition, characterized mainly by 45,X/46,XY karyotype mosaicism, asymmetrical gonadal development and various internal and external genital anatomy. Because of frequent disorder of genital development and a higher risk of germ cell neoplasia, management of these patients is complex and requires multidisciplinary approach. Case: We present a 45,X/46,XY mixed gonadal dysgenesis patient diagnosed with gonadoblastoma in both gonads after bilateral gonadectomy at 1 year of age. Conclusions: Because of high risk for malignant transformation, gonadectomy of a streak-like gonad and biopsy with orchidopexy or gonadectomy of a dysgenetic testicle is recommended at an early age.

Published

2022

270. Case Report: Severe Gonadal Dysgenesis Causing 46,XY Disorder of Sex Development Due to a Novel NR5A1 Variant

Author

Kheloud M. Alhamoudi, Balgees Alghamdi, Abeer Aljomaiah, Meshael Alswailem, Hindi Al-Hindi, and Ali S. Alzahrani

Subjects

NR5A1 mutation and gonadal dysgenesis, DSD, disorders of sex development, ambiguous genitalia, gonadal dysgenesis, NR5A1, Genetics, QH426-470

Abstract

Mutations in the nuclear receptor subfamily 5 group A member 1 (NR5A1) are the underlying cause of 10–20% of 46,XY disorders of sex development (DSDs). We describe a young girl with 46,XY DSD due to a unique novel mutation of the NR5A1 gene. An 11-year-old subject, raised as a female, was noticed to have clitromegly. She looked otherwise normal. However, her evaluation revealed a 46,XY karyotype, moderate clitromegly but otherwise normal female external genitalia, undescended atrophied testes, rudimentary uterus, no ovaries, and lack of breast development. Serum testosterone and estradiol were low, and gonadotropins were elevated. Adrenocortical function was normal. DNA was isolated from the peripheral leucocytes and used for whole exome sequencing. The results were confirmed by Sanger sequencing. We identified a novel mutation in NR5A1 changing the second nucleotide of the translation initiation codon (ATG>ACG) and resulting in a change of the first amino acid, methionine to threonine (p.Met1The). This led to severe gonadal dysgenesis with deficiency of testosterone and anti-Müllerian hormone (AMH) secretion. Lack of the former led to the development of female external genitalia, and lack of the latter allowed the Müllerian duct to develop into the uterus and the upper vagina. The patient has a female gender identity. Bilateral orchidectomy was performed and showed severely atrophic testes. Estrogen/progesterone therapy was initiated with excellent breast development and normal cyclical menses. In summary, we describe a severely affected case of 46,XY DSD due to a novel NR5A1 mutation involving the initiation codon that fully explains the clinical phenotype in this subject.

Published

2022

271. Case Report: Novel Compound Heterozygotic Variants in PPP2R3C Gene Causing Syndromic 46, XY Gonadal Dysgenesis and Literature Review

Author

Wei Zhang, Jiangfeng Mao, Xi Wang, Bang Sun, Zhiyuan Zhao, Xiaoxia Zhang, Min Nie, and Xueyan Wu

Subjects

disorders/differences of sex development(DSD), syndromic 46 XY DSD, gonadal dysgenesis, facial deformity, PPP2R3C mutations, compound heterozygous variants, Genetics, QH426-470

Abstract

Purpose: Patients with syndromic 46, XY disorders/differences of sex development (DSD) are characterized by gonadal and phenotypic genders inconsistent with their chromosomal sexes as well as abnormalities of multiple extragonadal organs. They are caused by mutations in specific genes, which are expressed in the affected organs and regulate their development, and over fourteen genes have been identified. In this study, we aimed to determine the underlying cause of a patient with syndromic 46, XY DSD and review the clinical presentations and genetic findings of all reported similar cases.Methods: Whole-exome sequencing (WES) was performed to find a molecular cause of the patient. In silico tools were used to analyze the pathogenicity of the variants. Reports of cases with similar clinical features and involved genes were summarized by searching through PubMed/MEDLINE using keywords “PPP2R3C” or “G5PR” and “46,XY disorders of sex development”.Results: Compound heterozygous variants (p.F229del/p.G417E) in PPP2R3C were identified in the 24-year-old female by WES and verified by Sanger sequencing. The patient presents complete testicular dysgenesis, low birth weight, facial deformity, cubitus valgus, and decreasing number of CD19+ B lymphocytes and CD4+ T lymphocytes. A total of thirteen 46, XY DSD cases with four homozygous PPP2R3C mutations (p.Leu103Pro, p.Leu193Ser, p.Phe350Ser, and p.Ser216_Tyr218dup) have been reported previously, and their clinical manifestations are roughly similar to those of our patient.Conclusion: Novel compound heterozygous variants in PPP2R3C cause specific syndromic 46, XY gonadal dysgenesis, which broadened the pathogenic variants spectrum of PPP2R3C. The typical phenotype of PPP2R3C mutation is complete 46, XY gonadal dysgenesis with multiple extragonadal anomalies, including facial deformities, skeletal system abnormalities, muscle abnormalities, impaired nervous system, impaired hearing and vision, heart and kidney anomalies, and gastrointestinal dysfunction.

Published

2022

272. Chromosomal abnormalities predisposing to infertility, testing, and management: a narrative review

Author

Tajudeen O. Yahaya, Esther O. Oladele, Daniel Anyebe, Chidiebere Obi, M. D. A. Bunza, Ridwan Sulaiman, and Usman U. Liman

Subjects

Amenorrhea, Azoospermia, Infertility, Gonadal dysgenesis, Spontaneous abortion, Science

Abstract

Abstract Background Much interest has not been placed on the role of chromosomal abnormalities in the pathogenesis and rising prevalence of infertility in recent times. This review was conducted to renew public interest on the chromosomal basis of infertility, testing, and management. Main text Meiotic and post-zygotic mitotic errors may cause infertility-predisposing chromosomal abnormalities, including Klinefelter syndrome, Jacob syndrome, Triple X syndrome, Turner syndrome, and Down syndrome. Chromosomal abnormalities such as deletion, translocation, duplication, inversion, and ring chromosome may also predispose to infertility. Notable features of male chromosomal infertility include spermatogenic failure, characterized by azoospermia, oligospermia, and gonadal dysgenesis, while females include premature ovarian insufficiency, amenorrhea, spontaneous abortion, and gonadal dysgenesis. The risk of these abnormalities is influenced by maternal age and environmental factors such as chemical exposure, smoking, and alcohol consumption. Most chromosomal abnormalities occur spontaneously and are not treatable. However, early prenatal screening and diagnostic tests can lessen the effects of the conditions. There is also a growing belief that certain diets and drugs capable of changing gene expressions can be formulated to neutralize the effects of chromosomal abnormalities. Conclusion Meiotic and mitotic errors during gametogenesis and fetal development, respectively, can cause chromosomal abnormalities, which predispose to infertility. Couples who are at increased risk, particularly those with a family history of infertility and women at an advanced age (≥ 35 years), should seek medical advice before getting pregnant.

Published

2021

273. A Clinical Study to Assess the Efficacy and Safety of DA-3002

Published

2018

274. Growth Hormone Treatment for the Prevention of Short Stature in Young Girls With Turner Syndrome Before the Age of 4 Years

Published

2018

275. Predictive Markers in Growth Hormone Deficiency (GHD) and Turner Syndrome (TS) Children Treated With SAIZEN®

Published

2018

276. Dry Eye in Women With Turner Syndrome and Women With Premature Ovarian Failure

Published

2018

277. Gonads under stress: A systematic review and meta-analysis on the effects of acute psychosocial stress on gonadal steroids secretion in humans.

Author

Domes, Gregor, Linnig, Katrin, and von Dawans, Bernadette

Subjects

*HYPOTHALAMIC-pituitary-gonadal axis, *PSYCHOSOCIAL factors, *SECRETION, *STEROIDS, *LITERATURE reviews, *GONADAL dysgenesis, GONADAL diseases

Abstract

Animal research has shown that the hypothalamus-pituitary-gonadal (HPG) axis is inhibited by (chronic and/or severe) stress, which can lead to impaired fertility and reproductive functioning, presumably caused by the inhibition of gonadal steroid secretion and in interactions with glucocorticoids. However, what has not been clarified is how acute psychosocial stress modulates gonadal steroid secretion in humans. Here we summarize the experimental research on the acute effects of stress on the secretion of gonadal steroids in humans. A systematic literature search revealed 21 studies (with N=881 individuals) measuring testosterone, progesterone or estradiol in response to a standardized acute laboratory stressor in healthy humans. Both our literature review and quantitative meta-analysis suggest that in humans, acute stress stimulates rather than inhibits HPG axis activity, although there is a considerable heterogeneity in the reported methods and results. Increased gonadal steroids in response to acute stress contrasts with many animal studies reporting the opposite pattern, at least regarding severe and/or chronic stressors. We discuss methodological issues and challenges for future research and hope to stimulate experimental studies within this area. A better understanding of these mechanisms is needed, and may have important implications for health and disease, as well as the modulation of various behaviors by acute stressors. • The HPG-axis regulates the release of gonadal steroids and thus mediates reproductive functioning. • Animal studies have reported the inhibition of HPG-axis and reproductive functioning in response to severe/chronic stress. • In humans, experimental studies have provided evidence that acute stress increases the secretion of gonadal steroids. • Methodological and conceptual differences between studies might in part explain these heterogenous results. [ABSTRACT FROM AUTHOR]

Published

2024

278. DHX37 and NR5A1 Variants Identified in Patients with 46,XY Partial Gonadal Dysgenesis

Author

Felipe Rodrigues de Oliveira, Taís Nitsch Mazzola, Maricilda Palandi de Mello, Ana Paula Francese-Santos, Sofia Helena V. de Lemos-Marini, Andrea Trevas Maciel-Guerra, Olaf Hiort, Ralf Werner, Gil Guerra-Junior, and Helena Fabbri-Scallet

Subjects

DHX37, NR5A1, disorders of sex development, gonadal dysgenesis, Science

Abstract

The group of disorders known as 46,XY gonadal dysgenesis (GD) is characterized by anomalies in testis determination, including complete and partial GD (PGD) and testicular regression syndrome (TRS). Several genes are known to be involved in sex development pathways, however approximately 50% of all cases remain elusive. Recent studies have identified variants in DHX37, a gene encoding a putative RNA helicase essential in ribosome biogenesis and previously associated with neurodevelopmental disorders, as a cause of PGD and TRS. To investigate the potential role of DHX37 in disorders of sexual development (DSD), 25 individuals with 46,XY DSD were analyzed and putative pathogenic variants were found in four of them. WES analyses were performed on these patients. In DHX37, the variant p.(Arg308Gln), recurrent associated with DSD, was identified in one patient; the p.(Leu467Val), predicted to be deleterious, was found together with an NR5A1 loss-of-function variant in patient 2; and, the p.(Val999Met) was identified in two unrelated patients, one of whom (patient 3) also carried a pathogenic NR5A1 variant. For both patients carrying DHX37 and NR5A1 pathogenic variants, a digenic inheritance is suggested. Our findings support the importance of DHX37 variants as a cause of disorders of sex development, implying a role in testis development.

Published

2023

279. A Study of PEG-somatropin Injection to Treat Children of Turner Syndrome

Author

Beijing Children's Hospital, The First Affiliated Hospital with Nanjing Medical University, Shanghai Children's Hospital, Children's Hospital of Fudan University, Xinhua Hospital, Shanghai Jiao Tong University School of Medicine, The First Hospital of Jilin University, Jiangxi Province Children's Hospital, Affiliated Hospital of Jiangnan University, and The Children's Hospital of Zhejiang University School of Medicine

Published

2017

280. Gonadoblastoma with Dysgerminoma Presenting as Virilizing Disorder in a Young Child with 46, XX Karyotype: A Case Report and Review of the Literature.

Author

Chandrapattan, Prathamesh, Jena, Amitabh, Patnayak, Rashmi, Mangaraj, Swayamsidha, Naik, Sujata, and Panda, Saroj

Subjects

*GONADAL dysgenesis, *KARYOTYPES, *LITERATURE reviews, *Y chromosome, *GERM cells, *SERTOLI cells

Abstract

Gonadoblastoma is a neoplasm containing an intimate mixture of germ cells and elements resembling immature granulosa or Sertoli cells. It has been considered as in situ germ cell malignancy that can be associated with malignant components. The tumor has been reported to almost exclusively develop in various types of gonadal gene mutation syndromes, such as in pure or mixed gonadal dysgenesis and among females carrying Y chromosome material. However, it can be rarely present in normal women with 46, XX karyotype. Ovarian gonadoblastoma presenting with signs of contrasexual puberty in a young female child with normal 46, XX karyotype is an extremely rare clinical entity and seldom reported in the literature. We report a case of a nine-year-old girl child who presented with signs of virilization and contrasexual pubertal development. A detailed clinical evaluation along with supportive biochemical and radiological findings pointed to the presence of a virilizing ovarian tumor. The patient underwent right salpingo-oophorectomy, pelvic node dissection, and infracolic omentectomy. The excised tumor was confirmed to be gonadoblastoma which was overgrown by dysgerminoma on histopathological evaluation. The presence of associated malignant tumors (like dysgerminoma) should always be ruled out in cases of gonadoblastoma. [ABSTRACT FROM AUTHOR]

Published

2022

281. Varicocoele embolization with sclerosing agents leads to lower radiation exposure and procedural costs than coils: Data from a real‐life before and after study.

Author

Boeri, Luca, Fulgheri, Irene, Cristina, Marco, Biondetti, Pierpaolo, Rossi, Silvia, Grimaldi, Elena, Lucignani, Gianpaolo, Gadda, Franco, Ierardi, Anna Maria, Salonia, Andrea, Viganò, Paola, Somigliana, Edgardo, Carrafiello, Gianpaolo, and Montanari, Emanuele

Subjects

*RADIATION exposure, *LINEAR statistical models, *SEMEN analysis, *THERAPEUTIC embolization, *BODY mass index, *VARICOCELE, *GONADAL dysgenesis

Abstract

Objectives: To investigate clinical outcomes, radiation exposure and procedural costs associated with percutaneous varicocoele embolization using coils and sclerosing agents (SAs) in a cohort of young‐adult men. Materials and methods: Data from consecutive men treated with percutaneous varicocoele embolization using coils and SA between 2017 and 2021 were analyzed. The allocation was based on a change of policy occurred in June 2020 with the substitution of coils with SA (before and after study). Semen analysis values were based on 2010 WHO reference criteria. Anatomic variants of gonadal veins were categorized according to Jargiello et al. Intraoperative radiation dose and procedural costs were collected for each patient. Descriptive statistics and linear regression models were used to describe the association between clinical parameters with procedural costs and radiation exposure. Results: One hundred sixteen men were included, of whom 76 (65.5%) received coils, and 40 (34.5%) received SA. Baseline characteristics of the two study groups did not differ. A type 3 Jargiello anatomic variation of left gonadal vein was found in 45.7% of cases. Radiation dose was lower in the SA group as compared to the coils one (13.2 [7–43] vs. 19.8 [12–57] Gy/cm2; p < 0.001). Similarly, procedural costs were lower for the SA group (169.6 [169–199] € vs. 642.5 [561–775] €; p < 0.001). At follow‐up, pain and sperm variables significantly improved in both groups (p < 0.01), without differences among the embolic materials. Linear regression model revealed that coils use was associated with higher radiation exposure (beta 8.8, p = 0.02) than SA after accounting for anatomic variation of gonadal vein, body mass index, and vascular access. Conclusions: SA and coils for varicocoele embolization are equally safe and effective. The use of SA was associated with lower radiation exposure and procedural costs than coils. These results should be considered in terms of public health cost and patient's safety. [ABSTRACT FROM AUTHOR]

Published

2022

282. 45,X/46,XY Mosaicism with Male Phenotype: Case Report.

Author

Carreño-Martínez, Angie Carolina, Mendoza Rojas, Victor Clemente, Gil Forero, Julian Arturo, Figueroa, Victor Hugo, and Contreras-García, Gustavo Adolfo

Subjects

*GONADAL dysgenesis, *MOSAICISM, *PHENOTYPES, *AORTIC coarctation, *SHORT stature, *SEX differentiation disorders

Abstract

Mixed gonadal dysgenesis is the most common chromosomal abnormality with ambiguous genitalia, defined as a 45,X/46,XY mosaicism. It can present with a normal male phenotype, ambiguous genitalia, or features of Turner syndrome. A 14-year-old patient was referred to the genetics clinic due to hypospadia, cryptorchidism, and aortic coarctation. During the physical examination, short stature, webbed neck, and Blashko lines on his back were noted. He had a previous karyotype reported as normal. However, due to an inadequate evolution and a low resolution on the previous test, a higher resolution karyotype was performed, identifying a mosaicism 45,X/46,XY. A multidisciplinary board examined the case, and follow-up with tumor markers was carried out to evaluate the presence of gonadoblastoma, one of the main complications in these patients. Treatment should be transdisciplinary and focused on the particular characteristics of each case. Other treatment alternatives include corrective surgery and hormonal therapy. [ABSTRACT FROM AUTHOR]

Published

2022

283. The roles of kisspeptin and neurokinin B in GnRH pulse generation in humans, and their potential clinical application.

Author

Anderson, Richard A. and Millar, Robert P.

Subjects

*KISSPEPTINS, *GONADOTROPIN releasing hormone, *KISSPEPTIN neurons, *GONADAL dysgenesis, *CLINICAL medicine, *POLYCYSTIC ovary syndrome

Abstract

The delivery of gonadotropin‐releasing hormone (GnRH) in a pulsatile mode to the gonadotropes has long been known to be essential for normal reproductive function. There have been numerous studies aimed at dissecting out the mechanisms underlying GnRH pulse generation. The discovery of kisspeptin as an upstream regulator of GnRH attracted the possibility that pulsatile kisspeptin governed the pulsatile secretion of GnRH. Subsequent studies have shown the importance of the neurokinin B (NKB) system in modulating kisspeptin secretion and this GnRH. A number of studies in laboratory rodents have supported this notion. By contrast, we present data from clinical studies in men and women, in a range of contexts, showing that continuous infusion of kisspeptin 10 at receptor‐saturating levels gives rise to an increase in luteinizing hormone (LH) (GnRH) pulse frequency. This has been demonstrated in normal healthy and hypogonadal men, in normal women during the mid‐cycle LH surge, in men and women with mutations in the genes encoding NKB or its receptor, neurokinin 3 receptor (NK3R), in women with polycystic ovary syndrome treated with NK3R antagonist, and in women treated with NK3R antagonist during the LH surge. These finds indicate that pulsatile secretion and action of kisspeptin on GnRH neurons is not required for the generation of LH (GnRH) pulses in humans. We also report that there is an absence of desensitization in humans exposed to continuous infusion of kisspeptin‐10 at receptor‐saturating concentrations over 22 h and briefly review GnRH, kisspeptin and NKB analogs and their clinical application. [ABSTRACT FROM AUTHOR]

Published

2022

284. Contribution of Clinical and Genetic Approaches for Diagnosing 209 Index Cases With 46,XY Differences of Sex Development.

Author

Lisboa Gomes, Nathalia, Loch Batista, Rafael, Nishi, Mirian Y., Marcondes Lerário, Antônio, Silva, Thatiana E., de Moraes Narcizo, Amanda, Figueredo Benedetti, Anna Flávia, de Assis Funari, Mariana Ferreira, Faria Junior, José Antônio, Rodrigues Moraes, Daniela, Lousada Quintão, Lia Mesquita, Ribeiro Montenegro, Luciana, Martins Ferrari, Maria Teresa, Jorge, Alexander A., Arnhold, Ivo J. P., Frade Costa, Elaine Maria, Domenice, Sorahia, and Bilharinho Mendonca, Berenice

Subjects

SEX differentiation disorders, GONADAL dysgenesis

Abstract

Context: Massively parallel sequencing (MPS) technologies have emerged as a first-tier approach for diagnosing several pediatric genetic syndromes. However, MPS has not been systematically integrated into the diagnostic workflow along with clinical/biochemical data for diagnosing 46,XY differences of sex development (DSD). Objective: To analyze the contribution of phenotypic classification either alone or in association with genetic evaluations, mainly MPS, for diagnosing a large cohort of 46,XY DSD patients. Design/patients: 209 nonsyndromic 46,XY DSD index cases from a Brazilian DSD center were included. Patients were initially classified into 3 subgroups according to clinical and biochemical data: gonadal dysgenesis (GD), disorders of androgen secretion/action, and DSD of unknown etiology. Molecular genetic studies were performed by Sanger sequencing and/or MPS. Results: Clinical/biochemical classification into either GD or disorders of hormone secretion/action was obtained in 68.4% of the index cases. Among these, a molecular diagnosis was obtained in 36% and 96.5%, respectively. For the remainder 31.6% classified as DSD of clinically unknown etiology, a molecular diagnosis was achieved in 31.8%. Overall, the molecular diagnosis was achieved in 59.3% of the cohort. The combination of clinical/biochemical and molecular approaches diagnosed 78.9% of the patients. Clinical/biochemical classification matched with the genetic diagnosis in all except 1 case. DHX37 and NR5A1 variants were the most frequent genetic causes among patients with GD and DSD of clinical unknown etiology, respectively. Conclusions: The combination of clinical/biochemical with genetic approaches significantly improved the diagnosis of 46,XY DSD. MPS potentially decreases the complexity of the diagnostic workup as a first-line approach for diagnosing 46,XY DSD. [ABSTRACT FROM AUTHOR]

Published

2022

285. Does coronavirus disease 2019 kill more elderly men than women due to different hormonal milieu.

Author

Tandon, Apurva, Tandon, Vishal, Sharma, Sudhaa, and Mahajan, Annil

Subjects

*COVID-19, *OLDER men, *GENDER, *CORONAVIRUS diseases, *COVID-19 pandemic, *GONADAL dysgenesis, *OLDER women

Abstract

Preliminary data depicts a much greater prevalence and high case-fatality rate in advanced age males as compared to age-matched women with severe acute respiratory syndrome-coronavirus-2 infections with high morbidity, mortality, high referral, and admission to intensive care unit with severe sequelae. However, the literature search revealed both for and against studies in this context. Thus, at present, in light of the mixed studies, it cannot be established whether low testosterone levels in aging hypogonadal males create a permissive environment for severe response to coronavirus disease 2019 (COVID-19) infection and can it increase the morbidity or mortality, or on the contrary if the virus inhibits androgen formation. Hence, it is highly warranted to establish the said hypothesis by conducting large statistically powered clinical studies in future. Further, it is highly indicated that impact of sex hormones and gender on the incidence and case fatality of the disease and hormones as a treatment according to sex and gender for COVID requires further scientific research by the research community before it is actually recommended to mitigate the COVID-19 disease course among elderly men and women at large. [ABSTRACT FROM AUTHOR]

Published

2022

286. The radiologist's role in assessing differences of sex development.

Author

Hryhorczuk, Anastasia L., Phelps, Andrew S., Yu, Richard N., and Chow, Jeanne S.

Abstract

When infants are identified with a difference of sex development (DSD), a thoughtful approach to imaging is essential to appropriate clinical management. This review provides a comprehensive guide for radiologists who are tasked with performing this critical assignment. We review the embryologic basis of DSDs, with attention to the imaging findings that can indicate specific diagnoses. We also discuss techniques for optimal imaging, including strategies for identifying the gonads by US, tactics for performing genitograms with fluoroscopy and contrast-enhanced US, and the appropriate utilization of MRI. Finally, we review the clinical data and imaging findings that characterize some of the most common DSDs, including congenital adrenal hyperplasia, complete androgen insensitivity syndrome and gonadal dysgenesis. [ABSTRACT FROM AUTHOR]

Published

2022

287. MAP3K1 Variant Causes Hyperactivation of Wnt4/β-Catenin/FOXL2 Signaling Contributing to 46,XY Disorders/Differences of Sex Development.

Author

Chen, Hong, Chen, Qingqing, Zhu, Yilin, Yuan, Ke, Li, Huizhu, Zhang, Bingtao, Jia, Zexiao, Zhou, Hui, Fan, Mingjie, Qiu, Yue, Zhuang, Qianqian, Lei, Zhaoying, Li, Mengyao, Huang, Wendong, Liang, Li, Yan, Qingfeng, and Wang, Chunlin

Subjects

WNT signal transduction, GONADAL dysgenesis, CHINESE people, MISSENSE mutation, PROTEIN-protein interactions

Abstract

Background: 46,XY disorders/differences of sex development (46,XY DSD) are congenital conditions that result from abnormal gonadal development (gonadal dysgenesis) or abnormalities in androgen synthesis or action. During early embryonic development, several genes are involved in regulating the initiation and maintenance of testicular or ovarian-specific pathways. Recent reports have shown that MAP3K1 genes mediate the development of the 46,XY DSD, which present as complete or partial gonadal dysgenesis. Previous functional studies have demonstrated that some MAP3K1 variants result in the gain of protein function. However, data on possible mechanisms of MAP3K1 genes in modulating protein functions remain scant. Methods: This study identified a Han Chinese family with the 46,XY DSD. To assess the history and clinical manifestations for the 46,XY DSD patients, the physical, operational, ultra-sonographical, pathological, and other examinations were performed for family members. Variant analysis was conducted using both trio whole-exome sequencing (trio WES) and Sanger sequencing. On the other hand, we generated transiently transfected testicular teratoma cells (NT2/D1) and ovary-derived granular cells (KGN), with mutant or wild-type MAP3K1 gene. We then performed functional assays such as determination of steady-state levels of gender related factors, protein interaction and luciferase assay system. Results: Two affected siblings were diagnosed with 46,XY DSD. Our analysis showed a missense c.556A > G/p.R186G variant in the MAP3K1 gene. Functional assays demonstrated that the MAP3K1R186G variant was associated with significantly decreased affinity to ubiquitin (Ub; 43–49%) and increased affinity to RhoA, which was 3.19 ± 0.18 fold, compared to MAP3K1. The MAP3K1R186G led to hyperphosphorylation of p38 and GSK3β, and promoted hyperactivation of the Wnt4/β-catenin signaling. In addition, there was increased recruitment of β-catenin into the nucleus, which enhanced the expression of pro-ovarian transcription factor FOXL2 gene, thus contributing to the 46,XY DSD. Conclusion: Our study identified a missense MAP3K1 variant associated with 46,XY DSD. We demonstrated that MAP3K1R186G variant enhances binding to the RhoA and improves its own stability, resulting in the activation of the Wnt4/β-catenin/FOXL2 pathway. Taken together, these findings provide novel insights into the molecular mechanisms of 46,XY DSD and promotes better clinical evaluation. [ABSTRACT FROM AUTHOR]

Published

2022

288. Masculinizing surgery in disorders/differences of sex development: clinician‐ and participant‐evaluated appearance and function.

Author

van de Grift, Tim C., Rapp, Marion, Holmdahl, Gundela, Duranteau, Lise, Nordenskjold, Agneta, Kohler, Birgit, Neumann, Uta, Cohen‐Kettenis, Peggy, Kreukels, Baudewijntje, de Vries, Annelou, Arlt, Wiebke, Wiesemann, Claudia, Slowikowska‐Hilczer, Jolanta, Thyen, Ute, de la Perriere, Aude Brac, Sultan, Charles, Paris, Francoise, Reisch, Nicole, Richter‐Unruh, Annette, and Claahsen–van der Grinten, Hedi

Subjects

*PATIENTS' attitudes, *ANDROGEN-insensitivity syndrome, *GONADAL dysgenesis, *SEX differentiation disorders, *PHYSICIANS

Abstract

Objectives: To report the long‐term follow‐up outcomes of masculinizing surgery in disorders/differences of sex development (DSD), including both physicians' and patients' perspectives on appearance and functional outcome, including sexuality. Patients and Methods: In total, 1040 adolescents (age ≥16 years) and adults with a DSD took part in this multicentre cross‐sectional clinical study in six European countries in 2014/2015. Of those, 150 living in other than the female gender had some kind of masculinizing surgery: hypospadias repair, orchidopexy, breast reduction and/or gonadectomy. The study protocol included medical data collection, an optional genital examination, and patient‐reported outcomes including satisfaction with appearance and current sexual functioning. Results: Diagnoses included partial and mixed gonadal dysgenesis (45,XO/46,XY; n = 38), Klinefelter syndrome/46,XX males (n = 57), and various 46,XY DSDs (n = 42; e.g. partial androgen insensitivity syndrome, severe hypospadias) and 13 with other diagnoses. Of the participants, 84 underwent hypospadias surgery, 86 orchidopexy, 52 gonadectomy and 32 breast reduction (combinations possible). Physicians evaluated anatomical appearance at genital examination as poor in approximately 11% of patients. After hypospadias surgery, 38% of participants reported that they were (very) dissatisfied with anatomical appearance and 20% with function. The physician and patient evaluations were moderately correlated (r = 0.43). Conclusion: The majority of participants were neutral to satisfied with the appearance and function in the long‐term after masculinizing surgery. Given the initial severe phenotype and a risk of unsatisfactory results after masculinizing surgery in DSD, treatment should be handled by experienced multidisciplinary teams in order to optimize the postoperative results. [ABSTRACT FROM AUTHOR]

Published

2022

289. Pathogenic Variants in MAP3K1 Cause 46,XY Gonadal Dysgenesis: A Review.

Author

Ostrer, Harry

Subjects

*GONADAL dysgenesis, *HUMAN abnormalities, *MITOGEN-activated protein kinases, *PROTEIN domains, *GENETIC variation, *STRIPES

Abstract

Pathogenic variants in the MAP3K1 gene are an important cause of 46,XY non-syndromic partial and complete gonadal dysgenesis, accounting for at least 4% of cases. Inheritance occurs in a sex-limited, autosomal dominant fashion with virtually complete penetrance in 46,XY individuals. 46,XX carriers appear to have normal fertility and no developmental abnormalities. Pathogenic variants occur almost exclusively within known domains of the MAP3K1 protein, facilitating annotation when identified. Where studied, these variants have been modeled to alter the local MAP3K1 folding and surface domains and have been shown to alter interactions with known binding partners. The net effect of these variants is to increase phosphorylation of downstream targets ERK1, ERK2, and p38, resulting in multiple gain-of-function effects interfering with testis determination and enabling ovarian determination. [ABSTRACT FROM AUTHOR]

Published

2022

290. DHX37 and 46,XY DSD: A New Ribosomopathy?

Author

McElreavey, Kenneth, Pailhoux, Eric, and Bashamboo, Anu

Subjects

*ORGANELLE formation, *MISSENSE mutation, *GENETIC variation, *CONGENITAL disorders, *GONADAL dysgenesis

Abstract

Recently, a series of recurrent missense variants in the RNA-helicase DHX37 have been reported associated with either 46,XY gonadal dysgenesis, 46,XY testicular regression syndrome (TRS), or anorchia. All affected children have non-syndromic forms of disorders/differences of sex development (DSD). These variants, which involve highly conserved amino acids within known functional domains of the protein, are predicted by in silico tools to have a deleterious effect on helicase function. DHX37 is required for ribosome biogenesis in eukaryotes, and how these variants cause DSD is unclear. The relationship between DHX37 and human congenital disorders is complex as compound heterozygous as well as de novo heterozygous missense variants in DHX37 are also associated with a complex congenital developmental syndrome (NEDBAVC, neurodevelopmental disorder with brain anomalies and with or without vertebral or cardiac anomalies; OMIM 618731), consisting of microcephaly, global developmental delay, seizures, facial dysmorphia, and kidney and cardiac anomalies. Here, we will give a brief overview of ribosome biogenesis and the role of DHX37 in this process. We will discuss variants in DHX37, their contribution to human disease in the general context of human ribosomopathies, and the possible disease mechanisms that may be involved. [ABSTRACT FROM AUTHOR]

Published

2022

291. The Desert Hedgehog Signalling Pathway in Human Gonadal Development and Differences of Sex Development.

Author

Pachernegg, Svenja, Georges, Elizabeth, and Ayers, Katie

Subjects

*CELLULAR signal transduction, *GONADAL dysgenesis, *DESERTS, *PERIPHERAL neuropathy, *TESTIS development

Abstract

While the Hedgehog signalling pathway is implicated in numerous developmental processes and maladies, variants in the Desert Hedgehog (DHH) ligand underlie a condition characterised by 46,XY gonadal dysgenesis with or without peripheral neuropathy. We discuss here the role and regulation of DHH and its signalling pathway in the developing gonads and examine the current understanding of how disruption to this pathway causes this difference of sex development (DSD) in humans. [ABSTRACT FROM AUTHOR]

Published

2022

292. DMRT1: An Ancient Sexual Regulator Required for Human Gonadogenesis.

Author

Zarkower, David and Murphy, Mark W.

Subjects

*GERM cell differentiation, *TESTIS physiology, *SOMATIC cells, *GRANULOSA cells, *GONADAL dysgenesis

Abstract

Transcriptional regulators related to the invertebrate sexual regulators doublesex and mab-3 occur throughout metazoans and control sex in most animal groups. Seven of these DMRT genes are found in mammals, and mouse genetics has shown that one, Dmrt1, plays a crucial role in testis differentiation, both in germ cells and somatic cells. Deletions and, more recently, point mutations affecting human DMRT1 have demonstrated that its heterozygosity is associated with 46,XY complete gonadal dysgenesis. Most of our detailed knowledge of DMRT1 function in the testis, the focus of this review, derives from mouse studies, which have revealed that DMRT1 is essential for male somatic and germ cell differentiation and maintenance of male somatic cell fate after differentiation. Moreover, ectopic DMRT1 can reprogram differentiated female granulosa cells into male Sertoli-like cells. The ability of DMRT1 to control sexual cell fate likely derives from at least 3 properties. First, DMRT1 functionally collaborates with another key male sex regulator, SOX9, and possibly other proteins to maintain and reprogram sexual cell fate. Second, and related, DMRT1 appears to function as a pioneer transcription factor, binding "closed" inaccessible chromatin and promoting its opening to allow binding by other regulators including SOX9. Third, DMRT1 binds DNA by a highly unusual form of interaction and can bind with different stoichiometries. [ABSTRACT FROM AUTHOR]

Published

2022

293. Novel androgen receptor gene variant containing a frameshift mutation in a patient with complete androgen insensitivity syndrome.

Author

Guangjie Chen, Dongyan Zhao, Linfeng Zhu, Yijun Zhao, Jiahua Zhang, Xiaohao Wang, Hongjuan Tian, Daxing Tang, Qiang Shu, and Shenglong Qiao

Subjects

*ANDROGEN receptors, *ANDROGEN-insensitivity syndrome, *FRAMESHIFT mutation, *GENETIC variation, *VULVA, *GONADAL dysgenesis

Abstract

A variety of mutations in the androgen receptor (AR) gene are linked to androgen insensitivity syndrome (AIS). AIS is the most common specific cause of 46, XY disorder in sex development. Here, we reported a patient which presented as a female with 46, XY karyotype and normal female external genitalia. The patient was diagnosed with complete AIS caused by a novel mutation (NM_000044, c.2678- 2726del, p. Pro893Leufs*35) in the AR gene. Targeted exome sequencing was used to detect the patient's androgen receptor gene mutations. Sanger sequencing was used to validate the mutation. This study showed that a novel mutation of the AR gene can cause complete AIS; the study also broadened the AR mutation spectrum and indicated that targeted exome sequencing could help facilitate the diagnosis of complicated disorders in sexual development. [ABSTRACT FROM AUTHOR]

Published

2022

294. Dissecting Gonadoblastoma of the Ovary Coexistent with an Atypical Endometriotic Cyst: Incidental Detection in Cystectomy Specimen of a Woman with 46,XX Karyotype.

Author

Jung, Hera, Yun, Bo Seong, Jung, Yoon Yang, and Kim, Hyun-Soo

Subjects

*KARYOTYPES, *OVARIES, *CYSTECTOMY, *CYSTS (Pathology), *GERM cells, *GONADAL dysgenesis

Abstract

Dissecting gonadoblastoma (DGB) of the ovary, a recently described terminology, defines a unique distribution of neoplastic germ cells. Here, we report a case of incidental DGB coexistent with an atypical endometriotic cyst occurring in a 23-year-old woman. The ovarian cyst was lined by endometrial-like glands and stroma. Some glands displayed nuclear enlargement and hyperchromasia, and abundant eosinophilic cytoplasm with occasional intracytoplasmic hemosiderin and mucin vacuoles. The neoplastic germ cells resembled those of ovarian dysgerminoma and were diffusely distributed within the ovarian stroma, which was stretched around the wall of the endometriotic cyst. These cells were arranged in nests and cords, possessing clear cytoplasm and centrally located round nuclei with prominent nucleoli and occasional mitoses. Chromosomal analysis revealed a 46,XX karyotype. We describe the clinical, histological, immunophenotypical, and genetic features of ovarian DGB incidentally detected in the ovarian cystectomy specimen of a woman with normal female karyotype. [ABSTRACT FROM AUTHOR]

Published

2022

295. Disorders of Sexual Development-Pathological Profile of 45 Cases at a Tertiary Care Centre.

Author

FERNANDES, GWENDOLYN, MHASHETE, POOJA, and DESALE, MINAL

Subjects

*SEX differentiation disorders, *SEX (Biology), *GONADAL dysgenesis, *TURNER'S syndrome, *BENIGN tumors, *ANDROGEN-insensitivity syndrome

Abstract

Disorders of Sexual Development (DSD) are rare syndromes, which show congenital discordance between chromosomal, gonadal and phenotypic sex. A retrospective analysis was performed to analyse the histopathological profile and spectrum of a large number of cases of DSD received at a tertiary care center. There were 45 cases of DSD encountered over a period of eight years, from January 2012 to December 2020. Detailed evaluation of each case with respect to demographic details, clinical features, imaging and pathology was done. All cases were classified as per Chicago Consensus Classification (2006) modified in 2010. The 46, XY DSD were the most common 26 (57.78%) cases, followed by sex chromosomal DSD 14 (31.1%) and 46,XX, DSD 5 (11.1%). Among 46, XY DSD, Complete Gonadal Dysgenesis (CGD) (Swyer syndrome) and Complete Androgen Insensitivity Syndrome (CAIS) had the highest number of cases, with 30.77% cases of each. Among 46XX, DSD, cases of ovotesticular DSD amounted to 80%. In sex chromosomal DSD, cases of Mixed Gonadal Dysgenesis (MGD) amounted to 78.57%. Out of 45 cases studied in this series, 20% cases showed neoplasms, of which 8.89% were malignancies. Nine out of 45 (20%) patients had neoplasms, out of which 5 (55.6%) had benign tumours while 4 (44.4%) had malignant tumours. Five patients had gonadoblastoma and three of these had coexistent dysgerminoma. Two patients had sertoli cell adenomas, one seminoma and one serous cystadenoma. Frequent clinical features noted were primary amenorrhea seen in 25 (55.5%) cases and ambiguous genitalia seen in 18 (40%) cases, while the most common location of gonad was intra-abdominal in 30 (66.6%) cases. Streak gonads were seen in CGD, MGD and Turner's syndrome. Malignant germ cell tumours were seen in CGD and CAIS. Early diagnosis, good histopathology and follow-up are essential in the management of DSDs. [ABSTRACT FROM AUTHOR]

Published

2022

296. Early-Onset Glaucoma in egl1 Mice Homozygous for Pitx2 Mutation.

Author

Kodati, Bindu, Merchant, Shawn A., Millar, J. Cameron, and Liu, Yang

Subjects

CONGENITAL glaucoma, SLIT lamp microscopy, CILIARY body, RETINAL ganglion cells, AQUEOUS humor, CORNEAL opacity, GONADAL dysgenesis

Abstract

Mutations in PITX2 cause Axenfeld–Rieger syndrome, with congenital glaucoma as an ocular feature. The egl1 mouse strain carries a chemically induced Pitx2 mutation and develops early-onset glaucoma. In this study, we characterized the glaucomatous features in egl1 mice. The eyes of egl1 and C57BL/6J control mice were assessed by slit lamp examination, total aqueous humor outflow facility, intraocular pressure (IOP) measurement, pattern electroretinography (PERG) recording, and histologic and immunohistochemistry assessment beginning at 3 weeks and up to 12 months of age. The egl1 mice developed elevated IOP as early as 4 weeks old. The IOP elevation was variable and asymmetric within and between the animals. The aqueous humor outflow facility was significantly reduced in 12-month-old animals. PERG detected a decreased response at 2 weeks after the development of IOP elevation. Retinal ganglion cell (RGC) loss was detected after 8 weeks of IOP elevation. Slit lamp and histologic evaluation revealed corneal opacity, iridocorneal adhesions (anterior synechiae), and ciliary body atrophy in egl1 mice. Immunohistochemistry assessment demonstrated glial cell activation and RGC axonal injury in response to IOP elevation. These results show that the eyes of egl1 mice exhibit anterior segment dysgenesis and early-onset glaucoma. The egl1 mouse strain may represent a useful model for the study of congenital glaucoma. [ABSTRACT FROM AUTHOR]

Published

2022

297. Cytogenetic abnormalities in essential thrombocythemia: Clinical and molecular correlates and prognostic relevance in 809 informative cases.

Author

Gangat, Naseema, Jadoon, Yamna, Szuber, Natasha, Hanson, Curtis A., Wolanskyj-Spinner, Alexandra P., Ketterling, Rhett P., Pardanani, Animesh, and Tefferi, Ayalew

Subjects

Y chromosome, THROMBOCYTOSIS, LEUKOCYTE count, KARYOTYPES, GONADAL dysgenesis, HUMAN abnormalities

Abstract

Cytogenetic studies among 809 consecutive patients with essential thrombocythemia (ET; median age 59 years; 65% females) revealed normal karyotype in 754 (93%), loss of chromosome Y only (-Y) in 16 (2%), and abnormalities other than -Y in 39 (4.8%), the most frequent being sole 20q- (n = 8). At presentation, abnormal karyotype, excluding -Y, was associated with older age (p = 0.04), higher leukocyte count (p = 0.03) and arterial thrombosis history (p = 0.02); no associations were apparent for JAK2/CALR/MPL mutations whereas ASXL1 mutations clustered with normal karyotype/-Y and TP53 with abnormal karyotype. Survival was significantly shorter in patients with abnormal karyotype or -Y, compared to those with normal karyotype (median 12, 10, and 21 years, respectively; p < 0.0001). During multivariable analysis that included IPSET (international prognostic score for ET) variables, abnormal karyotype (p < 0.01, HR 2.0), age >60 years (p < 0.01, HR 4.5), leukocytosis >11 × 109/L (p < 0.01, HR 1.5), and male gender (p < 0.01, HR 1.4) were independently associated with inferior survival; abnormal karyotype and age >60 years remained significant, along with SF3B1/SRSF2/U2AF1/TP53 mutations (p = 0.04; HR 2.9), when the latter was included in the multivariable model. The current study suggests prognostic relevance for karyotype in ET. [ABSTRACT FROM AUTHOR]

Published

2022

298. Critical Roles of the Circadian Transcription Factor BMAL1 in Reproductive Endocrinology and Fertility.

Author

Jiang, Yin, Li, Shiping, Xu, Wenming, Ying, Junjie, Qu, Yi, Jiang, Xiaohui, Zhang, Ayuan, Yue, Yan, Zhou, Ruixi, Ruan, Tiechao, Li, Jinhui, and Mu, Dezhi

Subjects

ENDOCRINOLOGY of human reproduction, TRANSCRIPTION factors, GENITALIA, SMALL interfering RNA, FERTILITY, GONADAL dysgenesis

Abstract

Brain and muscle aryl-hydrocarbon receptor nuclear translocator like protein1 (BMAL1), a core component of circadian oscillation, is involved in many physiological activities. Increasing evidence has demonstrated the essential role of BMAL1 in reproductive physiology. For instance, BMAL1 -knockout (KO) mice were infertile, with impaired reproductive organs and gametes. Additionally, in BMAL1 -KO mice, hormone secretion and signaling of hypothalamus-pituitary-gonadal (H-P-G) hormones were also disrupted, indicating that H-P-G axis was impaired in BMAL1 -KO mice. Moreover, both BMAL1 -KO mice and BMAL1-knockdown by small interfering RNA (siRNA) in vitro cultured steroidogenic cells showed that BMAL1 was associated with gonadal steroidogenesis and expression of related genes. Importantly, BMAL1 also participates in pathogenesis of human reproductive diseases. In this review, we elaborate on the impaired reproduction of BMAL1-KO mice including the reproductive organs, reproductive endocrine hormones, and reproductive processes, highlighting the vital role of BMAL1 in fertility and reproductive endocrinology. [ABSTRACT FROM AUTHOR]

Published

2022

299. Ambiguous Genitalia and Problems with Sexual Differentiation

Author

Angulo, Moris, Martin, Gilbert I., editor, and Rosenfeld, Warren, editor

Published

2019

300. Fertility Preservation in Patients with Disorders (Differences) of Sex Development

Author

Chen, Diane, Johnson, Emilie K., Finlayson, Courtney, Woodruff, Teresa K., editor, Shah, Divya K., editor, and Vitek, Wendy S., editor

Published

2019