Your search keyword '"ANDROGEN INSENSITIVITY SYNDROME"' showing total 757 results

1. Novel pathogenic variants in the androgen receptor gene associated with androgen insensitivity syndrome identified through exome sequencing and in silico analysis

Author

Li, Cui, Wang, Xiaoyan, Wang, Xiang, Li, Xu, Chen, Wei, Zhao, Minggang, Liu, Xiaogang, Li, Pingping, and Xue, Mei

Published

2023

2. Expanding the Molecular Landscape of Androgen Insensitivity Syndrome Through Next-Generation Sequencing

Author

Kałużewski T, Pinkier I, Wysocka U, Sałamunia J, Kępczyński Ł, Piotrowicz M, Kałużewski B, and Gach A

Subjects

androgen insensitivity syndrome, ais, androgen receptor gene, ar gene, next-generation sequencing, ngs, disorders of sex development, complete androgen insensitivity syndrome, cais., Medicine (General), R5-920, Genetics, QH426-470

Abstract

Tadeusz Kałużewski,1,2 Iwona Pinkier,1 Urszula Wysocka,1 Jordan Sałamunia,2 Łukasz Kępczyński,1,2 Małgorzata Piotrowicz,1 Bogdan Kałużewski,2 Agnieszka Gach1 1Department of Genetics, Polish Mother’s Memorial Hospital Research Institute, Lodz, 93-338, Poland; 2R&D Division, Laboratory of Medical Genetics, GENOS Sp. z o.o., Lodz, 91-033, PolandCorrespondence: Tadeusz Kałużewski, Email tadeusz.kaluzewski@iczmp.edu.plAbstract: Androgen insensitivity syndrome (AIS) is an X-linked genetic disorder caused by mutations in the androgen receptor gene (AR), leading to impaired androgen signaling and resulting in varying degrees of undermasculinization in individuals with a 46,XY karyotype. This study aimed to expand the molecular landscape of AIS by identifying and characterizing pathogenic variants in the AR gene via next-generation sequencing (NGS). Molecular diagnostics revealed eight distinct variants within the AR gene, two of which had not been previously described. These include the following novel variants: c.3G>A, and c.1344_1345insTA. This study broadens the spectrum of known AR gene mutations associated with AIS and highlights the critical role of molecular diagnostics in the accurate classification of variants. These findings will aid in enhancing the clinical management and genetic counseling of individuals affected by AIS.Keywords: androgen insensitivity syndrome, AIS, androgen receptor gene, AR gene, next-generation sequencing, NGS, disorders of sex development, complete androgen insensitivity syndrome, CAIS

Published

2024

3. Diverse phenotypes and fertility outcomes of patients with androgen insensitivity syndrome in a Chinese family harboring identical AR gene variant

Author

Hao Geng, Dongdong Tang, Kuokuo Li, Chuan Xu, Chao Wang, Xiansheng Zhang, Xiaojin He, and Yunxia Cao

Subjects

Androgen insensitivity syndrome, AR, Phenotype diversity, Fertility outcomes, Androgens concentration, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Androgen insensitivity syndrome (AIS) is a rare genetic disorder characterized by resistance to androgens, mainly due to mutations in the androgen receptor (AR) gene. It can manifest as complete AIS, partial AIS and mild AIS. While there have been studies linking specific AR gene mutations to AIS phenotypes, different clinical AIS phenotypes are also reported in patients with the same AR gene mutation. So far, the precise correlations between phenotypes and genotypes remain incompletely understood. Methods We conducted a thorough investigation involving four patients diagnosed with different types of AIS from a single Chinese family. Clinical manifestations, laboratory examinations, and fertility outcomes were well-documented. Furthermore, we performed genetic sequencing to detect possible pathogenetic variants. Results Whole exome sequencing identified a hemizygous missense variant (c.2263T > C; p.Phe755Leu) of AR gene in all four affected patients with different degrees of undermasculinisation and heterogeneous spermatogenesis. The proband, diagnosed with partial AIS, opted for treatment with donated sperm due to non-obstructive azoospermia, while their older sibling, diagnosed with complete AIS, was raised as a girl. His two maternal uncles were both diagnosed with mild AIS, the older uncle fathered two girls naturally, whereas the younger uncle utilized assisted reproductive technology to conceive a boy because of severe oligoasthenozoospermia. Conclusion Our study first identified the same AR variant (c.2263T > C;p.Phe755Leu) in four affected patients displaying highly diverse phenotypes of AIS and fertility outcomes, thereby significantly expanding the phenotypic spectrum of AIS. Notably, we presented a clear insight into different fertility outcomes of AIS patients with identical AR (c.2263T > C;p.Phe755Leu) variant, which provided reliable evidence that males harboring this variant may obtain biological offspring naturally or in combination with assisted reproductive technology. Furthermore, our study underscored the potential role of androgen concentration in shaping the phenotypic diversity of AIS, warranting further investigation.

Published

2024

4. Diverse phenotypes and fertility outcomes of patients with androgen insensitivity syndrome in a Chinese family harboring identical AR gene variant.

Author

Geng, Hao, Tang, Dongdong, Li, Kuokuo, Xu, Chuan, Wang, Chao, Zhang, Xiansheng, He, Xiaojin, and Cao, Yunxia

Subjects

ANDROGEN-insensitivity syndrome, REPRODUCTIVE technology, ANDROGEN receptors, GENETIC variation, FERTILITY

Abstract

Background: Androgen insensitivity syndrome (AIS) is a rare genetic disorder characterized by resistance to androgens, mainly due to mutations in the androgen receptor (AR) gene. It can manifest as complete AIS, partial AIS and mild AIS. While there have been studies linking specific AR gene mutations to AIS phenotypes, different clinical AIS phenotypes are also reported in patients with the same AR gene mutation. So far, the precise correlations between phenotypes and genotypes remain incompletely understood. Methods: We conducted a thorough investigation involving four patients diagnosed with different types of AIS from a single Chinese family. Clinical manifestations, laboratory examinations, and fertility outcomes were well-documented. Furthermore, we performed genetic sequencing to detect possible pathogenetic variants. Results: Whole exome sequencing identified a hemizygous missense variant (c.2263T > C; p.Phe755Leu) of AR gene in all four affected patients with different degrees of undermasculinisation and heterogeneous spermatogenesis. The proband, diagnosed with partial AIS, opted for treatment with donated sperm due to non-obstructive azoospermia, while their older sibling, diagnosed with complete AIS, was raised as a girl. His two maternal uncles were both diagnosed with mild AIS, the older uncle fathered two girls naturally, whereas the younger uncle utilized assisted reproductive technology to conceive a boy because of severe oligoasthenozoospermia. Conclusion: Our study first identified the same AR variant (c.2263T > C;p.Phe755Leu) in four affected patients displaying highly diverse phenotypes of AIS and fertility outcomes, thereby significantly expanding the phenotypic spectrum of AIS. Notably, we presented a clear insight into different fertility outcomes of AIS patients with identical AR (c.2263T > C;p.Phe755Leu) variant, which provided reliable evidence that males harboring this variant may obtain biological offspring naturally or in combination with assisted reproductive technology. Furthermore, our study underscored the potential role of androgen concentration in shaping the phenotypic diversity of AIS, warranting further investigation. [ABSTRACT FROM AUTHOR]

Published

2024

5. Molecular mechanism of androgen receptor mutation in multigenerational mild androgen insensitivity syndrome

Author

Ravind Pandher, Ruby Chang, Yiqun Chang, David E Hibbs, Jonathan J Du, Kristine McGrath, Alison Heather, Veena Jayadev, and David J Handelsman

Subjects

androgen insensitivity syndrome, androgen receptor, structural molecular modeling, clinical genetics, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Objective: Androgen insensitivity syndrome (AIS) due to androgen receptor (AR) mutations creates a spectrum of clinical presentations based on residual AR function with the mildest impairment creating mild AIS (MAIS) whose undefined molecular mechanism and subtle clinical features leave it less understood and underdiagnosed. Design: In silico modeling and in vitro androgen bioassay of the mutated AR are used to identify its structural and physiological mechanism. Clinical features and responses to high-dose testosterone treatment of three cases of MAIS across a six-generation family pedigree are described. Methods: Structural and dynamic in silico molecular modeling and in vitro yeast-based androgen bioassays of the mutant AR are employed. Three cases of MAIS with consistent (gynecomastia and micropenis) and variable (infertility) clinical features across generations are reported, and the effects of high-dose testosterone treatment are studied. Results: The missense AR exon 8 mutation (nucleotide aga → gga, p.R872G arginine to glycine), known to cause an increased ligand dissociation rate in mutant AR in binding assays, was analyzed. Modeling shows that the mutation weakens the closure energy of the ‘lid’ of the ligand-binding pocket, allowing easier ligand dissociation from the binding site but with unimpaired in vitro androgen bioactivity. High-dose testosterone treatment for 3 years in one young man caused increased virilization and height growth but was ineffective for treating micropenis. Genetic counseling allowed effective prediction of MAIS risks in progeny for carrier and noncarrier sisters. Conclusions: The differential diagnosis and clinical management of MAIS is reviewed. The novel molecular mechanism of an AR ligand-binding domain mutation in MAIS may be present in other cases of MAIS.

Published

2024

6. A Very Early Diagnosis of Complete Androgen Insensitivity Syndrome Due to a Novel Variant in the AR Gene: A Neonatal Case Study.

Author

Ferrante, Rossella, Tumini, Stefano, Saltarelli, Maria Alessandra, Di Rado, Sara, Scorrano, Vincenzo, Tommolini, Maria Lucia, Zucchelli, Mirco, Lauriola, Federico, Lisi, Gabriele, Lauriti, Giuseppe, Marino, Nino, Stuppia, Liborio, Rossi, Claudia, and Bucci, Ines

Subjects

ANDROGEN-insensitivity syndrome, SEX differentiation disorders, ANDROGEN receptors, GENETIC variation, MISSENSE mutation

Abstract

Androgen insensitivity syndrome (AIS) is one of the most common Disorders of Sexual Differentiation (DSDs). AIS is characterized by an X-linked recessive inheritance pattern associated with variants in the androgen receptor (AR) gene that affects the masculinization process in individuals with XY karyotype. Here, we report a neonatal case of a very early diagnosis of complete AIS due to a novel variant in the AR gene. In the present case, after the clinical evaluation, the infant has undergone the following tests: biochemical analyses, including newborn screening workflow, karyotype analysis, and Next-Generation Sequencing (NGS) panel of 50 genes involved in DSDs. The NGS analysis identified a missense variant, c.2108C>A, in the AR gene. According to a cytogenetic analysis, the patient presented a 46, XY karyotype, thus the resulting hemizygote for the AR gene variant. The variant is not currently described in the literature nor in the ClinVar database. However, according to computational models, the variant could have a pathogenetic effect. This clinical case reveals a novel variant of the AR gene with a possible pathogenetic effect associated with AIS and highlights the importance of a multidisciplinary approach for the timely diagnosis and appropriate follow-up of the patient. [ABSTRACT FROM AUTHOR]

Published

2024

7. Preimplantation Genetic Diagnosis of Androgen Resistance Syndrome Caused by Mutation on the AR Gene in Vietnam

Author

Tung NT, Sang TT, Khoa TV, Phong NV, and Phuong TH

Subjects

androgen insensitivity syndrome, ais, ar gene, preimplantation genetic diagnosis, short tandem repeats, str., Medicine (General), R5-920, Genetics, QH426-470

Abstract

Trieu Tien Sang,1 Khoa Tran Van,1 Nguyen Thanh Tung,2 Phong Nguyen Van,1 Phuong Tran Hoang3 1Department of Biology and Medical Genetics, Vietnam Military Medical University, Hanoi, 10000, Vietnam; 2Military Institute of Clinical Embryology and Histology, Vietnam Military Medical University, Hanoi, 10000, Vietnam; 3Department of Oncology, 108 Military Central Hospital, Hanoi, 10000, VietnamCorrespondence: Trieu Tien Sang, Vietnam Military Medical University, Hanoi, 10000, Vietnam, Email trieusangk83@yahoo.com.vnBackground: Androgen resistance syndrome or androgen insensitivity syndrome (AIS – Androgen Insensitivity Syndrome, OMIM 300068) is an X-linked recessive genetic syndrome causing disorders of sexual development in males. This disease is caused by mutations in the AR gene located on the X chromosome, which encodes the protein that structures the androgen receptor, with the role of receiving androgens. Mutation of the AR gene causes complete or partial loss of androgen receptor function, thereby androgen not being obtained and exerting its effect on target organs, resulting in abnormalities of the male reproductive system due to this organ system, differentiating towards feminization under the influence of estrogen. Disease prevention can be achieved by using pre-implantation genetic diagnosis, which enables couples carrying the mutation to have healthy offspring.Aim: To carry out preimplantation genetic diagnosis of androgen resistance syndrome.Methods: Sanger sequencing was used to detect the mutation in the blood samples of the couple, their son, and 01 embryo that were biopsied on the fifth day based on the findings of next-generation sequencing (NGS) of the affected son. We combined Sanger sequencing and linkage analysis using short tandem repeats (STR) to provide diagnostic results.Results: We performed preimplantation genetic diagnosis for AIS on an embryo from a couple who had previously had an affected son. Consequently, one healthy embryo was diagnosed without the variant NM_000044: c.796del (p.Asp266IlefsTer30).Conclusion: We report on a novel variant (NM_000044: c.796del (p.Asp266IlefsTer30)) in the AR gene discovered in Vietnam. The developed protocol was helpful for the preimplantation genetic diagnosis process to help families with the monogenic disease of AIS but wish to have healthy children.Keywords: androgen insensitivity syndrome, AIS, AR gene, preimplantation genetic diagnosis, short tandem repeats, STR

Published

2024

8. A CASE REPORT OF COMPLETE ANDROGEN INSENSITIVITY SYNDROME RISING A CONCERN ABOUT THE TIME OF SURGERY AND THE ROLE OF PARENTS' BEHAVIOR

Author

Victoria Spasova, Liliya Koleva, Svetlana Shumarova, Diana Hristova, Ventsislava Pencheva, Anatoli Kolev, Bozhidar Karamishev, Daria Koleva, Vladislav Petkov, Svetozar Marangozov, and Vesela Karamisheva

Subjects

androgen insensitivity syndrome, surgery, malignancy, disorders of sex development, psychology impact, Dentistry, RK1-715, Medicine (General), R5-920

Abstract

Purpose: This case study refers to a case of complete androgen insensitivity syndrome, which presented with amenorrhea back in the past. Case: After conformation of the diagnosis, parents decided not to reveal the condition’s specifics to the patient. At the age of 34 years, she attended our hospital with abdominal swelling, and the following CT scan showed an abdominal mass arising from the ovary of 13 cm x 14 cm size. A laparotomy was done, and a mixture of solid and cystic mass of 20 cm in diameter was found and removed with the ovary. Histopathology of the tumor showed features of testicular seminoma. Conclusion: The aim of this case report is to outline the difficulties in choosing whether and when to do the gonadectomy and whether and how to explain the condition to the patient.

Published

2024

9. Detection of Molecular Variations at Androgen Receptor Gene in 46,XY Differences in Sex Development Cases

Author

Nanis S. Marzuki, Hannie D. Kartapradja, Farah N. Coutrier, Irfan Wahyudi, and Jose R.L. Batubara

Subjects

46,xy dsd, androgen insensitivity syndrome, ar gene, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Introduction: One of the common causes of 46,XY differences in sex development (DSD) cases is androgen insensitivity syndrome. This X-linked recessive inherited condition is associated with pathological variations of the AR gene, leading to defects in androgen action. Affected 46,XY infants or individuals experience variable degrees of undervirilization and those with severe form will have female-like external genitalia. Therefore, they were more likely assigned and reared as females. The confirmatory molecular test is often needed due to similar clinical manifestations with other conditions causing 46,XY DSD. Since in our country, the molecular test for the AR gene is lacking, the study is conducted as a preliminary study to elaborate on the possibility of developing a molecular test for the AR gene in 46,XY DSD cases. Methods: Archived DNAs of 13 46,XY DSD cases were analyzed using polymerase chain reaction and direct sequencing for molecular defects in the AR gene. Clinical and hormonal data were collected and analyzed. Results: The study successfully amplified and visualized the eight exons of the AR gene and revealed two subjects carrying AR gene variants at exon 7. In the first case, 1.2-year-old boy carried heterozygous p.Gln825Arg, which has never been reported elsewhere, and the second subject, a 2.1-year-old girl with heterozygous p.Arg841His. Both subjects presented with severe undervirilization of external genitalia with external genitalia masculinization scores (EMS) of 1.5 and 3. Conclusion: In this series, two of 13 46,XY DSD cases carried variants at the AR gene, resulting in complete androgen insensitivity syndrome.

Published

2024

10. Androgen insensitivity syndrome: preventive gonadectomy, pros and cons

Author

E. A. Starostina, N. V. Frolkova, S. M. Seidova, E. G. Przhiyalkovskaya, N. M. Platonova, and E. A. Troshina

Subjects

androgen insensitivity syndrome, testicular feminization, androgen receptor, sex development disorders, Physiology, QP1-981, Biochemistry, QD415-436

Abstract

Androgen insensitivity syndrome is a genetic disorder characterized by complete or partial androgen insensitivity in individuals with a 46XY genotype. It is also the most common cause of disorders of sexual differentiation in patients with a 46XY karyotype. This condition is caused by a defect in the androgen receptor gene (AR), leading to abnormal development of male genitalia, impaired formation of male secondary sexual characteristics, and phenotypic features resembling the female sex.One of the important aspects related to the management of androgen insensitivity syndrome is the necessity of preventive gonadectomy. However, the rationale for prophylactic removal of gonads remains a subject of debate. This article presents a clinical case of a 37-year-old woman with complete androgen insensitivity syndrome who, despite recommendations for gonadectomy based on suspicious MRI characteristics of the gonads, made the decision to decline surgical intervention, justifying her choice by the positive impact of gonadal hormonal activity on her external appearance and physical characteristics. This clinical case highlights the complexity of decision-making in the management of androgen insensitivity syndrome, where patient preferences and needs may play a significant role, despite potential risks and concerns surrounding the preservation of gonads.

Published

2024

11. Detection of Molecular Variations at Androgen Receptor Gene in 46,XY Differences in Sex Development Cases.

Author

Marzuki, Nanis S., Kartapradja, Hannie D., Coutrier, Farah N., Wahyudi, Irfan, and Batubara, Jose R. L.

Subjects

ANDROGEN-insensitivity syndrome, ANDROGEN receptors, GENETIC variation, POLYMERASE chain reaction, GENITALIA

Abstract

Introduction: One of the common causes of 46,XY differences in sex development (DSD) cases is androgen insensitivity syndrome. This X-linked recessive inherited condition is associated with pathological variations of the AR gene, leading to defects in androgen action. Affected 46,XY infants or individuals experience variable degrees of undervirilization and those with severe form will have female-like external genitalia. Therefore, they were more likely assigned and reared as females. The confirmatory molecular test is often needed due to similar clinical manifestations with other conditions causing 46,XY DSD. Since in our country, the molecular test for the AR gene is lacking, the study is conducted as a preliminary study to elaborate on the possibility of developing a molecular test for the AR gene in 46,XY DSD cases. Methods: Archived DNAs of 13 46,XY DSD cases were analyzed using polymerase chain reaction and direct sequencing for molecular defects in the AR gene. Clinical and hormonal data were collected and analyzed. Results: The study successfully amplified and visualized the eight exons of the AR gene and revealed two subjects carrying AR gene variants at exon 7. In the first case, 1.2-year-old boy carried heterozygous p.Gln825Arg, which has never been reported elsewhere, and the second subject, a 2.1-year-old girl with heterozygous p.Arg841His. Both subjects presented with severe undervirilization of external genitalia with external genitalia masculinization scores (EMS) of 1.5 and 3. Conclusion: In this series, two of 13 46,XY DSD cases carried variants at the AR gene, resulting in complete androgen insensitivity syndrome. [ABSTRACT FROM AUTHOR]

Published

2024

12. Corrigendum: Androgen insensitivity syndrome: preventive gonadectomy, 'pros' and 'cons' (Obesity and metabolism. 2024;21(1):85-91. doi: https://doi.org/10.14341/omet13024)

Author

E. A. Starostina, N. V. Frolkova, S. M. Seidova, E. G. Przhiyalkovskaya, N. M. Platonova, and E. A. Troshina

Subjects

androgen insensitivity syndrome, testicular feminization, androgen receptor, sex development disorders, Physiology, QP1-981, Biochemistry, QD415-436

Abstract

A corrigendum on "Androgen insensitivity syndrome: preventive gonadectomy, "pros" and "cons"" (Obesity and metabolism by Еvgenia A. Starostina, Nadezhda V. Frolkova, Seidbike M. Seidova, Elena G. Przhiyalkovskaya, Nadezhda M. Platonova (2024). Obesity and metabolism. 2024;21(1):85-91. doi: https://doi.org/10.14341/omet13024On page 87 the sentence “In addition, testosterone preparations are used to treat infertility in patients with a mild form of STF [3]” was removed. Added paragraph “Birnbaum W et al. conducted a multicenter, double-blind, randomized, crossover study in three university medical centers and three specialized hospitals in Germany. In this study, patients aged 18-54 years with karyotype 46,XY, genetically confirmed CAIS, removed gonads, were treated with either estradiol drugs at a dose of 1.5 mg/day for 6 months, followed by a transition to testosterone 50 mg /day for 6 months (sequence A), or testosterone preparations 50 mg/day for 6 months, followed by a transition to estradiol 1.5 mg/day for 6 months (sequence B).In the study, testosterone was well tolerated and as safe as estrogen. The authors suggested that testosterone may be an ­alternative replacement therapy for CAIS, particularly for patients with reduced sexual function."A new source has been added in the reference list section under No. 30: “Birnbaum W, Marshall L, Werner R, et al. Oestrogen versus androgen in hormone-replacement therapy for complete androgen insensitivity syndrome: a multicentre, randomized, double-dummy, double-blind crossover trial. Lancet Diabetes Endocrinol. 2018;6(10):771-780. doi:10.1016/S2213-8587(18)30197-9.”The authors regret the error. The original version of the article has been replaced.

Published

2024

13. Clinical outcomes and genotype-phenotype correlations in patients with complete and partial androgen insensitivity syndromes

Author

Nae-yun Lee, Ja Hye Kim, Ji-Hee Yoon, Soojin Hwang, Gu-Hwan Kim, Han-Wook Yoo, and Jin-Ho Choi

Subjects

androgen insensitivity syndrome, ar, disorders of sex development, Pediatrics, RJ1-570

Abstract

Purpose Androgen insensitivity syndrome (AIS) is a rare X-linked recessive disorder caused by unresponsiveness to androgens because of mutations in the AR gene. Here, we investigated the clinical outcomes and molecular spectrum of AR variants in patients with AIS attending a single academic center. Methods This study included 19 patients with AIS who were confirmed by molecular analysis of AR. Clinical features and endocrinological findings were retrospectively collected, including presenting features, external genitalia, sex of rearing, timing of gonadectomy, pubertal outcomes, and sex hormone levels. Molecular analysis of AR was performed using Sanger, targeted gene panel, or whole-exome sequencing. Results Among all 19 patients, 14 (74%) were classified as having complete AIS (CAIS), whereas 5 (26%) had partial AIS (PAIS). All patients with CAIS, and 3 patients with PAIS were reared as female. One patient with CAIS manifested a mixed germ cell tumor at the age of 30 years. Molecular analysis of AR identified 19 sequence variants; 12 (63%) were previously reported, and the remaining 7 (37%) were novel. Missense mutations were the most common type (12 of 19, 63%), followed by small deletions, nonsense mutations, an insertion, and a splice site mutation. Conclusions Here, we describe the clinical outcomes and molecular characteristics of 19 Korean patients with AIS. Patients with PAIS manifested various degrees of masculinization of the external genitalia. Nonsense and frameshift mutations were frequent in patients with CAIS, whereas patients with PAIS harbored exclusively missense mutations.

Published

2023

14. Sex assignment and psychosexual peculiarities of individuals with different forms of androgen insensitivity syndrome: A qualitative study.

Author

Kristesashvili, Jenaro, Kobaladze, Levan, Chipashvili, Mariam, and Jibladze, Anna

Subjects

*ANDROGEN-insensitivity syndrome, *ANDROGEN receptors, *SEX (Biology), *GONADAL dysgenesis, *PRECOCIOUS puberty, *MALE reproductive organs, *SEX chromosomes

Abstract

Background: A mismatch between chromosomal, gonadal, and phenotypic sexes in individuals with androgen insensitivity syndrome (AIS) creates problems in sex assignment and psychosexual identification. Objective: To identify psychosexual and sex assignment peculiarities of individuals with different forms of AIS. Materials and Methods: In this qualitative study, 41 individuals with AIS aged between 15 and 31 yr who referred to the Universe Center for Reproductive Medicine Tbilisi, Georgia between 2016 and 2021 were studied. All individuals underwent clinical, genealogical, hormonal, ultrasonographic, and cytogenetic examinations. In-depth interviews and medical records assessed psychosexual profiles and sex assignment histories. Results: 32 cases were diagnosed with the complete form of AIS (CAIS), 8 individuals with the partial form (PAIS), and one with a mild form (MAIS). Individuals with CAIS and PAIS were assessed at birth and raised as girls. Individuals with CAIS and female psychosexual disposition were referred to us due to amenorrhea. Adolescent individuals with PAIS assessed as girls referred to us due to masculinization detected in puberty. An individual with MAIS was assessed at birth and raised as a boy with male genitalia. All individuals with AIS had typical hormonal data and sex chromosome complex for men. 20 sexually active individuals with CAIS had penile-vaginal contact with the man. None of the individuals with CAIS and PAIS thought about gender reassignment after being diagnosed, only the individual with MAIS aimed for male-to-female transition. Conclusion: Psychosexual identification remains a significant challenge in AIS management. Detection of female psychosexual disposition in one participant that is unusual to MAIS may be associated with somatic mosaicism of the androgen receptor gene. [ABSTRACT FROM AUTHOR]

Published

2023

15. Urethral reconstruction using amniotic membrane allograft in hereditary androgen insensitivity syndrome: a case series.

Author

Mansour, Marah, Raya, Maria, Jrdy, Abd Alrahman, Sires, Abdoul Majid, Wardeh, Jad Alhaq, Alsbekhan, Almoataz Ballah, Faour, Sabah, Kanas, Mahmoud, Safadi, Mhd Firas, and Alrebdawi, Khaled

Subjects

*ANDROGEN-insensitivity syndrome, *AMNION, *PLASTIC surgery, *HOMOGRAFTS, *SURGICAL complications

Abstract

Partial androgen insensitivity syndrome is a rare X-linked disorder. While most cases are sporadic, familial cases are less frequent. The management of this syndrome follows a multidisciplinary approach involving hormone substitution, psychological counseling, and surgical procedures. We present a case series of three young siblings with familial partial androgen insensitivity syndrome who presented with a female phenotype. All of them were managed with hormonal treatment for 6 months followed by surgical reconstruction. The operative procedure involved phalloplasty and urethroplasty using amniotic membrane transplant, which is considered a novel technique in this group of patients. No intraoperative or postoperative complications were observed and good results were achieved within 2 years of follow-up. [ABSTRACT FROM AUTHOR]

Published

2023

16. Clinical Case of the Complete Form of Androgen Insensitivity Syndrome (AIS)

Author

M. M. Damirov, I. V. Anchabadze, A. A. Medvedev, and M. A. Eremenko

Subjects

androgen insensitivity syndrome, testicular feminization syndrome, morris syndrome, disorder of sex development, gonadectomy, hormone replacement therapy, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

The article presents a clinical observation of an extremely rare in gynecological practice androgen insensitivity syndrome (AIS). The authors give data on the pathogenesis of the disease, modern classification and terminology of various forms of this pathology. The phenotypic manifestations of the disease, the results of clinical and instrumental studies and surgical treatment are described.The results of the study show the possibility of clinical diagnosis of AIS and timely surgical treatment of patients with this pathology, due to the high risk of gonadal malignancy.

Published

2023

17. A Very Early Diagnosis of Complete Androgen Insensitivity Syndrome Due to a Novel Variant in the AR Gene: A Neonatal Case Study

Author

Rossella Ferrante, Stefano Tumini, Maria Alessandra Saltarelli, Sara Di Rado, Vincenzo Scorrano, Maria Lucia Tommolini, Mirco Zucchelli, Federico Lauriola, Gabriele Lisi, Giuseppe Lauriti, Nino Marino, Liborio Stuppia, Claudia Rossi, and Ines Bucci

Subjects

disorders of sexual development, steroid profiling, next-generation sequencing, androgen receptor, androgen insensitivity syndrome, Biology (General), QH301-705.5

Abstract

Androgen insensitivity syndrome (AIS) is one of the most common Disorders of Sexual Differentiation (DSDs). AIS is characterized by an X-linked recessive inheritance pattern associated with variants in the androgen receptor (AR) gene that affects the masculinization process in individuals with XY karyotype. Here, we report a neonatal case of a very early diagnosis of complete AIS due to a novel variant in the AR gene. In the present case, after the clinical evaluation, the infant has undergone the following tests: biochemical analyses, including newborn screening workflow, karyotype analysis, and Next-Generation Sequencing (NGS) panel of 50 genes involved in DSDs. The NGS analysis identified a missense variant, c.2108C>A, in the AR gene. According to a cytogenetic analysis, the patient presented a 46, XY karyotype, thus the resulting hemizygote for the AR gene variant. The variant is not currently described in the literature nor in the ClinVar database. However, according to computational models, the variant could have a pathogenetic effect. This clinical case reveals a novel variant of the AR gene with a possible pathogenetic effect associated with AIS and highlights the importance of a multidisciplinary approach for the timely diagnosis and appropriate follow-up of the patient.

Published

2024

18. A prime editor efficiently repaired human induced pluripotent stem cells with AR gene mutation (c.2710G > A; p. V904M)

Author

Ruiqi Sun, Yiqiang Cui, Zhaode Liu, Jiayin Guo, Xin Zhang, Pinmou Zhu, Jiahao Sha, Xiaoyu Yang, and Yan Yuan

Subjects

Induced pluripotent stem cell, Gene editing, Androgen insensitivity syndrome, Prime editors, CRISPR-Cas9, Biology (General), QH301-705.5

Abstract

Prime Editor (PE) is a precise genome manipulation technology based on the CRISPR-Cas9 system, while its application in human induced pluripotent stem cells (iPSCs) remains limited. Here, we established a repaired hiPS cell line (SKLRMi001-A-1) from hiPSCs with androgen receptor (AR) mutation (c.2710G > A; p.V904M). The repaired iPSC line expressed pluripotency markers, retained normal karyotype, showed the capability of differentiating into three germ layers and was absence of mycoplasma infection. The repaired iPSC line will help to elucidate the mechanism of androgen insensitivity syndrome (AIS) and benefit treatment for AIS in the future.

Published

2023

19. Study of novel androgen receptor V770 variant in androgen insensitivity syndrome patients reveals the transitional state of the androgen receptor ligand binding domain homodimer.

Author

Helsen, Christine, Rocca, Maria Santa, Nguyen, Tien T., Eerlings, Roy, Lee, Xiao Yin, De Block, Sofie, Vinanzi, Cinzia, Di Millo, Francesco, Giagulli, Vito, Voet, Arnout, Ferlin, Alberto, and Claessens, Frank

Abstract

We report the discovery of the androgen receptor missense mutation V770D, that was found in two sisters suffering from complete androgen insensitivity. Experimental validation of AR V770 variants demonstrated that AR V770D was transcriptionally inactive due to the inability to dimerize and a reduced ligand binding affinity. The more conservative AR V770A variant showed a dimerization defect at low levels of DHT with a partial recovery of the transcriptional activity and of the receptor's ability to dimerize when increasing the DHT levels. With V770 located outside of the proposed LBD dimerization interface of the AR LBD homodimer crystal structure, the effects of the V770A mutation on AR dimerization were unexpected. We therefore explored whether the AR LBD dimerization interface would be better described by an alternative dimerization mode based on available human homodimeric LBD crystal structures of other nuclear receptors. Superposition of the monomeric AR LBD in the homodimeric crystal structures of GR, PR, ER, CAR, TRβ, and HNF‐4α showed that the GR‐like LBD dimer model was energetically the most stable. Moreover, V770 was a key energy residue in the GR‐like LBD dimer while it was not involved in the stabilization of the AR LBD homodimer according to the crystal structure. Additionally, the observation that 4 AIS mutations impacted the stability of the AR LBD dimer while 16 mutations affected the GR‐like LBD dimer, suggested that the AR LBD dimer crystal is a snapshot of a breathing AR LBD homodimer that can transition into the GR‐like LBD dimer model. [ABSTRACT FROM AUTHOR]

Published

2023

20. 'Distraction Vaginogenesis': Preliminary Results Using a Novel Method for Vaginal Canal Expansion in Rats.

Author

Meyer, Hannah, Trosclair, Lexus, Clayton, Sean D., O'Quin, Collyn, Connelly, Zachary, Rieger, Ross, Dao, Nhi, Alhaque, Ahmed, Minagar, Andrew, White, Luke A., Solitro, Giovanni, Shah-Bruce, Mila, Welch, Valerie L., Villalba, Stephanie, Alexander, Jonathan Steven, and Sorrells, Donald

Subjects

*SPRAGUE Dawley rats, *RATS, *PLASTIC surgery, *TISSUE fixation (Histology), *POLYETHYLENE terephthalate, *ANDROGEN-insensitivity syndrome

Abstract

Vaginal atresia is seen in genetic disorders such as Mayer–Rokitansky–Küster–Hauser (MRKH) syndrome, which can cause significant sexual dysfunction. Current treatments include surgical reconstruction or mechanical dilation of the vaginal canal. Mechanical dilation requires patients to be highly motivated and compliant while surgical reconstruction has high rates of complications. This study evaluated a novel vaginal expansion sleeve (VES) method as an alternative treatment for vaginal atresia. The proprietary cylindrical VES is a spring-like device consisting of polyethylene terephthalate helicoid trusses capped at each end with a fixed diameter resin cap for fixation within tissues. Following the development of the VES and mechanical characterization of the force–length relationships within the device, we deployed the VES in Sprague Dawley rat vaginas anchored with nonabsorbable sutures. We measured the VES length–tension relationships and post-implant vaginal canal expansion ex vivo. Vaginal histology was examined before and after implantation of the VES devices. Testing of 30 mm sleeves without caps resulted in an expansion force of 11.7 ± 3.4 N and 2.0 ± 0.1 N at 50% and 40%, respectively. The implanted 20 mm VES resulted in 5.36 mm ± 1.18 expansion of the vaginal canal, a 32.5 ± 23.6% increase (p = 0.004, Student t test). Histological evaluation of the VES implanted tissue showed a significant thinning of the vaginal wall when the VES was implanted. The novel VES device resulted in a significant expansion of the vaginal canal ex vivo. The VES device represents a unique alternative to traditional mechanical dilation therapy in the treatment of vaginal atresia and represents a useful platform for the mechanical distension of hollow compartments, which avoids reconstructive surgeries and progressive dilator approaches. [ABSTRACT FROM AUTHOR]

Published

2023

21. Mutations in AR or SRD5A2 Genes: Clinical Findings, Endocrine Pitfalls, and Genetic Features of Children with 46,XY DSD

Author

Neşe Akcan, Oya Uyguner, Firdevs Baş, Umut Altunoğlu, Güven Toksoy, Birsen Karaman, Şahin Avcı, Zehra Yavaş Abalı, Şükran Poyrazoğlu, Agharza Aghayev, Volkan Karaman, Rüveyde Bundak, Seher Başaran, and Feyza Darendeliler

Subjects

46, xy disorders of sex development, 5α, -reductase deficiency, androgen insensitivity syndrome, androgen receptor gene mutations, srd5a2 gene mutations, Pediatrics, RJ1-570, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

INTRODUCTION: Objective: Androgen insensivity syndrome (AIS) and 5α-reductase deficiency (5α-RD) present with indistinguishable phenotypes among the 46,XY disorders of sexual development (DSD) that usually necessitate molecular analyses for the definitive diagnosis in the prepubertal period. The aim was to evaluate the clinical, hormonal and genetic findings of 46,XY DSD patients who were diagnosed as AIS or 5α-RD. METHODS: Methods: Patients diagnosed as AIS or 5α-RD according to clinical and hormonal evaluations were investigated. Sequence variants of steroid 5-α-reductase type 2 were analyzed in cases with testosterone/dihydrotestosterone (T/DHT) ratio of ≥20, whereas the androgen receptor (AR) gene was screened when the ratio was T, p.Glu32*, c.330G>C, p.Leu110=; c.2084C>T, p.Pro695Leu, c.2585_2592delAGCTCCTG, p.(Lys862Argfs*16), of these c.330G>C with silent status remained undefined in terms of its causative effects. DISCUSSION AND CONCLUSION: Conclusion: T/DHT ratio is an important hormonal criterion, but in some cases, T/DHT ratio may lead to diagnostic confusion. Molecular diagnosis is important for the robust diagnosis of 46,XY DSD patients. Four novel AR variants were identified in our study.

Published

2022

22. Clinicopathological Study of Testicular Lesions in a Tertiary Care Centre of Dakshina Kannada, India.

Author

ATHIRA, K. P., UMASHANKAR, T., and KUMAR, MOHIT

Abstract

Introduction: Testicular biopsies are performed for both diagnostic and therapeutic purposes. Diagnostic testicular biopsies are usually performed as a part of a male infertility work-up. Therapeutic testicular excision biopsies are performed for a wide range of disorders, including neoplastic lesions, inflammatory lesions, cryptorchidism, testicular trauma, and as a part of prophylactic treatment of carcinoma prostate. Aim: To evaluate the indications for orchidectomy and diagnostic testicular biopsies and to understand the histopathological spectrum of testicular lesions and concordance with clinical diagnosis. Materials and Methods: This was a retrospective study conducted in the Department of Pathology, Father Muller Medical College, Mangalore, Karnataka, India. The study period is from July 2017 to June 2020. Data was collected and analysed in August 2020. All testis' biopsies, including excision and diagnostic biopsies, are included in the study. Histopathological findings and the clinical diagnosis were evaluated for concordance. Data were tabulated and statistically evaluated for age distribution, laterality, and frequency using Microsoft Excel 2021. Percentages for the variables and concordance rate were calculated. Results: A total of 139 cases (mean age 54.5 years) were included in the study. Prophylactic orchidectomy for carcinoma prostate (64/139=46.04%) was the most common clinical indication. Non neoplastic lesions account for 48.20% (67/139). Frequent non neoplastic lesions are testicular torsion (23/139=16.55%) and abscess (12/139=8.63%), followed by cryptorchidism (9/139=6.47%). Left-sided lesions are more frequent than right-sided lesions. Histopathology confirmed two cases of suspected male infertility and Androgen Insensitivity Syndrome (AIS). Neoplastic lesion accounts to 6.47% (9/139). Frequent neoplasm in the study was seminoma (3/139=2.16%), followed by lymphoma (2/139=1.44%). Other neoplasms included in the study were mixed germ cell tumours, post-pubertal teratoma, and spermatocytic tumour. Testicular tuberculosis accounts to 1.44% (2/139) in the present population. Conclusion: Non neoplastic lesions were common compared to testicular neoplasms. Testicular torsion, followed by abscess, was the most common indication for orchidectomy. Testicular Tuberculosis can mimic a neoplasm on clinical and radiological work-up. Hence, careful evaluation has to be performed in young suspected cases of tuberculosis. [ABSTRACT FROM AUTHOR]

Published

2023

23. A Gly684Ala substitution in the androgen receptor is the cause for azoospermia in a Chinese family with mild androgen insensitivity syndrome and normal hormone levels.

Author

Yuan Yuan, Wen-Qing Xu, Ying Chen, Tao Luo, and Hou-Yang Chen

Subjects

ANDROGEN-insensitivity syndrome, AZOOSPERMIA, MALE infertility, GENETIC models, MISSENSE mutation, ANDROGEN receptors

Abstract

Androgen receptor gene (AR) is essential for male growth and fertility. Its mutations are responsible for androgen insensitivity syndrome (AIS) that usually shows the phenotype of azoospermia resulting in male infertility. This study reported the first case of mild AIS with complete normal serum hormones in a Chinese family. The proband referred for infertility because of azoospermia. His uncle and two cousins are both infertile and have azoospermia. Wholeexome sequencing in the genetic analyses showed that the proband carries a novel hemizygous AR missense mutation, NM_000044.6: c.2051G>C (p.Gly684Ala), in exon four within the ligand-binding domain. His mother and maternal aunt are heterozygous carriers, while his father and brother are wildtype, indicating that the mutation in the proband was inherited from his mother. This pattern is consistent with the genetic model of the X-linked recessive inheritance of AR in AIS pathogenesis. HOPE predicts that p.Gly684Ala increases the hydrophobicity of AR but does not change the AR conformation. PolyPhen-2 predicts that p.Gly684Ala is harmful. This study provides the new knowledge to understand the AR gene mutations in MAIS. [ABSTRACT FROM AUTHOR]

Published

2022

24. Studies from Concord Hospital in the Area of Androgen Insensitivity Syndrome Described (Molecular mechanism of androgen receptor mutation in multigenerational mild androgen insensitivity syndrome).

Abstract

A recent study conducted at Concord Hospital focused on the molecular mechanism of androgen receptor mutation in multigenerational mild androgen insensitivity syndrome (MAIS). The research aimed to understand the clinical features and responses to high dose testosterone treatment in three cases of MAIS across a six-generation family pedigree. The study identified a missense AR exon 8 mutation that weakens the closure energy of the ligand binding pocket, allowing for easier ligand dissociation, but with unimpaired in vitro androgen bioactivity. The findings suggest that the novel molecular mechanism of this mutation in MAIS may be present in other cases of the syndrome. [Extracted from the article]

Published

2024

25. Mutations in AR or SRD5A2 Genes: Clinical Findings, Endocrine Pitfalls, and Genetic Features of Children with 46,XY DSD.

Author

Akcan, Neşe, Uyguner, Oya, Baş, Firdevs, Altunoğlu, Umut, Toksoy, Güven, Karaman, Birsen, Avcı, Şahin, Abalı, Zehra Yavaş, Poyrazoğlu, Şükran, Aghayev, Agharza, Karaman, Volkan, Bundak, Rüveyde, Başaran, Seher, and Darendeliler, Feyza

Subjects

GENETIC mutation, SEQUENCE analysis, ENDOCRINE diseases, SEX differentiation disorders, DISEASES in men, GENETIC testing, MOLECULAR pathology, RISK assessment, COMPARATIVE studies, DESCRIPTIVE statistics, OXIDOREDUCTASES, ANDROGEN-insensitivity syndrome, PHENOTYPES, DISEASE risk factors, DISEASE complications

Abstract

Objective: Androgen insensivity syndrome (AIS) and 5α-reductase deficiency (5α-RD) present with indistinguishable phenotypes among the 46,XY disorders of sexual development (DSD) that usually necessitate molecular analyses for the definitive diagnosis in the prepubertal period. The aim was to evaluate the clinical, hormonal and genetic findings of 46,XY DSD patients who were diagnosed as AIS or 5α-RD. Methods: Patients diagnosed as AIS or 5α-RD according to clinical and hormonal evaluations were investigated. Sequence variants of steroid 5-α-reductase type 2 were analyzed in cases with testosterone/dihydrotestosterone (T/DHT) ratio of ≥20, whereas the androgen receptor (AR) gene was screened when the ratio was <20. Stepwise analysis of other associated genes were screened in cases with no causative variant found in initial analysis. For statistical comparisons, the group was divided into three main groups and subgroups according to their genetic diagnosis and T/DHT ratios. Results: A total of 128 DSD patients from 125 non-related families were enrolled. Birth weight SDS and gestational weeks were significantly higher in 5α-RD group than in AIS and undiagnosed groups. Completely female phenotype was higher in all subgroups of both AIS and 5α-RD patients than in the undiagnosed subgroups. In those patients with stimulated T/DHT <20 in the prepubertal period, stimulated T/DHT ratio was significantly lower in AIS than in the undiagnosed group, and higher in 5α-RD. Phenotype associated variants were detected in 24% (n=18 AIS, n=14 5α-RD) of the patients, revealing four novel AR variants (c.94G>T, p.Glu32*, c.330G>C, p.Leu110=; c.2084C>T, p.Pro695Leu, c.2585_2592delAGCTCCTG, p.(Lys862Argfs*16), of these c.330G>C with silent status remained undefined in terms of its causative effects. Conclusion: T/DHT ratio is an important hormonal criterion, but in some cases, T/DHT ratio may lead to diagnostic confusion. Molecular diagnosis is important for the robust diagnosis of 46,XY DSD patients. Four novel AR variants were identified in our study. [ABSTRACT FROM AUTHOR]

Published

2022

26. Complete androgen insensitivity syndrome in a 13-year-old Lebanese child, reared as female, with bilateral inguinal hernia: a case report

Author

Stephanie Farah, Dana El Masri, and Kamal Hirbli

Subjects

Androgen insensitivity syndrome, Amenorrhea, Inguinal hernia, Case report, Medicine

Abstract

Abstract Background Androgen insensitivity syndrome is a rare X-linked disorder of sex development, caused by mutations in the androgen receptor. In this case, a 13-year-old child, reared as female, presenting for primary amenorrhea, was diagnosed with complete androgen insensitivity syndrome. Case presentation A 13-year-old Caucasian child, reared as female, presents with primary amenorrhea. Physical examination revealed female appearance and a short vagina with blind-ended pouch. Laboratory examination showed high levels of testosterone and anti-Müllerian hormone; uterus and ovaries were absent. Karyotype confirmed a 46,XY pattern. Deoxyribonucleic acid analysis of the androgen receptor gene revealed a homozygous mutation p.R856C in exon 7. Gender was assigned as female, and she was started on hormonal therapy and underwent gonadectomy. Conclusion Androgen insensitivity syndrome comprises a large spectrum of presentations. High index of suspicion is needed. Investigation of girls with bilateral inguinal hernia is critical.

Published

2021

27. Complete androgen insensitivity syndrome and risk of gonadal malignancy: systematic review

Author

Beatriz Amstalden Barros, Letícia Ribeiro de Oliveira, Cíntia Regina Crocetti Surur, Antonio de Azevedo Barros-Filho, Andrea Trevas Maciel-Guerra, and Gil Guerra-Junior

Subjects

androgen insensitivity syndrome, gonadectomy, neoplasia, puberty, Pediatrics, RJ1-570

Abstract

Complete androgen insensitivity syndrome (CAIS) is a rare condition characterized by 46,XY karyotype, female external genitalia, absence of uterus, and testes located intra-abdominally, in the inguinal ring or in the labia majora. In the present study, the frequency of testicular malignancy in prepubertal and pubertal patients with CAIS who underwent gonadectomy or gonadal biopsy were evaluated. Systematic review was performed using electronic databases according to the PRISMA-P (Preferred Reporting Items for Systematic Review and Meta-Analysis Protocols) guidelines. The samples included 15 articles published between 1998 and 2019. From a total of 456 patients who underwent gonadectomy or gonadal biopsy, 6.14% had a premalignant lesion and most were postpubertal (82.14%). A malignant lesion was found in 1.3% and all were postpubertal. Because the risk of malignancy is very low in prepubertal patients with CAIS, gonadectomy may be delayed until puberty is complete, allowing it to progress naturally; however, close follow-up of the patient is required.

Published

2021

28. Complete Androgen Insensitivity Syndrome: A Rare Case of Prenatal Diagnosis

Author

Maria Liz Coelho, Elisa Soares, Marília Freixo, Pedro Brandão, Carla Marinho, Juliana Rocha, and Graça Rodrigues

Subjects

prenatal diagnosis, prenatal genetic counseling, androgen insensitivity syndrome, disorder of sex development, 46, XY, androgen receptor, Gynecology and obstetrics, RG1-991

Abstract

Abstract With the widespread uptake of noninvasive prenatal testing (NIPT), a larger cohort of women has access to fetal chromosomal sex, which increases the potential to identify prenatal sex discordance. The prenatal diagnosis of androgen insensitivity syndrome (AIS) is an incidental and rare finding. We wish to present the diagnosis of a prenatal index case after NIPT of cell-free fetal DNA and mismatch between fetal sex and ultrasound phenotype. In this particular case, the molecular analysis of the androgen receptor (AR) gene showed the presence of a pathogenic mutation, not previously reported, consistent with complete androgen insensitivity syndrome. Carrier testing for the mother revealed the presence of the same variant, confirming maternal hemizygous inheritance. Identification of the molecular basis of these genetic conditions enables the preimplantation or prenatal diagnosis in future pregnancies.

Published

2021

29. Analysis of the androgen receptor (AR) gene in a cohort of Indonesian undermasculinized 46, XY DSD patients

Author

Nurin Aisyiyah Listyasari, Achmad Zulfa Juniarto, Gorjana Robevska, Katie L. Ayers, Andrew H. Sinclair, and Sultana M. H. Faradz

Subjects

Androgen receptor, Androgen insensitivity syndrome, Disorders of sex development (DSD), Molecular genetics, Sanger sequencing, Undermasculinization, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Background Pathogenic variants in the androgen receptor (AR) gene located on chromosome Xq11-12, are known to cause varying degrees of undermasculinization in 46, XY individuals. The aim of this study was to investigate the frequency of pathogenic variants in the AR gene in a cohort of 46, XY undermasculinized individuals from Indonesia who were suspected of having androgen insensitivity syndrome (AIS). All patients with 46, XY DSD referred to our center between 1994 and 2019 were collected from our clinical database. All 46, XY DSD patients without a prior molecular diagnosis with an external masculinization score (EMS) ≤ 9 were included in this study. All exons and intron–exon boundaries of AR gene were analyzed using Sanger sequencing to identify pathogenic variants of the AR gene. Results A cohort of 75 undermasculinized patients were selected for the study. Direct Sanger sequencing of all eight exons of the AR gene led to a genetic diagnosis in 11 patients (14.67%). All of the variants identified (p.Arg841His; p.Ile604Asn; p.Val731Met; p.Pro672Ser; p.Gln739Arg; p.Ser302Glufs*3) have been previously reported in patients with AIS. Conclusions This is the first study in Indonesia that highlights the significance of molecular analysis in providing a definitive diagnosis of AIS for patients with 46, XY DSD undermasculinization. This is an uncommon finding in the Indonesian population presenting with 46, XY DSD undermasculinization. A genetic diagnosis allows optimal clinical management and genetic counseling for patients and their families. As 46, XY DSD can be caused by pathogenic variants in other genes involved in gonadal development and differentiation, further genetic analysis, such as whole exome sequencing, should be carried out on those patients that did not carry an AR variant.

Published

2021

30. Genetic Analysis Reveals Complete Androgen Insensitivity Syndrome in Female Children Surgically Treated for Inguinal Hernia

Author

Nurin A. Listyasari, Gorjana Robevska, Ardy Santosa, Aurore Bouty, AZ Juniarto, Jocelyn van den Bergen, Katie L. Ayers, Andrew H. Sinclair, and Sultana MH Faradz

Subjects

androgen insensitivity syndrome, inguinal hernia, hernia repair, genetic testing, Surgery, RD1-811

Abstract

Background: Complete androgen insensitivity syndrome (CAIS) is a congenital condition caused by genetic defects in the androgen receptor (AR) gene located on the X chromosome, which lead to a phenotypical female individual with a 46, XY karyotype. Early diagnosis of CAIS is essential for proper clinical management, allows assessment of familial risk and contributes to healthcare decisions. However, diagnosis of CAIS can be overlooked in girls with inguinal hernia, resulting in inappropriate management. Methods: Five female patients from three unrelated families presented to our genetic clinic with primary amenorrhea. Each patient had been diagnosed with inguinal hernia in childhood and had undergone hernia repair without further investigation into what was contained in the hernial sac. We carried out physical examination, cytogenetic studies, hormonal evaluation, and molecular analysis to establish a comprehensive diagnosis. Family history and pedigree were collated to identify at-risk family members. Results: All patients presented with female external genitalia. Cytogenetic studies revealed a 46, XY karyotype and hormonal analysis suggested a diagnosis of CAIS. Sequencing of the AR gene in all patients and suspected family members revealed pathogenic variants in the AR gene and confirmed the molecular diagnosis of CAIS. Conclusions: We report the delayed diagnosis of CAIS in female Indonesian patients with a history of inguinal hernia in childhood. An early diagnosis of CAIS is essential for appropriate clinical management, as well as assessing familial risk. Increasing awareness among clinicians is paramount, and we encourage a CAIS diagnosis to be considered in any patient presenting with female appearance and inguinal hernia.

Published

2021

31. Clinical, etiological and laboratory profile of children with disorders of sexual development (dsd)-experience from a tertiary pediatric endocrine unit in western India

Author

Rahul Jahagirdar, Vaman Khadilkar, Ruma Deshpande, and Nikhil Lohiya

Subjects

androgen insensitivity syndrome, congenital adrenal hyperplasia, disorders of sex development, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Objectives: To present the clinical profile, diagnostic work-up, and management of children with Disorders of Sexual Development (DSD).Materials and Methods: A retrospective study from a tertiary pediatric endocrine unit of western India. We included 39 patients who presented over a period of 9 years from June 2009 to June 2018. Results: Nineteen patients (48.7%) were diagnosed with 46 XY DSD, 16 (41%) with 46 XX DSD, and 4 (10.3%) with sex chromosomal DSD. Out of 46 XY DSD, androgen insensitivity was observed in 8 (42.1%) patients, 5 alpha-reductase deficiency in 5 (26.3%), gonadal dysgenesis in 3 (15.8%), ovotesticular DSD in 2 (10.5%) and 17 beta-hydroxylase (17γ-HSD3) deficiency in 1 (5.3%). Congenital adrenal hyperplasia was the most common cause in 46 XX DSD observed in 11 (68.75%) out of 16 patients, ovotesticular DSD was seen in 4 (25%) patients and testicular DSD in 1 (6.25%) patient. In sex chromosomal DSD 3 (75%) patients had mixed gonadal dysgenesis and 1 (25%) had ovotesticular DSD out of a total of 4 patients. At presentation gender of rearing was assigned as male in 16 (41%) patients, female in 20 (51.3%) patients, and no gender was assigned in 3 (7.7%). The gender of rearing was changed after diagnosis in 6 (16.7%) children. Conclusion: CAH was the most common etiology of 46 XX DSD whereas androgen insensitivity among 46 XY DSD. Assigning the sex of rearing should not be hurried and should be done only after diagnosis and parental counseling. A multidisciplinary and systematic approach is required for children with DSD.

Published

2021

32. Novel missense mutation in ligand binding domain of AR gene identified in patient with androgen insensitivity syndrome from Ukraine

Author

Dmytro Sirokha, Olexandra Gorodna, Dmytro Lozhko, Ganna Livshyts, Nataliya Zelinska, and Liudmyla Livshits

Subjects

androgen insensitivity syndrome, androgen receptor, bioinformatics, ligand binding domain, pathogenic mutation, Medicine, Medicine (General), R5-920

Abstract

Abstract To improve diagnostic informativity of AR gene mutation analysis in patients with AIS, we recommend to include novel identified missense mutation c.2507T>G in the list of AIS‐causing mutations.

Published

2021

33. Growth Curves of Chinese Children with Androgen Insensitivity Syndrome: A Multicenter Registry Study.

Author

Zhao, Xiu, Su, Zhe, Chen, Shaoke, Wang, Xiumin, Yang, Yu, Chen, Linqi, Liang, Li, Liu, Geli, Wang, Yi, Song, Yanning, Fan, Lijun, Ren, Xiaoya, and Gong, Chunxiu

Subjects

*ANDROGEN-insensitivity syndrome, *CHINESE people, *GROWTH of children, *CHILD patients, *BODY mass index, *BIRTH weight

Abstract

Objective: To provide new information about androgen insensitivity syndrome (AIS), we studied growth patterns in Chinese children with AIS. Subjects: Data are from 118 untreated AIS patients who were admitted to eight pediatric endocrine centers from January 2010 to December 2019. Methods: In this retrospective cohort study, clinical data were collected from a multicenter database. We compared physical assessment data among AIS patients and standard growth charts for Chinese pediatric population. Results: 1. Children with AIS grew slightly less than the mean before 6 months of age, and then, height gradually increased before 12 years of age, from the median to +1 standard deviation (SD), according to the standard reference for Chinese pediatric population. After 12 years of age, height showed differently in profiles: The mean height in AIS patients gradually decreased from the mean to −1 SD, according to the standard for Chinese boys, and increased from the mean to +2 SD, according to the standard for Chinese girls. 2. The weights of children with AIS were greater than the mean standards of Chinese pediatric population from newborn to 11 years of age. From 12–16 years of age, the mean weight of children with AIS showed different profiles, from the mean to −1 SD, according to the standard for Chinese boys and from the mean to +1.5 SD, according to the standard for Chinese girls. 3. Weight standard deviation (WtSDS) and target height (THt) in northern Chinese AIS patients were significantly higher than those from the southern region (p = 0.035, 0.005, respectively). Age in northern Chinese AIS patients was significantly younger than those from the southern region (p = 0.034). No difference was found among birth weight (BW), birth length (BL), height standard deviation (HtSDS) and body mass index (BMI) in AIS patients from different regions (p > 0.05). 4. HtSDS and WtSDS in complete AIS (CAIS) patients were higher than those in partial AIS (PAIS) patients without significant difference (p > 0.05). Conclusions: Growth of children with AIS varied to different degrees. AIS patients seemed not to experience a puberty growth spurt. CAIS and PAIS patients show little difference in their growth. Regional differences have no effect on the height but influence the weight of AIS patients. [ABSTRACT FROM AUTHOR]

Published

2022

34. Androgens by immunoassay and mass spectrometry in children with 46,XY disorder of sex development

Author

Letícia Ribeiro Oliveira, Carlos Alberto Longui, Guilherme Guaragna-Filho, José Luiz Costa, Rafael Lanaro, David Antônio Silva, Maria Izabel Chiamolera, Maricilda Palandi de Mello, André Moreno Morcillo, Andrea Trevas Maciel-Guerra, and Gil Guerra-Junior

Subjects

testosterone, testicles, androstenedione, androgen insensitivity syndrome, 5α-reductase, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Objective: Steroid measurement is a challenge in pediatric endocrinology. Currently, liquid chromatography with tandem mass spectrometry (LC-MS/MS) is considered a gold standard for this purpose. The aim of this study was to co mpare both LC-MS/MS and immunoassay (IA) for androgens before and after human recom binant chorionic gonadotropin (rhCG) stimulus in children with 46,XY disorders o f sex development (DSD). Methods: Nineteen patients with 46,XY DSD were evaluated; all of them w ere prepubertal and non-gonadectomized. Testosterone, dihydrotestosterone (DHT), DHEA and androstenedione were measured by IA and LC-MS/MS before and 7 d ays after rhCG injection. The correlation between IA and LC-MS/MS was analyzed by the intraclass correlation coefficient (ICC) and Spearman’s rank correlation coe fficient (SCC). For concordance analysis the Passing and Bablok (PB) regression and the Bland and Altman (BA) method were used. Results: Testosterone showed excellent correlation (ICC = 0.960 and SCC = 0.964); DHT showed insignificant and moderate correlations as indicated by I CC (0.222) and SCC (0.631), respectively; DHEA showed moderate correlation (ICC = 0.585 and SCC = 0.716); and androstenedione had poor and moderate correlations in ICC ( 0.363) and SCC (0.735), respectively. Using the PB method, all hormones showed a linear correlation, but proportional and systematic concordance errors were detected fo r androstenedione, systematic errors for testosterone and no errors for DHEA and D HT. By the BA method, there was a trend of IA to overestimate testosterone and andros tenedione and underestimate DHEA and DHT when compared to LC-MS/MS. Conclusion: Traditional IA should be replaced by LC-MS/MS for the androgen s measurement in prepubertal children whenever is possible.

Published

2020

35. Male pseudohermaphroditism: A case study of 46,XY disorder of sexual development using whole‐exome sequencing

Author

Oxana Yu. Naumova, Sergey Yu. Rychkov, Olga V. Burenkova, Maria Yu. Solodunova, Irina V. Polyanskaya, Irina A. Arintcina, Marina A. Zhukova, Irina V. Ovchinnikova, Olga V. Zhukova, and Elena L. Grigorenko

Subjects

46, XY disorder of sexual development, androgen insensitivity syndrome, disease‐related variant, whole‐exome sequencing, Medicine, Medicine (General), R5-920

Abstract

Abstract The study shows that whole‐exome sequencing is a promising approach to detect novel variants—and gene candidates in DSD, that, as a future direction, may improve the diagnostic gene panels for this heterogeneous disorder.

Published

2020

36. Congenital uterovaginal abnormalities, it’s embryogenesis, surgical management and clinical implications

Author

Krishna Gopal Paul, Kalyan Chakravarthi Kosuri, and Hasam Bayad

Subjects

androgen insensitivity syndrome, infertility, vaginal agenesis, wolffian duct, Gynecology and obstetrics, RG1-991

Abstract

Objective Congenital Mullerian duct malformations are a challenging group of conditions for surgeons and need surgical experience and skill. Accordingly, the aim of this study is to present the diagnosis, surgical management, and clinical implications of congenital uterovaginal abnormalities. Methods Between 1980 and 2015, 8 patients with congenital uterovaginal abnormalities were diagnosed. In one patient a unique case of an unusual horseshoe shaped double uterus communicating via a transverse canal along with agenesis of the cervix and vagina was noted, and utero-vaginal agenesis was diagnosed in 6 patients. Complete androgen insensitivity syndrome with its female phenotype associated with bilateral testicular tissue in the inguinal canal with an accompanying absence of the ovaries, uterus, uterine tubes, vagina, and an imperforate hymen, was diagnosed in one patient. Clinical examination of all the patients revealed well-developed secondary sexual characteristics. A modified McIndoe vaginoplasty procedure was the surgical treatment common to all patients to treat vaginal agenesis. The surgery was performed by a consultant (Dr. K.G. Paul) using the standardized surgical technique. Results An unusual Mullerian duct anomaly, uterus bicornisacollis, was successfully corrected by uteroplasty and a new cervix was constructed. Complete vaginal agenesis was corrected by a modified McIndoe vaginoplasty technique. None of the patients had any significant post-operative complications. Conclusion Knowledge of congenital uterovaginal abnormalities diagnosed in this study is essential for surgeons, clinical anatomists, radiologists, and morphologists who may increase the success of their diagnostic evaluations and surgical approaches to the region.

Published

2020

37. TO DETERMINE CUT OFF OF FERTILITY PROFILE OF PATIENTS WITH ANDROGEN INSENSITIVITY SYNDROME (AIS) AT DIFFERENT AGES IN PAKISTANI POPULATION

Author

Waqas Hanif, Naveed Asif, Muhammad Younas, Zujaja Hina Haroon, Qurat Ul Ain, and Noreen .

Subjects

androgen insensitivity syndrome, disorders of sex development, dihydrotestosterone, Medicine, Medicine (General), R5-920

Abstract

Objective: Current study was aimed to determine cut off value of fertility profile in patients with Androgen Insensitivity Syndrome (AIS) presented at different ages tertiary care hospital of Rawalpindi, Pakistan. Study Design: Cross sectional study. Place and Duration of Study: Department of Chemical Pathology and Endocrinology, Armed Forces Institute of Pathology (AFIP) Rawalpindi, from Jan 2016 to Dec 2017. Methodology: Ninety-one (91) patients diagnosed as cases of AIS were included in the study. Subjects were consecutively selected as per inclusion and exclusion criteria. Blood samples were collected from each subject for basal serum testosterone, serum luteinizing hormone (LH) and serum follicular stimulating hormone (FSH) level. Human chorionic gonadotropins (hCG) stimulation test was performed in each subject as per laid down protocol. Sandwich chemiluminescence immunoassay technique was used to analyze serum testosterone, LH and FSH. Serum dihydrotestosterone was also analyzed to calculate testosterone and dihydrotestosterone (T/DHT) ratio. Results: Mean age of subjects was 1.78 ± 0.95 years. Cut off values of serum LH (IU) according to age in patients with AIS are; 6.80 (1 day to 1 year), 6.74 (1 year to 10 years) 6.6 (10 years to onward), serum FSH (IU) 9.71 (1 day to 1 year), 9.01 (1 year to 10 years), 10.01 (10 years to onward), serum testosterone (ng/dl) 107.32 (1 day to 1 year), 120.76 (1 year to 10 years), 98.32 10 years to onward) before and 310.39 (1 day to 1 year), 354.71 (1 year to 10 years), 293.43 (10 years to onward) after hCG, serum..........

Published

2020

38. An Early Case of Complete Androgen Insensitivity Syndrome.

Author

Matalka, Leen, Dean, S. Joy, Beauchamp, Giovanna, and Sunil, Bhuvana

Abstract

Inguinal hernias are rare in female infants, and when present, there is an increased incidence of androgen insensitivity in these infants. We present a case of bilateral inguinal hernias in a 26-day-old full-term phenotypic female. On physical exam, the patient was found to have bilateral palpable inguinal masses which were suspected to be testicular tissue on ultrasound. Patient also had bilateral inguinal hernias, but otherwise there were no other concerning symptoms, and the remaining physical examination was overall unremarkable. Initial workup included a pelvic ultrasound that did not visualize a uterus or ovaries. In addition, genetic testing confirmed normal male genotype with 100% 46, on fluorescence in situ hybridization (FISH) and array comparative genomic hybridization (CGH) was negative and did not reveal any copy number changes. Molecular testing was consistent with a diagnosis of androgen insensitivity syndrome with hemizygous pathogenic variant in the androgen receptor (AR) gene (deletion of Exon 2 of AR gene Xq12). This case highlights the importance of a high clinical suspicion of complete androgen insensitivity syndrome (CAIS) in a phenotypic female infant with inguinal hernias. To our knowledge, this is one of the earliest diagnoses of CAIS in a phenotypically female infant. [ABSTRACT FROM AUTHOR]

Published

2023

39. Potential risk of inguinal hernia in complete androgen insensitivity syndrome.

Author

Yu Kimizuka, Takeshi Sato, Satsuki Nakano, Tomohiro Ishii, and Tomonobu Hasegawa

Subjects

*ANDROGEN-insensitivity syndrome, *INGUINAL hernia, *PRENATAL diagnosis, *VULVA, *IDIOPATHIC thrombocytopenic purpura, *VENTRICULAR septal defects, *PRENATAL genetic testing

Published

2023

40. What Does Androgen Receptor Signaling Pathway in Sertoli Cells During Normal Spermatogenesis Tell Us?

Author

Jia-Ming Wang, Zhen-Fang Li, and Wan-Xi Yang

Subjects

androgen receptor, Sertoli cell, signaling pathway, spermatogenesis, androgen insensitivity syndrome, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Androgen receptor signaling pathway is necessary to complete spermatogenesis in testes. Difference between androgen binding location in Sertoli cell classifies androgen receptor signaling pathway into classical signaling pathway and non-classical signaling pathway. As the only somatic cell type in seminiferous tubule, Sertoli cells are under androgen receptor signaling pathway regulation via androgen receptor located in cytoplasm and plasma membrane. Androgen receptor signaling pathway is able to regulate biological processes in Sertoli cells as well as germ cells surrounded between Sertoli cells. Our review will summarize the major discoveries of androgen receptor signaling pathway in Sertoli cells and the paracrine action on germ cells. Androgen receptor signaling pathway regulates Sertoli cell proliferation and maturation, as well as maintain the integrity of blood-testis barrier formed between Sertoli cells. Also, Spermatogonia stem cells achieve a balance between self-renewal and differentiation under androgen receptor signaling regulation. Meiotic and post-meiotic processes including Sertoli cell - Spermatid attachment and Spermatid development are guaranteed by androgen receptor signaling until the final sperm release. This review also includes one disease related to androgen receptor signaling dysfunction named as androgen insensitivity syndrome. As a step further ahead, this review may be conducive to develop therapies which can cure impaired androgen receptor signaling in Sertoli cells.

Published

2022

41. What Does Androgen Receptor Signaling Pathway in Sertoli Cells During Normal Spermatogenesis Tell Us?

Author

Wang, Jia-Ming, Li, Zhen-Fang, and Yang, Wan-Xi

Subjects

ANDROGEN receptors, SERTOLI cells, CELLULAR signal transduction, SPERMATOGENESIS, ANDROGEN-insensitivity syndrome, PROSTATE cancer, CASTRATION-resistant prostate cancer

Abstract

Androgen receptor signaling pathway is necessary to complete spermatogenesis in testes. Difference between androgen binding location in Sertoli cell classifies androgen receptor signaling pathway into classical signaling pathway and non-classical signaling pathway. As the only somatic cell type in seminiferous tubule, Sertoli cells are under androgen receptor signaling pathway regulation via androgen receptor located in cytoplasm and plasma membrane. Androgen receptor signaling pathway is able to regulate biological processes in Sertoli cells as well as germ cells surrounded between Sertoli cells. Our review will summarize the major discoveries of androgen receptor signaling pathway in Sertoli cells and the paracrine action on germ cells. Androgen receptor signaling pathway regulates Sertoli cell proliferation and maturation, as well as maintain the integrity of blood-testis barrier formed between Sertoli cells. Also, Spermatogonia stem cells achieve a balance between self-renewal and differentiation under androgen receptor signaling regulation. Meiotic and post-meiotic processes including Sertoli cell - Spermatid attachment and Spermatid development are guaranteed by androgen receptor signaling until the final sperm release. This review also includes one disease related to androgen receptor signaling dysfunction named as androgen insensitivity syndrome. As a step further ahead, this review may be conducive to develop therapies which can cure impaired androgen receptor signaling in Sertoli cells. [ABSTRACT FROM AUTHOR]

Published

2022

42. Data on Androgen Insensitivity Syndrome Published by a Researcher at University of Michigan Medical School (Psychiatric Comorbidities in Women with Complete Androgen Insensitivity Syndrome or Mullerian Aplasia/Agenesis).

Abstract

A recent study conducted at the University of Michigan Medical School examined the prevalence of psychiatric diagnoses among individuals with complete androgen insensitivity syndrome (CAIS) or Mullerian duct aplasia/agenesis (MA) compared to male and female reference groups. The research found that individuals with CAIS and MA had higher rates of anxiety and depressive disorders compared to males without DSD, but the differences were less pronounced when compared to females. The study suggests the need for further research to understand the mental health status of individuals with CAIS and MA over time. [Extracted from the article]

Published

2024

43. New Assisted Reproductive Technology Study Findings Have Been Reported from First Affiliated Hospital of Anhui Medical University (Diverse phenotypes and fertility outcomes of patients with androgen insensitivity syndrome in a Chinese family...).

Abstract

A recent study conducted at the First Affiliated Hospital of Anhui Medical University in China explored the diverse phenotypes and fertility outcomes of patients with Androgen Insensitivity Syndrome (AIS) within a single Chinese family. The research identified a specific AR gene variant in four affected patients with varying degrees of AIS and fertility outcomes, expanding the understanding of the condition's phenotypic spectrum. The study highlighted the potential role of androgen concentration in shaping the diversity of AIS phenotypes and emphasized the importance of further investigation in this area. For more information, the full article can be accessed through BMC Medical Genomics. [Extracted from the article]

Published

2024

44. Research on Androgen Insensitivity Syndrome Published by a Researcher at Fondazione Policlinico Universitario A. Gemelli IRCCS (Complete Androgen Insensitivity Syndrome in a Young Girl with Primary Amenorrhea and Suspected Delayed Puberty: A...).

Abstract

The article discusses research on Complete Androgen Insensitivity Syndrome (CAIS) in a 14-year-old girl with primary amenorrhea and suspected delayed puberty. The study highlights the importance of a multidisciplinary approach in managing patients with CAIS, emphasizing individualized care to optimize outcomes. The research also addresses the risk of malignancy, surveillance options, hormone replacement therapy, timing of gonadectomy, and the psychosocial impact of the diagnosis. The study provides insights into the complexity of CAIS management and offers an algorithm for adolescent patients, focusing on a conservative approach for those unwilling to undergo gonadectomy. [Extracted from the article]

Published

2024

45. Studies from Government Medical College Update Current Data on Androgen Insensitivity Syndrome (Partial Androgen Insensitivity Syndrome: Incidentally Diagnosed in an Adolescent).

Abstract

A recent study conducted at Government Medical College in Kerala, India, focused on androgen insensitivity syndrome (AIS), an X-linked genetic disease that affects individuals with a 46, XY karyotype. The study described the case of a 10-year-old child who was incidentally diagnosed with partial AIS. The child had minor virilization of external genitalia and was reared as female. Further investigations revealed the presence of prostate- and testis-like structures, elevated hormone levels, and testicular tissue. The researchers emphasized the importance of early identification of minor virilizing features in order to prevent psychological trauma for both the child and parents. [Extracted from the article]

Published

2024

46. University of Glasgow Researcher Adds New Findings in the Area of Androgen Insensitivity Syndrome (Gynecomastia and Its Management In Boys With Partial Androgen Insensitivity Syndrome).

Abstract

A recent research report from the University of Glasgow discusses findings on androgen insensitivity syndrome (AIS) and its association with gynecomastia in males. The study examined the management of gynecomastia in males with partial androgen insensitivity syndrome (PAIS). The research found that gynecomastia was present in 91% of genetically confirmed cases of PAIS, with a median age of onset at 13.5 years. Surgical management was found to be potentially more effective than medical therapy, but further standardized studies are needed. The report provides valuable insights into the understanding and management of AIS and gynecomastia. [Extracted from the article]

Published

2024

47. Reports Summarize Androgen Insensitivity Syndrome Research from Command Hospital (Eastern Command) (Androgen Insensitivity Syndrome: A Rare Cause of Primary Amenorrhoea).

Abstract

A recent report discusses the research findings on androgen insensitivity syndrome (AIS), a rare disorder of sexual differentiation caused by a mutation in the Androgen Receptor (AR) gene. The report describes several cases of AIS, including patients who presented with inguinal masses, primary amenorrhoea, inguinal hernia, hirsutism, and clitoromegaly. The researchers emphasize the importance of investigating cases of primary amenorrhoea and inguinal hernia in young females, as these may be indicators of AIS. The report concludes that patients with absent pubic/axillary hair and absent uterus/ovaries should raise suspicion of AIS, and young female children with an inguinal hernia should be investigated for AIS. [Extracted from the article]

Published

2024

48. Identification of Potential Genes in Pathogenesis and Diagnostic Value Analysis of Partial Androgen Insensitivity Syndrome Using Bioinformatics Analysis

Author

Yajie Peng, Hui Zhu, Bing Han, Yue Xu, Xuemeng Liu, Huaidong Song, and Jie Qiao

Subjects

androgen insensitivity syndrome, RNA transcriptome, differentially expressed genes, reproduction, immune, metabolism, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

BackgroundAndrogen insensitivity syndrome (AIS) is a rare X-linked genetic disease and one of the causes of 46,XY disorder of sexual development. The unstraightforward diagnosis of AIS and the gender assignment dilemma still make a plague for this disorder due to the overlapping clinical phenotypes.MethodsPeripheral blood mononuclear cells (PBMCs) of partial AIS (PAIS) patients and healthy controls were separated, and RNA-seq was performed to investigate transcriptome variance. Then, tissue-specific gene expression, functional enrichment, and protein–protein interaction (PPI) network analyses were performed; and the key modules were identified. Finally, the RNA expression of differentially expressed genes (DEGs) of interest was validated by quantitative real-time PCR (qRT-PCR).ResultsIn our dataset, a total of 725 DEGs were captured, with functionally enriched reproduction and immune-related pathways and Gene Ontology (GO) functions. The most highly specific systems centered on hematologic/immune and reproductive/endocrine systems. We finally filtered out CCR1, PPBP, PF4, CLU, KMT2D, GP6, and SPARC by the key gene clusters of the PPI network and manual screening of tissue-specific gene expression. These genes provide novel insight into the pathogenesis of AIS in the immune system or metabolism and bring forward possible molecular markers for clinical screening. The qRT-PCR results showed a consistent trend in the expression levels of related genes between PAIS patients and healthy controls.ConclusionThe present study sheds light on the molecular mechanisms underlying the pathogenesis and progression of AIS, providing potential targets for diagnosis and future investigation.

Published

2021

49. Identification of Potential Genes in Pathogenesis and Diagnostic Value Analysis of Partial Androgen Insensitivity Syndrome Using Bioinformatics Analysis.

Author

Peng, Yajie, Zhu, Hui, Han, Bing, Xu, Yue, Liu, Xuemeng, Song, Huaidong, and Qiao, Jie

Subjects

ANDROGEN-insensitivity syndrome, MONONUCLEAR leukocytes, X-linked genetic disorders, SEX differentiation disorders, PATHOGENESIS

Abstract

Background: Androgen insensitivity syndrome (AIS) is a rare X-linked genetic disease and one of the causes of 46,XY disorder of sexual development. The unstraightforward diagnosis of AIS and the gender assignment dilemma still make a plague for this disorder due to the overlapping clinical phenotypes. Methods: Peripheral blood mononuclear cells (PBMCs) of partial AIS (PAIS) patients and healthy controls were separated, and RNA-seq was performed to investigate transcriptome variance. Then, tissue-specific gene expression, functional enrichment, and protein–protein interaction (PPI) network analyses were performed; and the key modules were identified. Finally, the RNA expression of differentially expressed genes (DEGs) of interest was validated by quantitative real-time PCR (qRT-PCR). Results: In our dataset, a total of 725 DEGs were captured, with functionally enriched reproduction and immune-related pathways and Gene Ontology (GO) functions. The most highly specific systems centered on hematologic/immune and reproductive/endocrine systems. We finally filtered out CCR1, PPBP, PF4, CLU, KMT2D, GP6, and SPARC by the key gene clusters of the PPI network and manual screening of tissue-specific gene expression. These genes provide novel insight into the pathogenesis of AIS in the immune system or metabolism and bring forward possible molecular markers for clinical screening. The qRT-PCR results showed a consistent trend in the expression levels of related genes between PAIS patients and healthy controls. Conclusion: The present study sheds light on the molecular mechanisms underlying the pathogenesis and progression of AIS, providing potential targets for diagnosis and future investigation. [ABSTRACT FROM AUTHOR]

Published

2021

50. Analysis of gender assignment in children with 46, XY disorders of sex development.

Author

LIANG Yan, LÜ Yi-qing, XIE Hua, HUANG Yi-chen, LI Xiao-xi, LI Pin, and XI Yi-qun

Abstract

Objective·To explore the results of gender assignment of the patients with 46, XY disorders of sex development (DSD), and provide reference for clinical decision-making of similar patients. Methods·The clinical data of 46,XY DSD patients who were treated in Children's Hospital of Shanghai Jiao Tong University from 2015 to 2018 were collected. All the patients completed comprehensive assessments in the Department of Pediatric Endocrinology. Gender assignment was carried out after multidisciplinary treatment team discussion and full communication with the patients and/or the family members. The gender assignment results of these patients with different conditions were analyzed. The follow-up began 1 month after operation until 18 years old. Psychological assessment was performed after puberty. Results·A total of 52 patients with 46,XY DSD were collected. Before admission, 26 cases were female and 26 cases were male. Thirteen female patients were assigned to the same gender, among whom 6 cases were diagnosed as having complete androgen insensitivity syndrome, 2 cases diagnosed as having 17α-hydroxylase deficiency with extremely poor testicular function, 1 diagnosed as having complete gonadal dysplasia, and 4 diagnosed as having testicular dysfunction; otherwise 13 female patients changed gender to male, because 3 patients had partial androgen insensitive syndrome, 4 patients had 5α-reductase deficiency, 2 patients had androgen synthesis disorder, and the etiology of 4 patients was unknown (gonadal biopsy showed that both gonads of the patients were testicular tissues). All the 26 male patients were assigned to the same gender, among whom 11 cases were diagnosed as having 5α -reductase deficiency, 6 diagnosed as having partial androgen insensitivity syndrome, 4 diagnosed as having androgen synthesis disorder, and 5 cases with unknown etiology (gonadal biopsy showed bilateral testicular tissues in 2 cases and unilateral gonadal dysplasia with contralateral testicular tissue in 3 cases). Thirteen patients who reached the age of psychological evaluation did not exist gender identity confusion. Conclusion·The 46,XY DSD patients with complete gonadal dysplasia, complete androgen insensitivity syndrome or testicular dysfunction can be considered for female gender assignment. The patients with 5α-reductase deficiency or partial androgen insensitivity syndrome can be considered for male selection. For the children with unknown etiology, it should be considered comprehensively according to the specific phenotype and the actual situation of children's families. [ABSTRACT FROM AUTHOR]

Published

2021