Your search keyword '"Hiort O."' showing total 20 results

1. Array-CGH analysis in patients with syndromic and non-syndromic XY gonadal dysgenesis: evaluation of array CGH as diagnostic tool and search for new candidate loci.

Author

Ledig, S., Hiort, O., Scherer, G., Hoffmann, M., Wolff, G., Morlot, S., Kuechler, A., and Wieacker, P.

Subjects

*COMPARATIVE genomic hybridization, *TURNER'S syndrome, *GENETIC mutation, *GENETIC disorder diagnosis, *KARYOTYPES, *PATIENTS, GONADAL diseases

Abstract

BACKGROUND: XY gonadal dysgenesis (XY-GD) is a heterogeneous disorder characterized by failure of testicular development despite a normal male karyotype. Non-syndromic and syndromic forms can be delineated. Currently, only a minority of cases can be explained by gene mutations. [ABSTRACT FROM AUTHOR]

Published

2010

2. Androgen insensitivity and male infertility1.

Author

Hiort, O. and Holterhus, P.-M.

Subjects

*SPERMATOGENESIS, *ANDROGENS, *GENETIC mutation

Abstract

Summary Abnormal human spermatogenesis can be caused by defects in androgen action because of androgen insensitivity. A variety of mutations have been described in the human androgen receptor gene associated with male infertility. These can be attributed to two molecular mechanisms. First, point mutations in the androgen receptor gene cause alterations in the amino acid sequence and, hence, lead to apparently slight changes in the androgen receptor effector mechanisms and mild androgen insensitivity. Secondly, variations in the polymorphic poly glutamine segment within the N-terminal end of the androgen receptor have been ascribed to correlate with fertility aspects possibly because of modifications of transcriptional regulatory mechanisms. It has been postulated that longer poly glutamine segments are associated with decreased sperm counts. However, the molecular mechanisms that lead to inhibition of spermatogenesis because of a mutated androgen receptor are poorly understood and will need more focus in the future. [ABSTRACT FROM AUTHOR]

Published

2003

3. Functional assessment and clinical classification of androgen sensitivity in patients with mutations of the androgen receptor gene. German Collaborative Intersex Study Group.

Author

Sinnecker, G H, Hiort, O, Nitsche, E M, Holterhus, P M, and Kruse, K

Abstract

Unlabelled: In the genetic male, mutations of the androgen receptor (AR) gene cause phenotypes ranging from female to subfertile male. Binding assays on genital skin fibroblasts and DNA analysis alone provide incomplete information about receptor function. We used the sex hormone-binding globulin (SHBG) response to stanozolol as a measure of AR function and correlated the results with phenotypes which were classified according to the degree of defective masculinization. Of the 34 patients investigated, 9 had complete, and 14 had partial androgen insensitivity syndrome (AIS) with predominantly female, ambiguous, or predominantly male phenotype. Eleven subjects served as controls. Mutations were characterized using polymerase chain reaction-single strand conformation polymorphism analysis and direct DNA sequencing. DNA analysis revealed two major deletions, two minor defects leading to premature stop codons in exon 1, and 19 point mutations in the DNA- and hormone-binding domains of the AR gene. After stanozolol, SHBG remained unchanged in patients with complete AIS (102.0 +/- 3.8 [SE]%; range 92.4%-129% of the initial value). The SHBG decrease was diminished in partial AIS with predominantly female (83.8% +/- 1.7%; range 81.3%-87.0%), ambiguous (80.4% +/- 4.4%, range 68.4%-89.1%), and predominantly male (mean 65.9% +/- 4.9%, range 48.6%-80.8%) phenotypes, and normal in controls (51.4% +/- 2.1%, range 35.6%-62.1%). Differences between controls and each AIS group were statistically significant (P < 0.05 - < 0.0001). A close correlation was found between the degree of undermasculinization (AIS phenotype) and the SHBG response.Conclusions: The SHBG test provides functional information about the severity of the receptor defect in vivo and hence adds to the structural information provided by DNA analysis. It detects receptor defects due to mutations within the entire gene, including the DNA-binding domain, and is a rapid, simple, and cost effective procedure. It may provide useful information for the diagnosis and management of affected children. [ABSTRACT FROM AUTHOR]

Published

1997

4. Male infertility and increased risk of diseases in future generations.

Author

Hiort, O, Horter, T, Schulze, W, Kremke, B, and Sinnecker, G H

Published

1999

5. Sex dimorphism of weight and length at birth: evidence based on disorders of sex development.

Author

Amais, D.S.R., da Silva, T.E.R., Barros, B.A., de Andrade, J.G.R., de Lemos-Marini, S.H.V., de Mello, M.P., Marques-de-Faria, A.P., Mazzola, T.N., Guaragna, M.S., Fabbri-Scallet, H., Vieira, T.A.P., Viguetti-Campos, N.L., Morcillo, A.M., Hiort, O., Maciel-Guerra, A.T., and Guerra-Junior, G.

Subjects

*BIRTH weight, *SEX differentiation disorders, *SEXUAL dimorphism, *ANDROGEN-insensitivity syndrome, *ADRENOGENITAL syndrome, *FRAGILE X syndrome

Abstract

Males have higher weight and length at birth than females. To verify the influence of the Y chromosome and the action of intrauterine androgens on weight and length at birth of children with Disorders of Sex Development (DSD). A cross-sectional and retrospective study. Patients with Turner syndrome (TS), complete (XX and XY), mixed (45,X/46,XY) and partial (XY) gonadal dysgenesis (GD), complete (CAIS) and partial (PAIS) androgen insensitivity syndromes and XX and XY congenital adrenal hyperplasia (CAH) were included. Weight and length at birth were evaluated. Weight and length at birth were lower in TS and mixed GD when compared to XY and XX DSD cases. In turn, patients with increased androgen action (117 cases) had higher weight and length at birth when compared to those with absent (108 cases) and decreased (68 cases) production/action. In birthweight, there was a negative influence of the 45,X/46,XY karyotype and a positive influence of increased androgen and gestational age. In birth length, there was a negative influence of the 45,X and 45,X/46,XY karyotypes and also a positive influence of increased androgen and gestational age. The sex dimorphism of weight and length at birth could possibly be influenced by intrauterine androgenic action. [ABSTRACT FROM AUTHOR]

Published

2022

6. Anabolic steroids, testosterone-precursors and virilizing androgens induce distinct activation profiles of androgen responsive promoter constructs

Author

Holterhus, P.M., Piefke, S., and Hiort, O.

Subjects

*ANDROGENS, *TESTOSTERONE

Abstract

Different androgens, e.g. virilizing androgens such as testosterone and its precursors as well as synthetic anabolic steroids, respectively, induce diverse biological effects. The molecular basis for this variety in biological actions, however, is not well understood. We hypothesized that this variability of actions may be due to steroid-specific target gene expression profiles following androgen receptor (AR)-activation. Therefore, we investigated androgen receptor dependent transactivation of three structurally different androgen responsive promoter constructs ((ARE)2TATA-luc, MMTV-luc, GRE-OCT-luc) in co-transfected Chinese hamster ovary (CHO)-cells as an artificial model simulating different natural target genes. Three virilizing androgens (dihydrotestosterone, testosterone, methyltrienolone), three anabolic steroids (oxandrolone, stanozolol, nandrolone) and two testosterone-precursors of gonadal and adrenal origin (dehydroepiandrosterone, androstenedione) were used as ligands (0.001–100 nM). All steroids proved to be potent activators of the AR. Remarkably, anabolic steroids and testosterone-precursors showed characteristic promoter activation profiles distinct from virilizing androgens with significantly lower (ARE)2TATA-luc activation. Hierarchical clustering based on similarity of activation profiles lead to a dendrogram with two major branches: first virilizing androgens, and second anabolics/testosterone-precursors. We conclude that steroid-specific differences in gene transcription profiles due to androgen receptor activation could contribute to differences in biological actions of androgens. [Copyright &y& Elsevier]

Published

2002

7. Parental expectations before and after 12‐month experience with video consultations combined with regular outpatient care for children with type 1 diabetes: a qualitative study.

Author

von Sengbusch, S., Doerdelmann, J., Lemke, S., Lange, K., Hiort, O., Katalinic, A., and Frielitz, F. S.

Subjects

*PARENT attitudes, *RESEARCH, *OUTPATIENT medical care, *HEALTH services accessibility, *CONFIDENCE, *TYPE 1 diabetes, *VIDEOCONFERENCING, *MEDICAL cooperation, *INTERVIEWING, *MEDICAL personnel, *EXPERIENCE, *QUALITATIVE research, *PRE-tests & post-tests, *INSULIN, *PATIENTS' families, *MEDICAL referrals, *CONTENT analysis, *MEDICAL appointments, *INTERNET service providers, *TELEMEDICINE

Abstract

Aim: To explore parents' expectations of the perceived barriers to and benefits of 1 year of monthly video consultations combined with regular outpatient care of children with type 1 diabetes. Methods: The Virtual Diabetes Outpatient Clinic for Children and Youth (VIDIKI) study was a controlled, multicentre, perennial study with 240 participants from northern Germany. Fifty‐four qualitative interviews with parents were analysed using qualitative content analysis. Before the intervention, 30 interviews were conducted to assess parents' expectations, and after 1 year, 24 interviews evaluated the experienced benefits and barriers to video consultations. Results: Four main topics were identified from parents' responses to the video consultation. The main advantages of the video consultation compared with standard care were a higher frequency of contact for optimized insulin dosing and saving time; difficulties with internet connections were identified as the main barrier. A feeling of increased confidence with respect to insulin dosing was directly associated with telemedicine. Digital prescriptions and meeting the same diabetologist in both outpatient and telemedical care were mentioned as important improvements. The majority of interviewees preferred intervals of 4–6 weeks between video consultations. Conclusion: The higher frequency of contact with the diabetes team was considered a great relief by parents of children with type 1 diabetes. Apart from the time savings and flexibility in appointments, the most important advantages were the higher frequency of contact leading to short‐term therapy adjustments and an increase in the ability to adjust therapy independently. (German Clinical Trials Registry No: DRKS00012645). [ABSTRACT FROM AUTHOR]

Published

2021

8. Linear skin atrophy preceding calcinosis cutis in pseudo-pseudohypoparathyroidism.

Author

Lau, K., Willig, R. P., Hiort, O., and Hoeger, P. H.

Subjects

*ATROPHY, *PSEUDOHYPOPARATHYROIDISM, *GENETIC mutation, *CALCIUM metabolism, *HISTOLOGY

Abstract

Albright hereditary osteodystrophy (AHO) is a syndrome caused by inactivating mutations in the GNAS (guanine nucleotide-binding protein, alpha-stimulating) gene. Patients with AHO have short stature, obesity, brachydactyly and subcutaneous calcifications. AHO can be associated with pseudohypoparathyroidism type IA (PHP-IA) with upregulation of parathyroid hormone, whereas in pseudo-pseudohypoparathyroidism (PPHP), an endocrinopathy is not present. We report the case of a 5-month-old male infant who presented with slowly progressive linear atrophic skin lesions. The histological findings showed evidence of dermal hypoplasia. The child's father had PHP-IA. Four months after presentation, the infant developed calcifications within the pre-existent atrophic lesions. No alterations in calcium metabolism were noted. Analysis of the GNAS gene identified a short duplication leading to a frameshift mutation. We conclude that linear atrophic skin lesions may be an early sign of imminent cutaneous calcifications in AHO. [ABSTRACT FROM AUTHOR]

Published

2012

9. The current landscape of European registries for rare endocrine conditions.

Author

Ali, S. R., Bryce, J., Cools, M., Korbonits, M., Beun, J. G., Taruscio, D., Danne, T., Dattani, M., Dekkers, O. M., Linglart, A., Netchine, I., Nordenstrom, A., Patocs, A., Persani, L., Reisch, N., Smyth, A., Sumnik, Z., Visser, W. E., Hiort, O., and Pereira, A. M.

Subjects

*SEX differentiation disorders, *DATABASE searching

Abstract

Objective: To identify cross-border international registries for rare endocrine conditions that are led from Europe and to understand the extent of engagement with these registries within a network of reference centres (RCs) for rare endocrine conditions. Methods: Database search of international registries and a survey of RCs in the European Reference Network for rare endocrine conditions (Endo-ERN) with an overall response rate of 82%. Results: Of the 42 conditions with orphacodes currently covered within Endo-ERN, international registries exist for 32 (76%). Of 27 registries identified in the Orphanet and RD-Con nect databases, Endo-ERN RCs were aware of 11 (41%). Of 21 registries identified by the RC, RD-Connect and Orphanet d id not have a record of 10 (48%). Of the 29 glucose RCs, the awareness and participation rate in an international registry was highest for rare diabetes at 75 and 56% respectively. Of the 37 sex development RCs, the corresponding rates were highest for disorders of sex development at 70 and 52%. Of the 33 adrenal RCs, the rates were highest for adrenocortical tumours at 68 and 43%. Of the 43 pituitary RCs, the rates were highest for pituitary adenomas at 43 and 29%. Of the 31 genetic tumour RCs, the rates were highest for MEN1 at 26 and 9%. For the remaining conditions, awareness and participation in registries was less than 25%. Conclusion: Although there is a need to develop new registries for rare endocrine conditions, there is a more immediate need to improve the awareness and participation in existing registries. [ABSTRACT FROM AUTHOR]

Published

2019

10. Approaches to molecular genetic diagnosis in the management of differences/disorders of sex development (DSD): position paper of EU COST Action BM 1303 'DSDnet'.

Author

Audí, L., Ahmed, S. F., Krone, N., Cools, M., McElreavey, K., Holterhus, P. M., Greenfield, A., Bashamboo, A., Hiort, O., Wudy, S. A., and McGowan, R.

Subjects

*SEX differentiation disorders, *MOLECULAR diagnosis, *MOLECULAR genetics

Abstract

The differential diagnosis of differences or disorders of sex development (DSD) belongs to the most complex fields in medicine. It requires a multidisciplinary team conducting a synoptic and complementary approach consisting of thorough clinical, hormonal and genetic workups. This position paper of EU COST (European Cooperation in Science and Technology) Action BM1303 'DSDnet' was written by leading experts in the field and focuses on current best practice in genetic diagnosis in DSD patients. Ascertainment of the karyotpye defines one of the three major diagnostic DSD subclasses and is therefore the mandatory initial step. Subsequently, further analyses comprise molecular studies of monogenic DSD causes or analysis of copy number variations (CNV) or both. Panels of candidate genes provide rapid and reliable results. Whole exome and genome sequencing (WES and WGS) represent valuable methodological developments that are currently in the transition from basic science to clinical routine service in the field of DSD. However, in addition to covering known DSD candidate genes, WES and WGS help to identify novel genetic causes for DSD. Diagnostic interpretation must be performed with utmost caution and needs careful scientific validation in each DSD case. [ABSTRACT FROM AUTHOR]

Published

2018

11. Steroid hormone analysis in diagnosis and treatment of DSD: position paper of EU COST Action BM 1303 'DSDnet'.

Author

Kulle, A., Krone, N., Holterhus, P. M., Schuler, G., Greaves, R. F., Juul, A., de Rijke, Y. B., Hartmann, M. F., Saba, A., Hiort, O., and Wudy, S. A.

Subjects

*STEROID hormones, *SEX differentiation disorders, *THERAPEUTICS

Abstract

Disorders or differences in sex development (DSD) comprise a heterogeneous group of conditions with an atypical sex development. For optimal diagnosis, highly specialised laboratory analyses are required across European countries. Working group 3 of EU COST (European Cooperation in Science and Technology) Action BM 1303 'DSDnet' 'Harmonisation of Laboratory Assessment' has developed recommendations on laboratory assessment for DSD regarding the use of technologies and analytes to be investigated. This position paper on steroid hormone analysis in diagnosis and treatment of DSD was compiled by a group of specialists in DSD and/or hormonal analysis, either from participating European countries or international partner countries. The topics discussed comprised analytical methods (immunoassay/mass spectrometry-based methods), matrices (urine/serum/saliva) and harmonisation of laboratory tests. The following positions were agreed upon: support of the appropriate use of immunoassay- and mass spectrometry-based methods for diagnosis and monitoring of DSD. Serum/plasma and urine are established matrices for analysis. Laboratories performing analyses for DSD need to operate within a quality framework and actively engage in harmonisation processes so that results and their interpretation are the same irrespective of the laboratory they are performed in. Participation in activities of peer comparison such as sample exchange or when available subscribing to a relevant external quality assurance program should be achieved. The ultimate aim of the guidelines is the implementation of clinical standards for diagnosis and appropriate treatment of DSD to achieve the best outcome for patients, no matter where patients are investigated or managed. [ABSTRACT FROM AUTHOR]

Published

2017

12. Testosterone Synthesis in Patients with 17β-Hydroxysteroid Dehydrogenase 3 Deficiency.

Author

Werner, R., Kulle, A., Sommerfeld, I., Riepe, F.G., Wudy, S., Hartmann, M.F., Merz, H., Döhnert, U., Bertelloni, S., Holterhus, P.-M., and Hiort, O.

Abstract

17β-hydroxysteroid dehydrogenase 3 (17β-HSD 3) deficiency is a rare cause of 46,XY disorders of sex development (DSD). At puberty, these patients experience a surge of androstenedione and also testosterone, leading to substantial virilization. The origin of testosterone synthesis in these patients remains elusive. We investigated the expression of the isoenzyme AKR1C3 (17β-HSD 5) in the testis and patient-derived genital skin fibroblasts (GSF) as well as the ability of GSF to synthesize testosterone. Supernatants of GSF cultures and serum samples of one patient before and after gonadectomy were analyzed by liquid and gas chromatography/mass spectrometry. The androgenic potential of GSF-derived supernatants was also assessed by androgen receptor-mediated transactivation of a reporter gene in transiently transfected Chinese hamster ovary cells. Although AKR1C3 is expressed both in the testes and in GSF, androstenedione is rapidly metabolized and is not synthesized to testosterone. The transactivation potential of GSF supernatants towards the androgen receptor is declining within 48 h. However, under testis-equivalent androstenedione concentration, testosterone can be synthesized in 17β-HSD 3-negative GSF. After gonadectomy, both androstenedione and testosterone decline rapidly in vivo. In 17β-HSD 3 deficiency, relevant amounts of testosterone are synthesized most probably through AKR1C3 in the testis and not peripherally in GSF. Copyright © 2012 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2012

13. Tissue-specific transcription profiles of sex steroid biosynthesis enzymes and the androgen receptor.

Author

Hoppe, U., Holterhus, P.-M., Wünsch, L., Jocham, D., Drechsler, T., Thiele, S., Marschke, C., and Hiort, O.

Subjects

*DEHYDROGENASES, *ISOENZYMES, *STEROID hormones, *ANDROGENS, *SEX hormones, *PERFORMANCE-enhancing drugs

Abstract

17β-hydroxysteroid dehydrogenase (17β-HSD) and 5α-reductase isoenzymes play a crucial role in the formation and metabolism of sex steroids. Not only the key androgens testosterone and dihydrotestosterone but also their precursors are potent activators of the androgen receptor and are, therefore, likely to act as determinants of male sexual differentiation and maturation in a differentially regulated way. The aim of the present study was to relatively quantify the expression of the mRNA of 17β-HSD isoenzymes, namely, type 1, 2, 3, 4, 5, 7, and 10, together with the 5α-reductase type 1 and 2, and the androgen receptor in normal human males and females. RNA was isolated from peripheral blood cells of both sexes and from genital skin fibroblasts (GSFs) of two different localizations (foreskin and scrotal skin) obtained from phenotypically normal males. mRNA expression was semi-quantified by quantitative reverse-transcriptase polymerase chain reaction with the LightCycler Instrument (Roche). The examined enzymes show statistically significant differences in their transcription pattern between the blood and the GSF RNA samples. Within the GSF samples, there are also significant variations between the two examined localizations in the transcription of 17β-HSD type 1, 2, 4, and 5 as well as for the androgen receptor. We found large interindividual variation of enzyme transcription patterns in all investigated tissues. In peripheral blood cells, no sex-specific differences were seen. We conclude that sex steroid enzymes are expressed not only in genital primary target tissues but also in peripheral blood. The expression in different target tissues may contribute to both the individual sexual and tissue-specific phenotype in humans. [ABSTRACT FROM AUTHOR]

Published

2006

14. Mobile diabetes education and care: intervention for children and young people with Type 1 diabetes in rural areas of northern Germany.

Author

von Sengbusch, S., Müller-Godeffroy, E., Häger, S., Reintjes, R., Hiort, O., and Wagner, V.

Subjects

*DIABETES in children, *DIABETES, *QUALITY of life, *MEDICAL care, *EDUCATION

Abstract

Aims To improve the quality of care in children with Type 1 diabetes who have limited access to specialized diabetes care in rural areas, by providing a mobile diabetes education and care team, affiliated with a University hospital paediatric diabetes centre. Methods A cohort of 107 children and their families from eight rural hospitals was followed between July 2000 and July 2002. Parameters on quality of metabolic control (HbA1c, hospitalization rate and number of episodes of severe hypoglycaemia), diabetes knowledge and quality of life at baseline (t0), 6 weeks (t1) and 6 months (t2) after the interventions were measured. Results Mean HbA1c was 7.9 ± 1.4% at t0. The proportion of HbA1c values < 6.8% increased significantly ( P < 0.05) and of values > 8.0% decreased significantly ( P < 0.01) at t1 and t2. The rate of hospitalization fell significantly by 9.4%, from 16.2% at baseline to 6.8% at t2 ( P < 0.05). The children reported significantly better diabetes-specific quality of life ( P < 0.05) and higher self-esteem ( P < 0.01) after the intervention. Theoretical diabetes knowledge was increased both in the short and long term ( P < 0.05). Conclusions The intervention improved metabolic control, diabetes knowledge and diabetes-specific quality of life. We conclude that high-quality diabetes care in a rural area can be provided by a mobile diabetes education and care team. [ABSTRACT FROM AUTHOR]

Published

2006

15. Effective NSAID treatment indicates that hyperprostaglandinism is affecting the clinical severity of childhood hypophosphatasia.

Author

Girschick, H. J., Schneider, P., Haubitz, I., Hiort, O., Collmann, H., Beer, M., Shin, Y. S., and Seyberth, H. W.

Subjects

*HYPOPHOSPHATASIA, *PROSTAGLANDINS, *BONE metastasis, *PHENOTYPES, *FIBROBLASTS, *GENE expression

Abstract

Background: Hypophosphatasia (HP) is an inborn error of bone metabolism characterized by a genetic defect in the gene encoding the tissue-nonspecific alkaline phosphatase (TNSALP). There is a lack of knowledge as to how the variability and clinical severity of the HP phenotype (especially pain and walking impairment) are related to metabolic disturbances or impairments, subsequent to the molecular defect. Methods: We analyzed the changes in clinical symptoms and the prostaglandin (PG) metabolism in response to treatment with non-steroidal anti-inflammatory drugs (NSAIDs) in six children affected by childhood HP. In addition, by exposing HP fibroblasts to pyridoxal phosphate and/or calcium pyrophosphate in vitro, we analyzed whether the alterations in PG levels are sequelae related to the metabolic defect. Results: Childhood HP patients, who often complain about pain in the lower limbs without evident fractures, have systemic hyperprostaglandinism. Symptomatic anti-inflammatory treatment with NSAIDs significantly improved pain-associated physical impairment. Calcium pyrophosphate, but not pyridoxal phosphate, induced cyclooxygenase-2 (COX-2) gene expression and PG production in HP and normal fibroblasts in vitro. Conclusion: Clinical features of childhood HP related to pain in the lower legs may be, at least in part, sequelae related to elevated PG levels, secondary to the primary metabolic defect. Consequently, NSAID treatment does improve the clinical features of childhood HP. [ABSTRACT FROM AUTHOR]

Published

2006

16. Molecular features and clinical phenotypes in androgen insensitivity syndrome in the absence and presence of androgen receptor gene mutations.

Author

Holterhus, P. M., Werner, R., Hoppe, U., Bassler, J., Korsch, E., Ranke, M. B., Dörr, H. G., and Hiort, O.

Subjects

*INTERSEXUALITY, *SEX differentiation disorders, *ANDROGEN-insensitivity syndrome, *SEXUAL dysfunction, *VIRILISM, *GENETIC mutation, *HORMONE receptors, *CELL receptors, *DRUG receptors, *GENETICS

Abstract

Androgen insensitivity syndrome (AIS) is characterized by deficient or absent virilization in 46,XY individuals despite normal or even elevated androgen levels. AIS is usually caused by mutations in the androgen receptor (AR) gene. We aimed at contrasting clinical, biochemical, and molecular genetic characteristics of three patients (P1–P3) with clinically evident partial (P1) and complete (P2, P3) AIS with and without AR gene mutations. AR expression was studied in cultured genital skin fibroblasts (GSF) by Western immunoblotting, ligand binding analyses, Northern blotting, semiquantitative reverse transcription–polymerase chain reaction (RT-PCR), and RT-PCR spanning exons 1–8. AR gene DNA sequence was analyzed by single-strand conformation analysis (SSCA), and DNA sequencing. GSF revealed reduced (P1) or absent (P2, P3) ligand binding. Northern blots showed either slightly reduced hybridization of the 10.5-kb AR transcript (P3) or no hybridization (P1, P2), as confirmed by semiquantitative RT-PCR. RT-PCR spanning exons 1–8 detected single AR mRNA bands in P1–P3 excluding splicing errors. Western analyses showed either low (P1) or no (P2, P3) AR protein. While SSCA initially did not reveal any molecular abnormality, sequencing showed a novel CAG (Gln) to TAG (stop) mutation at codon 59 (P3) and a previously described 2-bp deletion at codon 472, leading to a frameshift and premature stop in codon 499 (P2). Intriguingly, P1 showed an unaltered DNA sequence of the coding region of the AR gene including all intron–exon boundaries. In conclusion, patients with clinically evident complete AIS are likely to harbor an AR gene mutation, demanding that the two polymorphic regions must always be included in molecular analyses of the AR gene. Moreover, our data support the concept that in a subset of AIS patients, particularly those with partial AIS, molecular alterations outside the coding region of the AR gene must be presumed. [ABSTRACT FROM AUTHOR]

Published

2005

17. Transactivation Properties of Wild-Type and Mutant Androgen Receptors in Transiently Transfected Primary Human Fibroblasts.

Author

Holterhus, P. M., Salzburg, J., Werner, R., and Hiort, O.

Subjects

*ANDROGENS, *ANDROSTANE, *FIBROBLASTS, *CELLS, *CONNECTIVE tissue cells, *PLASMIDS

Abstract

Background: Stromal cells play key roles during androgen-mediated male sexual differentiation. Our objective was to establish a transient transfection method for primary human fibroblasts enabling functional characterization of wild-type (wt) and mutant androgen receptor (AR) plasmid constructs, corresponding to partial and complete androgen insensitivity syndrome (PAIS/CAIS). Methods: An AR-negative fibroblast strain (ARD842) was established from the gonads of a CAIS patient. Wt-AR or either mutants L712F (PAIS), R774C or V866M (CAIS) were transfected using a polyamine-based procedure. Alternatively, two AR-positive male foreskin fibroblast strains were investigated. Androgen-induced activation of two co-transfected reporter plasmids ((ARE)2TATA-, MMTV-luciferase) was measured. Results: All three fibroblast strains showed a ligand-dependent rise of luciferase activity after transfection of wt-AR. Mutant plasmids were assessed in AR-negative ARD842 cells. While L712F showed high partial activity, R774C and V866M were nearly inactive. The intrinsic AR of normal foreskin fibroblasts revealed no measurable ligand-inducible reporter gene activity. Conclusions: Polyamine-based transfection of AR plasmids into cultured fibroblasts provides a promising tool for analysis of AR transactivation, thereby considering a stromal cellular background. This is supported by the mutant ARs which showed the expected levels of impaired transactivation with respect to the corresponding AIS phenotypes. The role of the intrinsic AR in normal male human foreskin fibroblasts needs further exploration. Copyright © 2005 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2005

18. Expression of two functionally different androgen receptors in a patient with androgen insensitivity.

Author

Holterhus, P. M., Sinnecker, G. H. G., Wollmann, H. A., Struve, D., Homburg, N., Kruse, K., Hiort, O., and Sinnecker, G H

Subjects

*ANDROGENS, *GENETIC mutation, *INFANT diseases

Abstract

Recently, we demonstrated a previously unknown high rate of de novo mutations of the androgen receptor (AR) gene in androgen insensitivity syndrome (AIS) with some resulting in somatic mosaicism of mutant and wild type AR alleles. However, data on the genotype-phenotype relationship in the latter patients are sparse. We present here a 46,XY newborn with ambiguous genitalia carrying a mosaic of an 866 GTG (Val) --> ATG (Met) mutation with the wild type AR gene. This mutation has usually been associated with complete AIS. Accordingly, we found markedly impaired transactivation due to the mutant Met866 AR. Essential information arose from Scatchard analysis of methyltrienolone binding on cultured genital skin fibroblasts. We demonstrated for the first time the expression of two functionally different ARs (Kd1: 5.58 nM = mutant, Kd2: 0.06 nM = wild type) in one AIS individual. This finding not only represents an important confirmation for the presence of the somatic mosaicism in the patient, it also indicates the most likely molecular mechanism responsible for the unexpectedly strong virilization of the patient: Androgen action through the wild type AR expressed by part of the somatic cells. The present case clearly demonstrates the molecular mechanism by which somatic mosaicism of the androgen receptor gene can modulate in vivo androgen action. It underlines the importance of particular notice on somatic mosaicism in all androgen insensitivity syndrome patients carrying de novo mutations of the androgen receptor gene. [ABSTRACT FROM AUTHOR]

Published

1999

19. Defective sexual development in an infant with 46, XY, der(9)t(8;9)(q23.1;p23)mat.

Author

Pfeiffer, R. A., Rauch, A., Trautmann, U., Dörr, H. G., Hiort, O., Scherer, G., Rösch, G., Papadopoulos, T., v. d. Hardt, K., Lachmann, E., Dörr, H G, and Rösch, G

Subjects

*HYPOSPADIAS, *GENITAL abnormalities, *ANDROGENS, *MORPHOGENESIS, *GENETIC mutation

Abstract

Unlabelled: We report on a male infant with ambiguous genitalia (scrotal hypospadias, sinus urogenitalis) trisomic for 8q23-ter and monosomic for 9p23-ter, who shared craniofacial and other abnormalities with either phenotype. Gonadal histology was nearly normal for age. Normal endocrinological findings and exclusion of mutations in SRY, androgen receptor and alpha-reductase genes point to supplementary gene(s) located in 9p2305-ter, haplo-insufficiency (by deletion) of which is expected to cause defective male morphogenesis.Conclusion: This observation lends further support to the hypothesis that genetic factors are located at 9p23-ter which are involved in normal sex determination. [ABSTRACT FROM AUTHOR]

Published

1999

20. Evaluation of DSD training schools organized by cost action BM1303 "DSDnet".

Author

Bertalan, R., Lucas-Herald, A., Kolesinska, Z., Berra, M., Cools, Martine, Balsamo, A., and Hiort, O.

Subjects

*SEX differentiation disorders, *SEXUAL dysfunction, *ENDOCRINOLOGY, *MEDICAL schools, *MEDICAL personnel training, *CLINICAL medicine

Abstract

Background: The Differences of Sex Development network (DSDnet) aims to establish interactive relationships between clinicians, scientists, support groups and people with a difference of sex development (DSD) to improve the overall care for people affected by such condition. DSDnet has hosted three Training Schools (TSs) in Ghent, Bologna and Budapest between 2015 and 2017 with the primary purpose of providing multidisciplinary training to young professionals and encouraging ongoing activity in the field of DSD. The aim of our study was to evaluate the success and long-term effect effectiveness of these three TSs.Methods and Results: Eighty-seven trainees (70 women, 17 men) attended one of three TSs. The distribution of trainees according to their professional field was: 47 (54.0%) from Pediatrics/Endocrinology, 13 (14.9%) from Biology/Genetics, 12 (13.8%) from Psychology/Psychiatry and 15 (17.2%) from Surgical Professions. All trainees were asked to complete an evaluation form on the last day of the TS to gain feedback on how to improve the next one. A further survey was sent at the end of 2017 to provide information about the overall long-term impact of the TSs. Seventy-eight (89.7%) trainees completed evaluation forms at the end of the respective TSs. Replies to the subsequent survey were received from 76 (87.4%) of trainees. A total of 72/76 (94.7%) responders reported that they continue to be active in the field of DSD. The vast majority (64/68, 94.1%) reported that the TSs had enlarged their professional networks. Among the 76 respondent trainees, 11.8% (n = 9) had applied for a research grant and 10.5% (n = 8) had received a fellowship related to DSD since their TS attendance.Conclusions: According to our results, the majority of TS participants continue to be active in the field of DSD and have enlarged their professional networks following participation at the TS. These findings indicate the need of this type of educational program and justify ongoing efforts to provide postgraduate multidisciplinary training in rare diseases such as DSD. [ABSTRACT FROM AUTHOR]

Published

2018