Your search keyword '"H. G. Doerr"' showing total 12 results

1. Malformationen des Zentralnervensystems : Seltene Ursachen eines organischen Wachstumshormonmangels bei Kindern

Author

H. L. Mueller, Klaus Mohnike, M. Bettendorf, Thomas Reinehr, Joachim Woelfle, Günter K. Stalla, G. Binder, H. G. Doerr, and Berthold P. Hauffa

Subjects

0301 basic medicine, medicine.medical_specialty, Pituitary gland, Organic Growth Hormone Deficiency, business.industry, Central nervous system, Medizin, 030209 endocrinology & metabolism, Septo-optic dysplasia, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, medicine.anatomical_structure, Internal medicine, Pediatrics, Perinatology and Child Health, Mutation (genetic algorithm), medicine, Etiology, Surgery, Maxillary central incisor, business, Rare disease

Published

2020

2. Evolutionary conserved networks of human height identify multiple Mendelian causes of short stature

Author

Christian Thiel, H. G. Doerr, Christian Büttner, Martin Zenker, Christiane Zweier, Perundurai S. Dhandapany, Steffen Uebe, Carina Vogl, Heinrich Sticht, André Reis, Dagmar Wieczorek, Cornelia Kraus, Rami Abou Jamra, Alessandro De Luca, Anna Marie Jung, Leila Taher, Patrizia Klinger, Bernt Popp, Arif B. Ekici, Fulvia Ferrazzi, Anita Rauch, Tilman R. Rohrer, Erdmute Kunstmann, Antje Wiesener, and Nadine N. Hauer

Subjects

Male, Candidate gene, Multifactorial Inheritance, Population, Medizin, Dwarfism, Biology, Short stature, Article, 03 medical and health sciences, symbols.namesake, Exome Sequencing, Genetics, medicine, Humans, Exome, DNA sequencing, Human height, education, Child, Genetics (clinical), Exome sequencing, 0303 health sciences, education.field_of_study, Genetic counselling, Disease genetics, 030305 genetics & heredity, Infant, medicine.disease, Idiopathic short stature, Cytoskeletal Proteins, Child, Preschool, Mendelian inheritance, symbols, Female, medicine.symptom

Abstract

Height is a heritable and highly heterogeneous trait. Short stature affects 3% of the population and in most cases is genetic in origin. After excluding known causes, 67% of affected individuals remain without diagnosis. To identify novel candidate genes for short stature, we performed exome sequencing in 254 unrelated families with short stature of unknown cause and identified variants in 63 candidate genes in 92 (36%) independent families. Based on systematic characterization of variants and functional analysis including expression in chondrocytes, we classified 13 genes as strong candidates. Whereas variants in at least two families were detected for all 13 candidates, two genes had variants in 6 (UBR4) and 8 (LAMA5) families, respectively. To facilitate their characterization, we established a clustered network of 1025 known growth and short stature genes, which yielded 29 significantly enriched clusters, including skeletal system development, appendage development, metabolic processes, and ciliopathy. Eleven of the candidate genes mapped to 21 of these clusters, including CPZ, EDEM3, FBRS, IFT81, KCND1, PLXNA3, RASA3, SLC7A8, UBR4, USP45, and ZFHX3. Fifty additional growth-related candidates we identified await confirmation in other affected families. Our study identifies Mendelian forms of growth retardation as an important component of idiopathic short stature.

Published

2018

3. Height Gain in Ullrich-Turner Syndrome after Early and Late Growth Hormone Treatment Start: Results from a Large Retrospective German Study and Potential Basis for an Individualized Treatment Approach

Author

Otto Mehls, Michael B. Ranke, H. G. Doerr, Berthold P. Hauffa, Markus Bettendorf, and Ioana Inta

Subjects

Pediatrics, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, education, Medizin, MEDLINE, Turner Syndrome, Individualized treatment, Short stature, German, Endocrinology, Medizinische Fakultät, Germany, Internal medicine, Turner syndrome, medicine, Humans, ddc:610, Child, Retrospective Studies, Human Growth Hormone, business.industry, Age Factors, Retrospective cohort study, medicine.disease, Body Height, language.human_language, Clinical trial, Growth hormone treatment, Child, Preschool, Pediatrics, Perinatology and Child Health, language, Female, medicine.symptom, business

Abstract

Background: Ullrich-Turner syndrome (UTS) girls often present with short stature in adolescence to the endocrinologist when the efficacy of growth hormone (GH) to improve growth remains unknown and parameters to estimate individual GH responsiveness have yet to be determined. Objective: Retrospective evaluation of adult height (AH) and predicted adult height at GH start (descriptive model of Ranke, Model PredAH) in early and late GH-treated German UTS patients. Subjects/Methods: 313 patients treated with GH, early [chronological age (CA) at GH start Results: AH (152.5 ± 5.9 vs. 151.1 ± 5.4 cm, p = n.s.) after GH treatment for 7.5 ± 2.12 years (GH start early) and for 5.2 ± 1.2 years (GH start late) were similar (p = n.s.) as Model PredAH (155.7 ± 4.8 vs. 154.7 ± 4.8 cm; p = n.s.) but higher (p < 0.001) than projected adult height (Ranke, ProjAH; 148.2 ± 5.5 vs. 145.2 ± 6.7 cm; p = 0.001). Total height gain over ProjAH was 4.3 ± 4.6 cm (GH start early) and 5.8 ± 4.7 cm (GH start late, p = 0.021), respectively. Conclusions: GH may improve AH in UTS patients even when started late. The individual growth response could be estimated by the descriptive Model PredAH independent of age at treatment start.

Published

2013

4. Transition of young women with Turner syndrome to adult medicine : Current recommendations of an expert workshop

Author

D. Fuehrer, A. P. Athanasoulia, Patricia G. Oppelt, P. Frank-Herrmann, Günter K. Stalla, Berthold P. Hauffa, and H. G. Doerr

Subjects

Gynecology, medicine.medical_specialty, business.industry, Pediatrics, Perinatology and Child Health, medicine, Medizin, Surgery, business

Abstract

Das Ullrich-Turner-Syndrom (UTS) ist eine genetische Erkrankung, die mit einem kompletten oder partiellen Verlust eines X-Chromosoms einhergeht. Kinder oder erwachsene Patientinnen mit UTS leiden haufig unter metabolischen, kardiovaskularen, renalen und gastrointestinalen Komorbiditaten, unter Ostrogenmangelerscheinungen und psychosozialen Problemen. Wahrend der Kindheit werden die Patientinnen traditionell in spezialisierten Kinderkliniken behandelt, aber es fehlt das Konzept fur die weiterfuhrende Therapie in der Transitionsperiode und danach. Zielsetzung dieses Artikels ist es, die wichtigsten publizierten Empfehlungen zur Behandlung von Madchen und Frauen mit UTS mit dem Fokus auf Transition sowie die Ergebnisse eines interdisziplinaren Expertentreffens fur ein strukturiertes Behandlungskonzept zusammenzustellen. Analysiert man die bisherigen Publikationen, lassen sich die Mangel in der Nachsorge der UTS-Frauen auf folgende Punkte reduzieren: fehlende Gesamtkonzepte in der Weiterbetreuung, Unsicherheiten und Uberforderung bei der Betreuung der Frauen mit UTS durch einige Hausarzte, aber auch fehlendes Krankheitsbewusstsein bei einigen Betroffenen. Komorbiditaten bei erwachsenen Patientinnen mit UTS sind vielfaltig und umfassen metabolische, kardiovaskulare, gastrointestinale und renale Erkrankungen, Hormonmangelerscheinungen, gynakologische Aspekte sowie psychosoziale Probleme. Die notwendige Hormonsubstitutionstherapie u. a. mit Ostrogen/Gestagenen erfordert eine Langzeitbetreuung durch erfahrene Spezialisten. Wir empfehlen eine ausfuhrliche Diagnostik zum Zeitpunkt der Transition sowie konsequente 1- bis 5-jahrliche Untersuchungen nach Klinik und Risikoprofil.

Published

2013

5. QUALITY OF LIFE/AFTERCARE

Author

S. Rednam, M. Scheurer, A. Adesina, C. Lau, M. Okcu, J. Deatrick, S. Ogle, M. Fisher, L. Barakat, T. Hardie, Y. Li, J. Ginsberg, M. Ben-Arush, E. Krivoy, R. Rosenkranz, M. Peretz-Nahum, R. J. Brown, J. Love, D. Warburton, W. H. McBride, S. Bluml, S. Mueller, K. Sear, N. Hills, N. Chettout, S. Afghani, L. Lew, E. Tolentino, D. Haas-Kogan, H. Fullerton, W. Reddick, S. Palmer, J. Glass, R. Ogg, A. Gajjar, A. Omar, S. Perkins, E. Shinohara, D. Spoljaric, J. Isenberg, M. Whittington, M. Hauff, A. King, K. Litzelman, E. Barker, K. Catrine, D. Puccetti, P. Possin, W. Witt, C. Mallucci, R. Kumar, B. Pizer, D. Williams, B. Pettorini, J. Piscione, E. Bouffet, I. Shams, A. Kulkarni, T. Remes, A. Harila-Saari, M. Suo-Palosaari, P. Arikoski, P. Riikonen, A. Sutela, P. Koskenkorva, M. Ojaniemi, H. Rantala, C. J. Campen, D. Ashby, P. G. Fisher, M. Monje, A. V. Kulkarni, H. Nakamura, K. Makino, S. Yano, J.-i. Kuratsu, F. Jadrijevic-Cvrlje, M. Batinica, H. Toledano, T. Hoffman, Y. Ezer-Cohen, S. Michowiz, I. Yaniv, I. J. Cohen, I. Adler, S. Mindel, M. Gopalakrishnamoorthy, D. Saunders, M. Gaze, H. Spoudeas, V. Kieffer, G. Dellatolas, M. Chevignard, S. Puget, F. Dhermain, J. Grill, C. Dufour, R. Muir, A. Hunter, A. Latchman, O. de Camargo, K. Scheinemann, N. Dhir, W. Zaky, T. Zomorodian, K. Wong, G. Dhall, M. Macy, C. Lauro, P. Zeitler, N. Foreman, A. Liu, M. Chocholous, P. Dodier, A. Peyrl, K. Dieckmann, G. Hausler, I. Slavc, S. Avula, D. Garlick, G. Armstrong, T. Kawashima, W. Leisenring, M. Stovall, C. Sklar, L. Robison, C. Samaan, J. Duckworth, N. Greenberg-Kushnir, S. Freedman, R. Eshel, N. Zverling, R. Elhasid, R. Dvir, M. Yalon, S. Constantini, S. Wilne, J.-F. Liu, J. Trusler, S. Lundsell, C. Kennedy, L. Clough, N. Dickson, M. Lakhanpaul, M. Baker, J. Dudley, R. Grundy, D. Walker, K. von Hoff, N. Herzog, H. Ottensmeier, D. Grabow, N. U. Gerber, C. Friedrich, A. O. von Bueren, A. Resch, R. D. Kortmann, P. Kaatsch, H. G. Doerr, S. Rutkowski, F. del Bufalo, A. Mastronuzzi, A. Serra, L. de Sio, F. Locatelli, V. Biassoni, M. Leonardi, D. Ajovalasit, D. Riva, C. Vago, A. Usilla, P. Fidani, E. Schiavello, F. Gariboldi, M. Massimino, R. Lober, S. Perrault, S. Partap, M. Edwards, P. Fisher, K. Yeom, D. Salgado, S. Nunes, S. Vinhais, E. M. Wells, K. Seidel, N. J. Ullrich, L. Diller, K. R. Krull, J. Neglia, L. L. Robison, K. Whelan, C. E. Russell, D. Brownstone, C. Kaise, K. Bull, D. Culliford, G. Calaminus, D. Bertin, S. Vallero, E. Romano, M. E. Basso, E. Biasin, F. Fagioli, K. Ziara, A. L'Hotta, A. Williams, R. Thede, K. Moore, A. James, E. Bjorn, P. Franzen, A. Haag, A.-K. Lax, I. Moreno, J. Obeid, B. W. Timmons, W. Iwata, S. Wagner, J.-S. Lai, K. Waddell, S. VanLeeuwen, M. Newmark, J. Noonan, K. O'Connell, M. Urban, S. Yount, S. Goldman, D. Igoe, T. Cunningham, M. Orfus, D. Mabbott, C. Liptak, P. Manley, C. Recklitis, P. Zhang, F. Shaikh, I. Narang, K. Matsumoto, K. Yamasaki, K. Okada, H. Fujisaki, Y. Osugi, J. Hara, K. Phipps, D. Gumley, T. Jacques, D. Hargrave, A. Michalski, C. Chordas, S. Chi, N. Robison, P. Bandopadhayay, K. Marcus, M. A. Zimmerman, L. Goumnerova, M. Kieran, S. Brand, T. Brinkman, B. Delaney, T. Diver, C. Rey, J. R. Madden, M. S. Hemenway, L. Dorneman, D. Stiller, A. K. Liu, N. K. Foreman, R. Vibhakar, M. Mitchell, M. Hemenway, J. Madden, M. Ryan, R. O'Kane, S. Picton, T. Kenny, C. Stiller, P. Chumas, A. Bendel, R. Patterson, M. Barrera, F. Schulte, U. Bartels, L. Janzen, D. Johnston, D. Cataudella, J. Chung, L. Sung, K. Hancock, J. Hukin, S. Zelcer, S. Brandon, I. Montour-Proulx, D. Strother, R. Cooksey, D. Bowers, L. Gargan, A. Gode, L. Klesse, J. Oden, G. Vega, F. Sala, D. Nuzzi, M. Mulino, B. Masotto, C. Mazza, A. Bricolo, M. Gerosa, M. Tong, S. Laughlin, S. Mackie, L. Taylor, G. Sharpe, O. Al-Salihi, and G. Nicolin

Subjects

Oncology, Medulloblastoma, Cancer Research, medicine.medical_specialty, Chemotherapy, business.industry, medicine.medical_treatment, Amifostine, Multimodality Therapy, medicine.disease, Clinical trial, Abstracts, Ototoxicity, Primitive neuroectodermal tumor, Internal medicine, Immunology, medicine, Neurology (clinical), Adverse effect, business, medicine.drug

Abstract

BACKGROUND: Glutathione S-transferase (GST) enzymes are involved in detoxifying chemotherapy agents and clearing reactive oxygen species formed by radiation. In this study, we explored the relationship between the host GSTP1-105 polymorphism (rs1695), tumor GSTpi protein expression, and clinical outcomes in pediatric medulloblastoma. We hypothesized that the GSTP1-105 G-allele and increased tumor GSTpi expression would be associated with lower progression-free survival and fewer adverse events. METHODS: The study included 106 medulloblastoma/primitive neuroectodermal tumor (PNET) patients seen at Texas Children’s Cancer Center. Genotyping was performed using an Illumina HumanOmni1-Quad BeadChip and tumor GSTpi expression was assessed using immunohistochemistry. We used the Kaplan-Meier method for survival analyses and multivariable logistic regression for toxicity comparisons. RESULTS: Patients with a GSTP1-105 AG/GG genotype or who had received a higher dose of craniospinal radiation (median 36 Gy) had a greater risk of requiring hearing aids than their respective counterparts (OR 4.0, 95%CI 1.2 - 13.6, and OR 3.1, 95%CI 1.1 - 8.8, respectively). Additionally, there was a statistically significant interaction between the two variables. Compared with the lowest risk group (GSTP1-105 AA-lower dose radiation) patients with a GSTP1-105 AG/GG genotype who received a higher dose radiation were 8.4 times more likely to require hearing aids (95%CI 1.4 - 49.9, p-trend ¼ 0.005). When adjusted for age, gender, and amifostine use, the association remained. CONCLUSIONS: The GSTP1-105 G-allele is associated with permanent ototoxicity in pediatric medulloblastoma/PNET and strongly interacts with radiation dose. A possible mechanism for this finding is that the GSTP1-105 G-allele leads to reduced GSTpi free radical detoxification in the setting of multimodality therapy including cisplatin and radiation. Patients with this allele should be considered for clinical trials employing radiation dose modifications and more targeted cytoprotectant strategies than are currently being used with amifostine.

Published

2012

6. Impact of Overweight on Effectiveness of Treatment with Human Growth Hormone in Growth Hormone Deficient Children: Analysis of German KIGS Data

Author

Thomas Reinehr, Bettina Gohlke, Karl Otfried Schwab, Stefan Kaspers, H. G. Doerr, C. Land, Nikolaus Stahnke, Otto Mehls, Markus Bettendorf, S. Bechtold-Dalla Pozza, Berthold P. Hauffa, Michael B. Ranke, and German KIGS Study Board (Beitragende*r)

Subjects

Male, Pediatrics, medicine.medical_specialty, Hormone Replacement Therapy, Endocrinology, Diabetes and Metabolism, Medizin, Overweight, Models, Biological, Group B, Growth hormone deficiency, Body Mass Index, Endocrinology, Child Development, Thinness, Internal medicine, Germany, Internal Medicine, medicine, Humans, Obesity, Registries, Insulin-Like Growth Factor I, Child, Retrospective Studies, business.industry, Human Growth Hormone, Age Factors, General Medicine, medicine.disease, Body Height, Recombinant Proteins, Growth hormone treatment, Transgender hormone therapy, Child, Preschool, Cohort, Female, medicine.symptom, Underweight, business

Abstract

We hypothesized that overweight children with growth hormone deficiency (GHD) demonstrate a lower response to growth hormone (GH) as a result of a misclassification since obesity is associated with lower GH peaks in stimulation tests.Anthropometric data, response, and responsiveness to GH in the first year of treatment were compared in 1.712 prepubertal children with GHD from the German KIGS database according to BMI (underweight=group A, normal weight=group B, overweight=group C) (median age: group A, B, C: 7.3, 7.28, and 8.4 years).Maximum GH levels to tests (median: group A, B, C: 5.8, 5.8, and 4.0 µg/ml) were significantly lower in group C. IGF-I SDS levels were not different between the groups. Growth velocity in the first year of GH treatment was significantly lower in the underweight cohort (median: group A, B, C: 8.2, 8.8, and 9.0 cm/yr), while the gain in height was not different between groups. The difference between observed and predicted growth velocity expressed as Studentized residuals was not significantly different between groups. Separating the 164 overweight children into obese children (BMI>97th centile; n=71) and moderate overweight children (BMI>90th to 97th centile, n=93) demonstrated no significant difference in any parameter.Overweight prepubertal children with idiopathic GHD demonstrated similar levels of responsiveness to GH treatment compared to normal weight children. Furthermore, the IGF-I levels were low in overweight children. Therefore, a misclassification of GHD in overweight prepubertal children within the KIGS database seems unlikely. The first year growth prediction models can be applied to overweight and obese GHD children.

Published

2011

7. Effects of dehydroepiandrosterone therapy on pubic hair growth and psychological well-being in adolescent girls and young women with central adrenal insufficiency: a double-blind, randomized, placebo-controlled phase III trial

Author

M. Ehrismann, M.B. Ranke, Gerhard Binder, Michaela F. Hartmann, Markus Bettendorf, L. Maier, Stefan A. Wudy, Udo Heinrich, S. Weber, C. Meisner, Eberhard Keller, H. G. Doerr, N. Zaiser, and R. W. Pfaeffle

Subjects

Adult, medicine.medical_specialty, Adolescent, Hydrocortisone, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Dehydroepiandrosterone, Context (language use), Blood Pressure, Central adrenal insufficiency, Placebo, Biochemistry, Hypopituitarism, law.invention, Young Adult, Endocrinology, Randomized controlled trial, Adrenocorticotropic Hormone, Double-Blind Method, law, Internal medicine, medicine, Adrenal insufficiency, Humans, Obesity, Young adult, business.industry, Brain Neoplasms, Biochemistry (medical), medicine.disease, Pubic hair, medicine.anatomical_structure, Female, business, Adrenal Insufficiency, Hair

Abstract

The efficacy of oral dehydroepiandrosterone (DHEA) in the treatment of atrichia pubis and psychological distress in young females with central adrenal insufficiency is unknown. Our study aimed to evaluate this therapy.A total of 23 young females (mean age 18 yr, range 13-25) was enrolled in a double-blind randomized placebo-controlled trial. Inclusion criteria were ACTH deficiency plus two or more additional pituitary deficiencies, serum DHEA less than 400 ng/ml, and pubertal stage more than B2. Exclusion criteria were cerebral radiation with more than 30 Gy, tumor remission less than 1 yr, amaurosis, hypothalamic obesity, psychiatric disorders, and unstable hormone medication.Patients were randomized to placebo (n = 12) or 25 mg HPLC-purified DHEA/d (n = 11) orally for 12 months after stratification into a nontumor (n = 7) and a tumor group (n = 16).Clinical scoring of pubic hair stage was performed at 0, 6, and 12 months (primary endpoint), and psychometrical evaluation (Symptom Check-List-90-R and the Centre for Epidemiological Studies-Depression Scale) at 0 and 12 months (secondary endpoint). Androgen levels and safety parameters were measured at 0, 6, and 12 months; 24-h androgen urinary excretion rates were calculated at 0 and 12 months.In the placebo group, four patients dropped out because of recurrence of craniopharyngioma, manifestation of type 1 diabetes, and change of residence (n = 2); in the DHEA group, one patient dropped out because of recurrent anxiety attacks. DHEA substitution resulted in normalization of DHEA sulfate and androstanediol glucuronide morning serum levels 2 h after drug intake (P0.006), and of its 24 h urinary metabolite levels (P0.0001), placebo had no effect. Morning serum levels of androstenedione increased in the DHEA group (P0.02) but did not normalize. The DHEA group exhibited significant progress in pubic hair growth from Tanner stage I-III to II-V (mean: +1.5 stages), whereas the placebo group did not (relative risk 0.138; 95% confidence interval 0.021-0.914; P = 0.0046). Importantly, eight of the 10 Symptom Check-List-90-R scores, including those for depression, anxiety, and interpersonal sensitivity, and the global severity index improved in the DHEA group in comparison to the placebo group (P0.048). DHEA was well tolerated.In adolescent girls with central adrenal insufficiency, daily replacement with 25 mg DHEA orally is beneficial: atrichia pubis vanishes, and psychological well-being improves significantly.

Published

2009

8. Is the response to growth hormone in short children born small for gestational age dependent on genetic or maternal factors?

Author

Markus Bettendorf, Tilman R. Rohrer, H. G. Doerr, Otto Mehls, Berthold P. Hauffa, N. Stahnke, Stefan Kaspers, M.B. Ranke, and Anders Lindberg

Subjects

Heart Defects, Congenital, Male, Pediatrics, medicine.medical_specialty, Medizinische Fakultät -ohne weitere Spezifikation, Endocrinology, Diabetes and Metabolism, Growth hormone, Infections, Endocrinology, Child Development, Environmental risk, Pregnancy, Risk Factors, medicine, Humans, ddc:610, Child, Retrospective Studies, business.industry, Human Growth Hormone, Silver–Russell syndrome, Smoking, Infant, Newborn, Retrospective cohort study, medicine.disease, Child development, Body Height, Growth hormone treatment, Child, Preschool, Pediatrics, Perinatology and Child Health, Infant, Small for Gestational Age, Small for gestational age, Female, business

Abstract

Background/Aims: We investigated whether genetic or maternal/environmental risk factors for being born small for gestational age (SGA), e.g. Silver-Russell syndrome, congenital heart defects, infections of mothers or smoking during pregnancy, explain the variation in the first-year growth response to GH therapy. Methods: Secondary analysis was made of growth response in 135 short prepubertal German children (66% males) enrolled in a SGA phase III trial. Initial mean patient age was 6.8 ± 2.6 years; mean patient height SDS –3.8 ± 1.2, and GH treatment dose was 0.066 mg/kg body weight per day. Results: Growth velocity increased by 4.5 ± 2.0 cm/year and height SDS by 1.0 ± 0.5 SDS. Although patient number was limited and variation was high, both growth response (cm/year) and change in height SDS did not appear to differ between subgroups which also did not differ in terms of Studentized residuals set up in the KIGS growth prediction model for SGA. Likewise, in a step-forward multivariate analysis, the variables Silver-Russell syndrome, congenital heart defects, infections of mothers and smoking were not identified as independent factors influencing growth velocity. Conclusion: The retrospectively analyzed genetic and maternal/environmental risk factors for SGA do not appear to explain the observed patient variance in response to GH. Larger prospective studies are needed, however, to substantiate these preliminary findings.

Published

2008

9. Reduzierte Genexpression der beiden Cortisol metabolisierenden Enzyme 11ß-Hydroxysteroiddehydrogenase Typ 1 und Typ 2 in Plazenten von hypotrophen Neugeborenen

Author

M. W. Beckmann, Ellen Struwe, W. Rascher, Jörg Dötsch, H. G. Doerr, Ralf L. Schild, and G. Berzl

Subjects

Maternity and Midwifery, Obstetrics and Gynecology

Published

2006

10. V-C-U-A-M-Klassifiktion (Vagina-Cervix-Uterus-Adnex-associated Malformation)–Eine neue Klassifikation weiblicher genitaler Fehlbildungen

Author

Patricia G. Oppelt, P. G. Oppelt, Sara Y. Brucker, D. Wallwiener, Stefan P. Renner, M. W. Beckmann, H. G. Doerr, Reiner Strick, G. E. Schott, J. Hucke, and Pamela L. Strissel

Subjects

Maternity and Midwifery, Obstetrics and Gynecology

Published

2006

11. Uterine size in women with Turner syndrome after induction of puberty with estrogens and long-term growth hormone therapy: results of the German IGLU Follow-up Study 2001

Author

Elfriede Said, Sabine Sander, Otto Mehls, Hans-Peter Schwarz, Markus Bettendorf, Berthold P. Hauffa, Carl-Joachim Partsch, Michael B. Ranke, H. G. Doerr, Nikolaus Stahnke, and Heiner Steinkamp

Subjects

Adult, medicine.medical_specialty, Gonad, Adolescent, medicine.drug_class, medicine.medical_treatment, Uterus, Turner Syndrome, Biology, Reference Values, Turner syndrome, medicine, Humans, Ultrasonography, Gynecology, Breast development, Human Growth Hormone, Rehabilitation, Puberty, Obstetrics and Gynecology, Karyotype, Organ Size, medicine.disease, medicine.anatomical_structure, Cross-Sectional Studies, Reproductive Medicine, In utero, Estrogen, Karyotyping, Female, Hormone therapy, Follow-Up Studies

Abstract

BACKGROUND: To evaluate the factors influencing uterine size in young adult women with Turner syndrome (TS) after long-term growth hormone (GH) treatment. METHODS: Cross-sectional study. Out of 188 women with TS from 96 German centres, whose longitudinal growth was documented within KIGS (Pfizer International Growth Database), data on uterine size were collected voluntarily at a standardized follow-up visit: 75 TS women (ages: 15.8-30.8 years) with complete data were included. Classification according to karyotype: 45,X (78.6%), 45,X/46,XX (5.4%), 45,X/46,iXq (8%), 45,X/46,XY (8%). Puberty was induced with estrogens in all women. At follow-up, 66 were on cyclic estrogens and progestins. RESULTS: 13/66 (19.6%) TS women who received estrogens had a reduced uterine length

Published

2005

12. Different therapeutic efficacy of ketoconazole in patients with Cushing's syndrome

Author

D. Engelhardt, K. Jacob, and H. G. Doerr

Subjects

Adenoma, Adult, Male, endocrine system, medicine.medical_specialty, Hydrocortisone, Endocrinology, Diabetes and Metabolism, Urinary system, Disease, Dexamethasone, Adrenocortical adenoma, Endocrinology, Adrenocorticotropic Hormone, Internal medicine, Drug Discovery, medicine, Humans, Adrenocortical carcinoma, In patient, Cushing Syndrome, Genetics (clinical), S syndrome, business.industry, General Medicine, medicine.disease, Molecular medicine, Adrenal Cortex Neoplasms, ACTH Syndrome, Ectopic, Ketoconazole, Molecular Medicine, Female, business, Serum cortisol, hormones, hormone substitutes, and hormone antagonists, Follow-Up Studies, medicine.drug

Abstract

The property of ketoconazole to inhibit adrenal biosynthesis of cortisol was used in a clinical study of 14 patients with Cushing's syndrome (pituitary-dependent Cushing's disease,n=10; adrenocortical adenoma,n=2; adrenocortical carcinoma,n=1; ectopic ACTH syndrome,n=1). Five patients were treated in a short-term manner (1000 mg over 24 h) and nine patients for a longer period (600 mg/die from 1 week up to 12 months). After short-term administration of ketoconazole, serum cortisol levels fell distinctly only in the patient with adrenocortical adenoma, but not at all or only slightly in the other patients, whereas serum levels of progesterone and 11-deoxy-compounds increased markedly in all patients, with the exception of the patient with adrenocortical carcinoma. Plasma ACTH levels increased in the patients with Cushing's disease but not in the patients with tumor. After long-term treatment of three patients with Cushing's disease over 3, 10, and 12 months, the clinical signs of hypercortisolism persisted or were only slightly ameliorated. In these three patients as well as in three other patients with Cushing's disease treated for a shorter period of 1 to 4 weeks, serum and urinary cortisol levels decreased, but were not normalized, whereas plasma ACTH levels increased variably. Only in one patient with Cushing's disease, in the second patient with adrenocortical adenoma, and in the patient with ectopic ACTH syndrome, serum and urinary cortisol levels returned to normal. We concluded from our data, that the antimycotic drug inhibits biosynthesis of cortisol by blocking adrenal 11β- and 17α-hydroxylase activity. This effect was compensated in part by a rebound increase of pituitary ACTH secretion in most patients with Cushing's disease. Therefore, ketoconazole treatment is above all effective in patients with Cushing's syndrome due to an adrenal tumor or in patients with ectopic ACTH syndrome, who cannot respond with an increased pituitary ACTH secretion.

Published

1989