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2. Human MAMLD1 Gene Variations Seem Not Sufficient to Explain a 46,XY DSD Phenotype.

Author

Núria Camats, Mónica Fernández-Cancio, Laura Audí, Primus E Mullis, Francisca Moreno, Isabel González Casado, Juan Pedro López-Siguero, Raquel Corripio, José Antonio Bermúdez de la Vega, José Antonio Blanco, and Christa E Flück

Subjects
Medicine, Science
Abstract

MAMLD1 is thought to cause disordered sex development in 46,XY patients. But its role is controversial because some MAMLD1 variants are also detected in normal individuals, several MAMLD1 mutations have wild-type activity in functional tests, and the male Mamld1-knockout mouse has normal genitalia and reproduction. Our aim was to search for MAMLD1 variations in 108 46,XY patients with disordered sex development, and to test them functionally. We detected MAMDL1 variations and compared SNP frequencies in controls and patients. We tested MAMLD1 transcriptional activity on promoters involved in sex development and assessed the effect of MAMLD1 on androgen production. MAMLD1 expression in normal steroid-producing tissues and mutant MAMLD1 protein expression were also assessed. Nine MAMLD1 mutations (7 novel) were characterized. In vitro, most MAMLD1 variants acted similarly to wild type. Only the L210X mutation showed loss of function in all tests. We detected no effect of wild-type or MAMLD1 variants on CYP17A1 enzyme activity in our cell experiments, and Western blots revealed no significant differences for MAMLD1 protein expression. MAMLD1 was expressed in human adult testes and adrenals. In conclusion, our data support the notion that MAMLD1 sequence variations may not suffice to explain the phenotype in carriers and that MAMLD1 may also have a role in adult life.

Published
2015
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3. Butyrate increases intracellular calcium levels and enhances growth hormone release from rat anterior pituitary cells via the G-protein-coupled receptors GPR41 and 43.

Author

Maria Consolata Miletta, Vibor Petkovic, Andrée Eblé, Roland A Ammann, Christa E Flück, and Primus-E Mullis

Subjects
Medicine, Science
Abstract

Butyrate is a short-chain fatty acid (SCFA) closely related to the ketone body ß-hydroxybutyrate (BHB), which is considered to be the major energy substrate during prolonged exercise or starvation. During fasting, serum growth hormone (GH) rises concomitantly with the accumulation of BHB and butyrate. Interactions between GH, ketone bodies and SCFA during the metabolic adaptation to fasting have been poorly investigated to date. In this study, we examined the effect of butyrate, an endogenous agonist for the two G-protein-coupled receptors (GPCR), GPR41 and 43, on non-stimulated and GH-releasing hormone (GHRH)-stimulated hGH secretion. Furthermore, we investigated the potential role of GPR41 and 43 on the generation of butyrate-induced intracellular Ca2+ signal and its ultimate impact on hGH secretion. To study this, wt-hGH was transfected into a rat pituitary tumour cell line stably expressing the human GHRH receptor. Treatment with butyrate promoted hGH synthesis and improved basal and GHRH-induced hGH-secretion. By acting through GPR41 and 43, butyrate enhanced intracellular free cytosolic Ca2+. Gene-specific silencing of these receptors led to a partial inhibition of the butyrate-induced intracellular Ca2+ rise resulting in a decrease of hGH secretion. This study suggests that butyrate is a metabolic intermediary, which contributes to the secretion and, therefore, to the metabolic actions of GH during fasting.

Published
2014
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4. Estimation of HIV incidence in a large, community-based, randomized clinical trial: NIMH project accept (HIV Prevention Trials Network 043).

Author

Oliver Laeyendecker, Estelle Piwowar-Manning, Agnes Fiamma, Michal Kulich, Deborah Donnell, Deb Bassuk, Caroline E Mullis, Craig Chin, Priscilla Swanson, John Hackett, William Clarke, Mark Marzinke, Greg Szekeres, Glenda Gray, Linda Richter, Michel W Alexandre, Suwat Chariyalertsak, Alfred Chingono, David D Celentano, Stephen F Morin, Michael Sweat, Thomas Coates, and Susan H Eshleman

Subjects
Medicine, Science
Abstract

BackgroundNational Institute of Mental Health Project Accept (HIV Prevention Trials Network [HPTN] 043) is a large, Phase III, community-randomized, HIV prevention trial conducted in 48 matched communities in Africa and Thailand. The study intervention included enhanced community-based voluntary counseling and testing. The primary endpoint was HIV incidence, assessed in a single, cross-sectional, post-intervention survey of >50,000 participants.MethodsHIV rapid tests were performed in-country. HIV status was confirmed at a central laboratory in the United States. HIV incidence was estimated using a multi-assay algorithm (MAA) that included the BED capture immunoassay, an avidity assay, CD4 cell count, and HIV viral load.ResultsData from Thailand was not used in the endpoint analysis because HIV prevalence was low. Overall, 7,361 HIV infections were identified (4 acute, 3 early, and 7,354 established infections). Samples from established infections were analyzed using the MAA; 467 MAA positive samples were identified; 29 of those samples were excluded because they contained antiretroviral drugs. HIV prevalence was 16.5% (range at study sites: 5.93% to 30.8%). HIV incidence was 1.60% (range at study sites: 0.78% to 3.90%).ConclusionsIn this community-randomized trial, a MAA was used to estimate HIV incidence in a single, cross-sectional post-intervention survey. Results from this analysis were subsequently used to compare HIV incidence in the control and intervention communities.Trial registrationClinicalTrials.gov NCT00203749.

Published
2013
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5. Development of methods for cross-sectional HIV incidence estimation in a large, community randomized trial.

Author

Oliver Laeyendecker, Michal Kulich, Deborah Donnell, Arnošt Komárek, Marek Omelka, Caroline E Mullis, Greg Szekeres, Estelle Piwowar-Manning, Agnes Fiamma, Ronald H Gray, Tom Lutalo, Charles S Morrison, Robert A Salata, Tsungai Chipato, Connie Celum, Erin M Kahle, Taha E Taha, Newton I Kumwenda, Quarraisha Abdool Karim, Vivek Naranbhai, Jairam R Lingappa, Michael D Sweat, Thomas Coates, and Susan H Eshleman

Subjects
Medicine, Science
Abstract

BackgroundAccurate methods of HIV incidence determination are critically needed to monitor the epidemic and determine the population level impact of prevention trials. One such trial, Project Accept, a Phase III, community-randomized trial, evaluated the impact of enhanced, community-based voluntary counseling and testing on population-level HIV incidence. The primary endpoint of the trial was based on a single, cross-sectional, post-intervention HIV incidence assessment.Methods and findingsTest performance of HIV incidence determination was evaluated for 403 multi-assay algorithms [MAAs] that included the BED capture immunoassay [BED-CEIA] alone, an avidity assay alone, and combinations of these assays at different cutoff values with and without CD4 and viral load testing on samples from seven African cohorts (5,325 samples from 3,436 individuals with known duration of HIV infection [1 month to >10 years]). The mean window period (average time individuals appear positive for a given algorithm) and performance in estimating an incidence estimate (in terms of bias and variance) of these MAAs were evaluated in three simulated epidemic scenarios (stable, emerging and waning). The power of different test methods to detect a 35% reduction in incidence in the matched communities of Project Accept was also assessed. A MAA was identified that included BED-CEIA, the avidity assay, CD4 cell count, and viral load that had a window period of 259 days, accurately estimated HIV incidence in all three epidemic settings and provided sufficient power to detect an intervention effect in Project Accept.ConclusionsIn a Southern African setting, HIV incidence estimates and intervention effects can be accurately estimated from cross-sectional surveys using a MAA. The improved accuracy in cross-sectional incidence testing that a MAA provides is a powerful tool for HIV surveillance and program evaluation.

Published
2013
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6. Transient Neonatal Zinc Deficiency Caused by a Heterozygous G87R Mutation in the Zinc Transporter ZnT-2 (SLC30A2) Gene in the Mother Highlighting the Importance of Zn2+ for Normal Growth and Development

Author

Maria Consolata Miletta, Andreas Bieri, Kristin Kernland, Martin H. Schöni, Vibor Petkovic, Christa E. Flück, Andrée Eblé, and Primus E. Mullis

Subjects
Diseases of the endocrine glands. Clinical endocrinology, RC648-665
Abstract

Suboptimal dietary zinc (Zn2+) intake is increasingly appreciated as an important public health issue. Zn2+ is an essential mineral, and infants are particularly vulnerable to Zn2+ deficiency, as they require large amounts of Zn2+ for their normal growth and development. Although term infants are born with an important hepatic Zn2+ storage, adequate Zn2+ nutrition of infants mostly depends on breast milk or formula feeding, which contains an adequate amount of Zn2+ to meet the infants’ requirements. An exclusively breast-fed 6 months old infant suffering from Zn2+ deficiency caused by an autosomal dominant negative G87R mutation in the Slc30a2 gene (encoding for the zinc transporter 2 (ZnT-2)) in the mother is reported. More than 20 zinc transporters characterized up to date, classified into two families (Slc30a/ZnT and Slc39a/Zip), reflect the complexity and importance of maintaining cellular Zn2+ homeostasis and dynamics. The role of ZnTs is to reduce intracellular Zn2+ by transporting it from the cytoplasm into various intracellular organelles and by moving Zn2+ into extracellular space. Zips increase intracellular Zn2+ by transporting it in the opposite direction. Thus the coordinated action of both is essential for the maintenance of Zn2+ homeostasis in the cytoplasm, and accumulating evidence suggests that this is also true for the secretory pathway of growth hormone.

Published
2013
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7. Antibody maturation and viral diversification in HIV-infected women.

Author

Maria M James, Oliver Laeyendecker, Jin Sun, Donald R Hoover, Caroline E Mullis, Matthew M Cousins, Thomas Coates, Richard D Moore, Gabor D Kelen, Mary Glenn Fowler, Johnstone J Kumwenda, Lynne M Mofenson, Newton I Kumwenda, Taha E Taha, and Susan H Eshleman

Subjects
Medicine, Science
Abstract

The Post-exposure Prophylaxis in Infants (PEPI)-Malawi trial evaluated infant antiretroviral regimens for prevention of post-natal HIV transmission. A multi-assay algorithm (MAA) that includes the BED capture immunoassay, an avidity assay, CD4 cell count, and viral load was used to identify women who were vs. were not recently infected at the time of enrollment (MAA recent, N = 73; MAA non-recent, N = 2,488); a subset of the women in the MAA non-recent group known to have been HIV infected for at least 2 years before enrollment (known non-recent, N = 54). Antibody maturation and viral diversification were examined in these women.Samples collected at enrollment (N = 2,561) and 12-24 months later (N = 1,306) were available for serologic analysis using the BED and avidity assays. A subset of those samples was used for analysis of viral diversity, which was performed using a high resolution melting (HRM) diversity assay. Viral diversity analysis was performed using all available samples from women in the MAA recent group (61 enrollment samples, 38 follow-up samples) and the known non-recent group (43 enrollment samples, 22 follow-up samples). Diversity data from PEPI-Malawi were also compared to similar data from 169 adults in the United States (US) with known recent infection (N = 102) and known non-recent infection (N = 67).In PEPI-Malawi, results from the BED and avidity assays increased over time in the MAA recent group, but did not change significantly in the MAA non-recent group. At enrollment, HIV diversity was lower in the MAA recent group than in the known non-recent group. HRM diversity assay results from women in PEPI-Malawi were similar to those from adults in the US with known duration of HIV infection.Antibody maturation and HIV diversification patterns in African women provide additional support for use of the MAA to identify populations with recent HIV infection.

Published
2013
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8. Differential regulation of human 3β-hydroxysteroid dehydrogenase type 2 for steroid hormone biosynthesis by starvation and cyclic AMP stimulation: studies in the human adrenal NCI-H295R cell model.

Author

Sameer Udhane, Petra Kempna, Gaby Hofer, Primus E Mullis, and Christa E Flück

Subjects
Medicine, Science
Abstract

Human steroid biosynthesis depends on a specifically regulated cascade of enzymes including 3β-hydroxysteroid dehydrogenases (HSD3Bs). Type 2 HSD3B catalyzes the conversion of pregnenolone, 17α-hydroxypregnenolone and dehydroepiandrosterone to progesterone, 17α-hydroxyprogesterone and androstenedione in the human adrenal cortex and the gonads but the exact regulation of this enzyme is unknown. Therefore, specific downregulation of HSD3B2 at adrenarche around age 6-8 years and characteristic upregulation of HSD3B2 in the ovaries of women suffering from the polycystic ovary syndrome remain unexplained prompting us to study the regulation of HSD3B2 in adrenal NCI-H295R cells. Our studies confirm that the HSD3B2 promoter is regulated by transcription factors GATA, Nur77 and SF1/LRH1 in concert and that the NBRE/Nur77 site is crucial for hormonal stimulation with cAMP. In fact, these three transcription factors together were able to transactivate the HSD3B2 promoter in placental JEG3 cells which normally do not express HSD3B2. By contrast, epigenetic mechanisms such as methylation and acetylation seem not involved in controlling HSD3B2 expression. Cyclic AMP was found to exert differential effects on HSD3B2 when comparing short (acute) versus long-term (chronic) stimulation. Short cAMP stimulation inhibited HSD3B2 activity directly possibly due to regulation at co-factor or substrate level or posttranslational modification of the protein. Long cAMP stimulation attenuated HSD3B2 inhibition and increased HSD3B2 expression through transcriptional regulation. Although PKA and MAPK pathways are obvious candidates for possibly transmitting the cAMP signal to HSD3B2, our studies using PKA and MEK1/2 inhibitors revealed no such downstream signaling of cAMP. However, both signaling pathways were clearly regulating HSD3B2 expression.

Published
2013
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9. Effect of natural and ARV-induced viral suppression and viral breakthrough on anti-HIV antibody proportion and avidity in patients with HIV-1 subtype B infection.

Author

Sarah K Wendel, Caroline E Mullis, Susan H Eshleman, Joel N Blankson, Richard D Moore, Jeanne C Keruly, Ron Brookmeyer, Thomas C Quinn, and Oliver Laeyendecker

Subjects
Medicine, Science
Abstract

Viral suppression and viral breakthrough impact the humoral immune response to HIV infection. We evaluated the impact of viral suppression and viral breakthrough on results obtained with two cross-sectional HIV incidence assays.All samples were collected from adults in the US who were HIV infected for >2 years. Samples were tested with the BED capture enzyme immunoassay (BED-CEIA) which measures the proportion of IgG that is HIV-specific, and with an antibody avidity assay based on the Genetic Systems 1/2+ O ELISA. We tested 281 samples: (1) 30 samples from 18 patients with natural control of HIV-1 infection known as elite controllers or suppressors (2) 72 samples from 18 adults on antiretroviral therapy (ART), with 1 sample before and 2-6 samples after ART initiation, and (3) 179 samples from 20 virally-suppressed adults who had evidence of viral breakthrough receiving ART (>400 copies/ml HIV RNA) and with subsequent viral suppression.For elite suppressors, 10/18 had BED-CEIA values

Published
2013
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10. Role of AMP-activated protein kinase on steroid hormone biosynthesis in adrenal NCI-H295R cells.

Author

Andrea Hirsch, Dagmar Hahn, Petra Kempná, Gaby Hofer, Primus E Mullis, Jean-Marc Nuoffer, and Christa E Flück

Subjects
Medicine, Science
Abstract

Regulation of human androgen biosynthesis is poorly understood. However, detailed knowledge is needed to eventually solve disorders with androgen dysbalance. We showed that starvation growth conditions shift steroidogenesis of human adrenal NCI-H295R cells towards androgen production attributable to decreased HSD3B2 expression and activity and increased CYP17A1 phosphorylation and 17,20-lyase activity. Generally, starvation induces stress and energy deprivation that need to be counteracted to maintain proper cell functions. AMP-activated protein kinase (AMPK) is a master energy sensor that regulates cellular energy balance. AMPK regulates steroidogenesis in the gonad. Therefore, we investigated whether AMPK is also a regulator of adrenal steroidogenesis. We hypothesized that starvation uses AMPK signaling to enhance androgen production in NCI-H295R cells. We found that AMPK subunits are expressed in NCI-H295 cells, normal adrenal tissue and human as well as pig ovary cells. Starvation growth conditions decreased phosphorylation, but not activity of AMPK in NCI-H295 cells. In contrast, the AMPK activator 5-aminoimidazole-4-carboxamide (AICAR) increased AMPKα phosphorylation and increased CYP17A1-17,20 lyase activity. Compound C (an AMPK inhibitor), directly inhibited CYP17A1 activities and can therefore not be used for AMPK signaling studies in steroidogenesis. HSD3B2 activity was neither altered by AICAR nor compound C. Starvation did not affect mitochondrial respiratory chain function in NCI-H295R cells suggesting that there is no indirect energy effect on AMPK through this avenue. In summary, starvation-mediated increase of androgen production in NCI-H295 cells does not seem to be mediated by AMPK signaling. But AMPK activation can enhance androgen production through a specific increase in CYP17A1-17,20 lyase activity.

Published
2012
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11. Characterization of novel StAR (steroidogenic acute regulatory protein) mutations causing non-classic lipoid adrenal hyperplasia.

Author

Christa E Flück, Amit V Pandey, Bernhard Dick, Núria Camats, Mónica Fernández-Cancio, María Clemente, Miquel Gussinyé, Antonio Carrascosa, Primus E Mullis, and Laura Audi

Subjects
Medicine, Science
Abstract

CONTEXT: Steroidogenic acute regulatory protein (StAR) is crucial for transport of cholesterol to mitochondria where biosynthesis of steroids is initiated. Loss of StAR function causes lipoid congenital adrenal hyperplasia (LCAH). OBJECTIVE: StAR gene mutations causing partial loss of function manifest atypical and may be mistaken as familial glucocorticoid deficiency. Only a few mutations have been reported. DESIGN: To report clinical, biochemical, genetic, protein structure and functional data on two novel StAR mutations, and to compare them with published literature. SETTING: Collaboration between the University Children's Hospital Bern, Switzerland, and the CIBERER, Hospital Vall d'Hebron, Autonomous University, Barcelona, Spain. PATIENTS: Two subjects of a non-consanguineous Caucasian family were studied. The 46,XX phenotypic normal female was diagnosed with adrenal insufficiency at the age of 10 months, had normal pubertal development and still has no signs of hypergonodatropic hypogonadism at 32 years of age. Her 46,XY brother was born with normal male external genitalia and was diagnosed with adrenal insufficiency at 14 months. Puberty was normal and no signs of hypergonadotropic hypogonadism are present at 29 years of age. RESULTS: StAR gene analysis revealed two novel compound heterozygote mutations T44HfsX3 and G221S. T44HfsX3 is a loss-of-function StAR mutation. G221S retains partial activity (∼30%) and is therefore responsible for a milder, non-classic phenotype. G221S is located in the cholesterol binding pocket and seems to alter binding/release of cholesterol. CONCLUSIONS: StAR mutations located in the cholesterol binding pocket (V187M, R188C, R192C, G221D/S) seem to cause non-classic lipoid CAH. Accuracy of genotype-phenotype prediction by in vitro testing may vary with the assays employed.

Published
2011
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12. Störungen der Kalziumhomöostase im Kindesalter – wann muss man daran denken?

Author

M. Janner and P. E. Mullis

Subjects
Calcium metabolism, medicine.medical_specialty, business.industry, Plasma calcium, chemistry.chemical_element, General Medicine, Calcium, Plasma calcium level, Endocrinology, chemistry, Internal medicine, Extracellular fluid, medicine, Bone formation, business
Abstract

Abnormalities of the calcium homeostasis are, with exception of the neonatal period, not often to diagnose in childhood. However, as the clinical features may not only be quite heterogeneous but also present with a very changing pattern, abnormalities of calcium homeostasis have to be considered in many differential diagnoses. Extracellular fluid calcium or plasma calcium is very carefully controlled by fluxes of calcium, which occur between the extracellular fluid and the skeleton, as well as between gut and the kidneys. Therefore, in this review, first, the factors physiologically regulating calcium homeostasis and bone formation are summarized; and then, the situations in which the plasma calcium level should be measured in daily clinical practices are discussed.

Published
2007

13. Effect of Growth Hormone and Oxandrolone Treatment on Glucose Metabolism in Turner Syndrome

Author

O. Tönz, P. E. Mullis, E. E. Joss, and R. P. Zurbrügg

Subjects
medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, Human growth hormone, Oxandrolone, Carbohydrate metabolism, medicine.disease, Growth hormone, law.invention, Endocrinology, law, Internal medicine, Pediatrics, Perinatology and Child Health, Turner syndrome, medicine, Recombinant DNA, business, medicine.drug
Abstract

In 18 girls with Turner syndrome, glucose tolerance was studied before treatment and after 6 and 24 months of growth-promoting treatment with recombinant human growth hormone (24 IU/m2/week; 8 mg/m2/week) and oxandrolone (0.06 mg/kg/day), as well as after termination of the treatment. One girl developed an overt non-ketotic diabetes mellitus 50 months after termination of treatment. The results of the remaining 17 girls in whom the effect of treatment on glucose metabolism was reversible are presented as a group. Their median age at the beginning of the treatment was 10.4 years (range 6.9–15.9), and 15.0 years (range 12.1–19.9) at the final assessment. There was a moderate, but not significant rise in fasting glucose throughout the course of the longitudinal study. At oral glucose tolerance testing (oGTT), the area under the curve for glucose rose significantly (p = 0.013) during the period of treatment and returned to the basic value thereafter. Fasting insulin and especially the integrated insulin values (AUCi; area under the curve for insulin) during oGTT increased continuously during treatment, declined after termination of treatment but were still significantly (p = 0.04) higher than before treatment. Considering the fact that in untreated girls with Turner syndrome the fasting insulin and the AUCi increase with age, one can conclude that the insulinaemia returned to age-specific norm after termination of treatment. Thus the effect of a combined growth hormone and oxandrolone growth-promoting treatment on glucose metabolism was fully reversible in these 17 girls with Turner syndrome.

Published
2000

15. Impact of different doses of ethinyl oestradiol on reduction of final height in constitutionally tall girls

Author

J. Zeuner, P. E. Mullis, R. P. Zurbrügg, and E. E. Joss

Subjects
medicine.medical_specialty, Ethinyl oestradiol, Adolescent, Dose-Response Relationship, Drug, Dose, business.industry, Untreated group, Final height, Tall Stature, Bone age, Ethinyl Estradiol, Body Height, Endocrinology, Age Determination by Skeleton, Internal medicine, Ethinylestradiol, Pediatrics, Perinatology and Child Health, medicine, Humans, Female, Child, Inverse correlation, business, medicine.drug
Abstract

Fifty-two tall girls were treated for constitutionally tall stature with different ethinyl oestradiol (EE) dosages. They were divided into three different treatment groups: group B (100 micrograms EE/day; n = 11); group C (300 micrograms; n = 25) and group D (500 micrograms; n = 16) and compared with an untreated group A (n = 21) matched for age, height, bone age (BA) and height prediction. Using the height prediction method TW II, EE treatment reduced final height compared with the untreated girls in a weak dose-dependent manner, 2.3 cm (100 micrograms/day), 3.0 cm (300 micrograms/day), and 3.8 cm (500 micrograms/day). Such a dose dependency was not found on applying the Bayley-Pineau height prediction method (100 micrograms/day; 4.1 cm; 300 micrograms/day: 4.2 cm; 500 micrograms/day: 4.5 cm). However, there was a striking inverse correlation of the BA at the onset of treatment with the height reduction achieved using the TW II method (r: -0.43; P0.001). Importantly, girls with a BA below 12 years at the onset of treatment experienced a height reduction of more than 6 cm. CONCLUSION The EE dose used in the range of 100-500 micrograms/day is not crucial for the amount of height reduction in tall girls. In general high dose EE treatment should be given restrictively, and especially so in girls with a BA (TW2 RUS-ZH) above 12.0 years.

Published
1994

17. Contents, Vol. 64,1993

Author

Bruno Baggio, Yasushi Sato, C.A. Lawton, Kiyoshi Hirano, L. Raffaele, F. Scaccia, Ermanno Bonucci, P.-E. Mullis, N Di Paolo, P.K. Srivastava, Giuliano Barsotti, Hikaru Koide, G. Calconi, O.H. Oetliker, Heiko Mühl, Ralph J. Butkowski, Naoto Shikura, P. Calzavara, Adeera Levin, Suguru Tomooka, Daniel Séréni, C. Arici, G. Sacchi, F. Loi, Uri Shaked, Miroslaw Smogorzewski, E. Vilella, George Z. Fadda, P. Viale, S. Amato, Pedro Esbrit, G. Rossi, David V. Milford, M.P. Beraldi, C. Mirabella, V. Scafidi, Minoru Kubota, Michael Field, Kamel S. Kamel, J.E. Moulder, Hana Manor, Toshitaka Fujishiro, Perez Perez, Jean-François Morin, Antonio Piccoli, Bernard Bourbigot, Yvon L. Pennec, Shim Kamakura, P.G. Simeoni, Jeannette M. Goguen, G. Pedroni, Lopez Guerre, M. Desperati, Kazuo Haze, Kazuhiro Saito, Shaul G. Massry, Gabriele Bertolone, S. Kiyama, V. Sparacino, C. Villabona, F. Locatelli, Takashi Miyazaki, F.A. Cattaneo, F. Pietrobon, Nicoletta Galardi, M.R. Averna, M. Migliori, E. Tanzariello, Hirofumi Makino, Deoraj Appaiha, Gilles Sarfati, M. Daglio, R. Giordano, F. Fabrizi, A. Notarbartolo, Toshimitsu Niwa, Daniela Gabizon, E. Francavilla, Kanji Uema, G. Bacchini, Hidetoshi Kanai, M. C. Maresca, E.P. Cohen, Yasushi Yamasaki, Adrian Fine, José Ortega, Katsuro Shimomura, Mono Kuramochi, M.G. Bianchetti, Mitchell L. Halperin, A. Guarnieri, Joseph Maor, Adamasco Cupisti, Dieter Kunz, Robert M. Richardson, Alfred J. Fish, G. Erba, Marc E. De Broe, A. Galione, G. Zullo, Ross R. Bailey, Ben-Ami Sela, D. Tacconi, M. De Gennaro, Martin Tieder, Vincenzo Puro, Olivier Tauléra, A.M. Mangiarotti, Maurizio Nordio, Simon Strauss, C. Campieri, Yoshihiro Tominaga, Seiya Okuda, Sergio Costantini, J. Joven, César García-Cantón, K. Tripathi, Tetsuya Tsuzuki, Judith Blonder, I. Guarnori, D. Marchesi, Helmut Schiffl, M. Di Paolo, Paola Ballanti, J.R. Larrañaga, Giuseppe Ippolito, Olivera Stojceva-Taneva, G. Duss, Claude Bachmeyer, Masatoshi Fujishima, Monique Elseviers, Yutaka Emoto, R. Izquierdo, Hiro Matsukura, D. Orazi, Jean-Pierre Codet, Giovanni Gambaro, Adolfo García-Ocaña, R.C. Ash, Michel Garre, Della Volpe, C.M. Barbagallo, G.F. Romagnoli, Thomas Sitter, P. Maggi, Dalla Rosa, C.G. Becker, R. Di Legge, Hideki Hirakata, Kazue Hironaka, Georges Cremer, S. Petricca, Osamu Kinoshita, Jai Prakash, Mario Andriani, C. Mancino, Michael H. Winterborn, E. Caputo, Genjiro Kimura, R. Kramer, Carol A. Pollock, Giorgio Mattiello, Sergio Giovannetti, Zensuke Ota, Josef Pfeilschifter, S. Cesare, F. Martinelli, P.G. Poisetti, Teruo Omae, Keiichi Takada, Gabriel Le Menn, Isao Ishikawa, E. Peheim, Nicola Petrosillo, Kenji Maeda, V. Portelli, Gilles Grateau, Yolanda González-García, Ronan S. Tanneau, S. Soffritti, A.B. Cefalù, Yasuhiko Tomino, D. Vlacos, and F. Manescalchi

Subjects
Traditional medicine, business.industry, Medicine, business
Published
1993

18. Adult height in constitutionally tall stature: accuracy of five different height prediction methods

Author

R Temperli, P E Mullis, and E. E. Joss

Subjects
Male, Aging, Adolescent, Child Development, Sex Factors, Predictive Value of Tests, Prediction methods, Humans, Medicine, Child, Retrospective Studies, Bone Development, business.industry, Final height, Tall Stature, Bone age, Chronological age, Body Height, Confidence interval, Adult height, Predictive value of tests, Pediatrics, Perinatology and Child Health, Female, business, Research Article, Demography
Abstract

The accuracy of height predictions at various ages based on five different methods (Tanner-Whitehouse mark I; Tanner-Whitehouse mark II; index of potential height; Bayley-Pinneau; Roche-Wainer-Thissen) was compared at yearly intervals with final height achieved in 32 boys (78 predictions) and 100 girls (227 predictions) with constitutionally tall stature. The boys were initially seen at a mean (SD) chronological age of 12.5 (3) years whereas the mean chronological age in girls was 11.8 (2.1) years. In tall boys Tanner-Whitehouse mark II gives a good estimation of final height up to the bone age of 13 years with a mean overestimation of 1 cm. The overestimation of final height is higher in the bone age groups 13-14 years (2.7 cm) and 14-15 years (3.4 cm) mainly due to the tall boys with a height greater than 3 SD scores. Up to the bone age of 12 years the final height is massively overestimated by the Bayley-Pinneau method but this method give relatively accurate estimations thereafter. The estimated confidence limits are large (+/- 8 cm) for the two methods up to a bone age of 15 years. In tall girls the Tanner-Whitehouse mark II method was accurate from bone age nine to 12 years but overestimated final height in the bone age groups 12-13 years and 13-15 years by a mean of 1.8 and 1.4 cm respectively. The Bayley-Pinneau method overestimated final height in the bone age groups 12-14 years whereas the height predictions are accurate thereafter. Up to a bone age of 13 years the estimated confidence limits for the two methods are large, +/- cm, but tend to improve thereafter. It is concluded that there is no best or most accurate method for predicting adult height in tall children. There are methods of first choice differing with respect to sex and bone age. In addition, correcting factors may improve their accuracy and correct their tendency to overestimate or underestimate adult height.

Published
1992

19. [Role of complementary medicine in type 1 diabetes mellitus in two Swiss centres]

Author

U A, Scheidegger, C E, Flück, K, Scheidegger, P, Diem, and P E, Mullis

Subjects
Adult, Complementary Therapies, Male, Adolescent, Middle Aged, Combined Modality Therapy, Young Adult, Diabetes Mellitus, Type 1, Treatment Outcome, Child, Preschool, Surveys and Questionnaires, Utilization Review, Humans, Insulin, Female, Child, Switzerland, Aged
Abstract

Insulin replacement is the only effective treatment of type 1 Diabetes mellitus (T1DM). Nevertheless, many complementary treatments are in use for T1DM. In this study we assessed by questionnaire that out of 342 patients with T1DM, 48 (14%; 13.4% adult, 18.5% paediatric; 20 male, 28 female) used complementary medicine (CM) in addition to their insulin therapy. The purpose of the use of CM was to improve general well-being, ameliorate glucose homeostasis, reduce blood glucose levels as well as insulin doses, improve physical fitness, reduce the frequency of hypoglycaemia, and control appetite. The modalities most frequently used are cinnamon, homeopathy, magnesium and special beverages (mainly teas). Thus, good collaboration between health care professionals will allow optimal patient care.

Published
2009

20. [Growth: what is normal?]

Author

P-E, Mullis and M, Janner

Subjects
Male, Adolescent, Puberty, Age Factors, Infant, Newborn, Infant, Body Height, Diagnosis, Differential, Sex Factors, Reference Values, Age Determination by Skeleton, Child, Preschool, Humans, Mass Screening, Female, Child, Physical Examination, Growth Disorders
Abstract

Growth is an inherent property of life, which has to be checked and controlled by any general physician following children. Therefore, the common knowledge about the normal pattern/course of growth is essential in order to act proactively whenever the child's growth does not progress adequately.

Published
2009

21. [Hermaphroditos in Greek mythology--DSD in moderne medicine]

Author

A, Oestmann, P E, Mullis, and Z, Stanga

Subjects
Adult, Diagnosis, Differential, Addison Disease, Adrenal Hyperplasia, Congenital, Homozygote, Mutation, Disorders of Sex Development, Humans, Infant, Female, Mythology, Algorithms
Abstract

We report a case of 34 year old woman how has been hospitalized at the age of 6 month with persistent vomitus. The vomitus was found to be caused by adrenal insufficiency with lack of all hormones of steroidobiosynthesis. The phenotypical femal child was diagnosed to have congenital lipoid adrenal hyperplasia with 46,XY DSD. 24 years later a homozygote mutation in the StAR-gene (L260P), which was first described in Switzerland, has been identified.

Published
2009

22. [Impaired calcium homeostasis, clinical impact]

Author

M, Janner and P E, Mullis

Subjects
Adult, Adolescent, Hypocalcemia, Infant, Newborn, Infant, Vitamin D Deficiency, Bone and Bones, Phosphates, Diagnosis, Differential, Reference Values, Child, Preschool, Hypercalcemia, Homeostasis, Humans, Calcium, Child
Abstract

Abnormalities of the calcium homeostasis are, with exception of the neonatal period, not often to diagnose in childhood. However, as the clinical features may not only be quite heterogeneous but also present with a very changing pattern, abnormalities of calcium homeostasis have to be considered in many differential diagnoses. Extracellular fluid calcium or plasma calcium is very carefully controlled by fluxes of calcium, which occur between the extracellular fluid and the skeleton, as well as between gut and the kidneys. Therefore, in this review, first, the factors physiologically regulating calcium homeostasis and bone formation are summarized; and then, the situations in which the plasma calcium level should be measured in daily clinical practices are discussed.

Published
2007

23. [Doping in adolescence]

Author

M, Kamber and P-E, Mullis

Subjects
Doping in Sports, Anabolic Agents, Adolescent, Substance-Related Disorders, Growth Hormone, Humans, Central Nervous System Stimulants, Switzerland
Abstract

Doping in sport is often very present in the media. Doping does not only concern top level sports but it also has an impact on sport as a whole. Young athletes may be influenced by its role models. In Switzerland there are no exact data on this influence or on the use of doping by adolescents. In this article, the effects and side-effects especially on adolescents of some current doping substances are discussed. As well, the regulations of the therapeutic use exemptions for doping substances are explained.

Published
2007

24. [Sun-tanned and still not healthy!]

Author

D, Spörri and P E, Mullis

Subjects
Adolescent, Hydrocortisone, Anti-Inflammatory Agents, Infant, Newborn, Infant, Shock, Prognosis, Celiac Disease, Treatment Outcome, Addison Disease, Child, Preschool, Fludrocortisone, Humans, Female, Child
Abstract

We describe a case of a 10 years old girl, which presented to the emergency room with non-specific gastro-intestinal symptoms, fatigue and low blood pressure. The clinical signs and laboratory value supported the diagnosis of Addison crisis with hypovolaemic shock. The pathophysiology and the therapy of this entity are discussed. Importantly, in children the aetiology may differ depending on age and sex. Based on the family history of autoimmune disorders, in our patient presenting with autoimmune adrenalitis and celiac disease, the diagnosis of an autoimmune polyendocrinopathy was made. A therapy of mineralcorticoids and glucocorticoids was initiated and a special gluten-free diet was prescribed. On this treatment our patient recovered promptly.

Published
2006

25. [Is the metabolic syndrome a new childhood disease?]

Author

M, Janner, P E, Mullis, and C E, Flück

Subjects
Adult, Male, Metabolic Syndrome, Adolescent, Age Factors, Infant, Prognosis, Body Mass Index, Diagnosis, Differential, Risk Factors, Child, Preschool, Hypertension, Humans, Obesity, Insulin Resistance, Child, Exercise, Algorithms, Dyslipidemias
Abstract

Overweight and obesity in children and adolescents have become a major public health problem in recent years throughout the world. The medical consequences of obesity may manifest as an increase in the prevalence of the metabolic syndrome in children and adolescents putting them at increased risk for future cardiovascular diseases. Obesity can cause insulin resistance and might disturb glucose homeostasis eventually leading to type 2 diabetes in susceptible patients. Insulin resistance is also involved in the pathogenesis of dyslipidemia in obese children characteristically presenting as hypertriglyceridemia and low HDL cholesterol. Even elevated blood pressure might be present in obese kids. Here we present a 12-year-old boy diagnosed with the metabolic syndrome. The diagnostic criteria of the metabolic syndrome in children and adolescents are discussed. Thoughts about pathophysiology and therapeutic options are offered.

Published
2006

26. [Follow-up in a boy with Leydig cell tumor after selective surgery]

Author

T, Gozzi, Ch E, Flück, and P-E, Mullis

Subjects
Diagnosis, Differential, Male, Testicular Neoplasms, Testis, Humans, Puberty, Precocious, Child, Gonadal Steroid Hormones, Follow-Up Studies, Leydig Cell Tumor, Ultrasonography
Abstract

A 8(6/12) year-old-boy presented with precocious puberty and a slightly enlarged left testis. After a detailed examination a Leydig cell tumour was diagnosed. Surgical exploration revealed an encapsulated tumour, 2.7 cm in length, which was selectively removed without orchidectomy. Within one year the clinical signs of pubertal precocity disappeared, the bone age did not further advance and height velocity declined from 8.2 cm / year (+3.9 SDS) to 4.1 cm/year (-1.0 SDS). Physiologically, he entered puberty at the chronological age of twelve years, presenting at that age, in comparison to his peer group, a slightly decreased pubertal growth spurt. However, bearing in mind that being precocious in puberty he started in fact his pubertal growth spurt at a far earlier age, therefore, this acceleration of height before operation has to be added to the centimetres gained during pubertal development thereafter resuiting consequently in an absolute normal pubertal growth spurt. This underlines the fact that the individual growth spurt and, therefore, the total amount of centimetres gained is very much robust. Ten years later, the patient ended up well within his familial target height and remained free of disease. We report on a long-term follow-up of a prepubertal boy after testis-sparing surgery for Leydig-cell-tumour.

Published
2006

27. [Hypoglycaemia--diagnosis and therapy in emergencies]

Author

J M, Nuoffer and P E, Mullis

Subjects
Blood Glucose, Critical Care, Infant, Newborn, Infant, Risk Assessment, Hypoglycemia, Risk Factors, Child, Preschool, Germany, Practice Guidelines as Topic, Emergency Medicine, Humans, Emergencies, Practice Patterns, Physicians', Child, Emergency Treatment
Abstract

Hypoglycaemia defined as blood sugar below 2.5 mmol/L, is always an important medical emergency. The primary therapy is simple and consists of iv glucose. The occurrence of hypoglycaemia is directly connected to fuel balance, determined by the availability of glucose, free fatty acids and ketone bodies. An intact fuel balance and maintenance of normal blood sugar concentration is dependent upon: (1) an adequate caloric and qualitative dietary intake; (2) afunctionally intact hepatic glucogenolytic and gluconeogenic enzyme system; (3) an adequate supply of endogenous gluconeogenic substrates (lactate, amino acids and glycerol) (4) an adequate energy supply provided by the beta-oxidation of fatty acids to synthesize glucose and ketone bodies and (5) a normal endocrine system (insulin, glucagon, catecholamines and growth hormone) for integrating and modulating these processes. Disturbances in each of these factors may lead to hypoglycaemia. Glucose, like oxygen, is of essential and fundamental importance for the brain metabolism. The major contribution of the brain to the basal metabolic rate (70% in neonates versus 20% in adults) is an important factor contributing to the frequency and severity of a hypoglycaemic syndrome in the paediatric age. If hypoglycaemia is suspected, blood should be obtained prior to treatment for serum glucose determination and an extra tube (5 ml) serum should be obtained and refrigerated for further investigations. The first voided urine has to be tested for ketones using a dipstick and also refrigerated for further investigations. Basic laboratory investigations, anamnestic informations and clinical findings allow rapid tentative diagnosis and determine the specialized investigations out of the refrigerated material. A rapid definitive diagnosis is important for the specific treatment and to avoid recurrent and prolonged hypoglycaemia.

Published
2005

28. [The diabetic child in the emergency room]

Author

Ch E, Flück and P E, Mullis

Subjects
Adolescent, Critical Care, Pediatrics, Risk Assessment, Hypoglycemia, Diagnosis, Differential, Neurology, Risk Factors, Child, Preschool, Germany, Acute Disease, Practice Guidelines as Topic, Diabetes Mellitus, Emergency Medicine, Humans, Emergencies, Practice Patterns, Physicians', Child, Emergency Treatment
Abstract

The WHO announced diabetes mellitus as one of the main threats to human health in the 21st century. In children and adolescents the prevalence of both the autoimmune type 1 and the obesity-related type 2 diabetes is increasing. Common to all types of diabetes is an absolute or relative lack of insulin to keep glucose homeostasis under control. Thus children and adolescents with newly diagnosed diabetes present with hyperglycemia which is often accompanied by ketoacidosis bearing the risk of cerebral edema. Children and adolescents with known diabetes treated with insulin or orale antidiabetic agents may also suffer from hyperglycemia or even ketoacidosis during times of non-compliance with diet and drugs or during concomitant illnesses. Hyperglycemia with ketoacidosis is an emergency situation for which patients need to be admitted to the next hospital for administration of insulin, fluids and potassium. In contrast, insulin treatment in diabetic patients may also lead to a hypoglycemia, the sudden drop in blood glucose, at any moment. Thus recognition and correction of mild hypoglycemia should be familiar to every diabetic child and their caretaker. Severe hypoglycemia with or without seizures may bring the diabetic child in a sudden emergency situation for which the administration of glucagon intramuscularly or glucose intravenously is mandatory. After every severe hypoglycemia the insulin and diet regimen of the diabetic child or adolescent must be reviewed with the diabetes specialist. For unexplained hypoglycemia or major treatment adjustments the diabetic child or adolescent may need to be readmitted to the diabetic ward of a hospital to avoid repeat, potentially life-threatening hypoglycemia.

Published
2005

29. Osteonpenia and pathological fractures in an adolescent with lactose intolerance and high oxalate intake

Author

M. Janner and P. E. Mullis

Subjects
Gynecology, medicine.medical_specialty, business.industry, Pediatrics, Perinatology and Child Health, medicine, Child and adolescent psychiatry, Surgery, 610 Medicine & health, business
Abstract

Zusammenfassung: Wir stellen einen Jugendlichen mit Osteopenie und pathologischen Frakturen vor. Der Fall soll auf folgende Punkte aufmerksam machen: Eine adäquate Kalziumzufuhr während Kindheit und Adoleszenz ist für die Entwicklung einer normalen "peak bone mass" von ausschlaggebender Bedeutung. Es ist wahrscheinlich, dass moderne Ernährungsgewohnheiten (Junkfood und Softdrinks) bisher noch zu wenig erkannte Auswirkungen auf die Gesundheit unserer Knochen haben

Published
2005

31. Effect of growth hormone and oxandrolone treatment on glucose metabolism in Turner syndrome. A longitudinal study

Author

E E, Joss, R P, Zurbrügg, O, Tönz, and P E, Mullis

Subjects
Adult, Blood Glucose, Adolescent, Human Growth Hormone, Turner Syndrome, Glucose Tolerance Test, Oxandrolone, Anabolic Agents, Insulin Secretion, Diabetes Mellitus, Humans, Insulin, Drug Therapy, Combination, Female, Safety, Child
Abstract

In 18 girls with Turner syndrome, glucose tolerance was studied before treatment and after 6 and 24 months of growth-promoting treatment with recombinant human growth hormone (24 IU/m(2)/week; 8 mg/m(2)/week) and oxandrolone (0.06 mg/kg/day), as well as after termination of the treatment. One girl developed an overt non-ketotic diabetes mellitus 50 months after termination of treatment. The results of the remaining 17 girls in whom the effect of treatment on glucose metabolism was reversible are presented as a group. Their median age at the beginning of the treatment was 10.4 years (range 6.9-15.9), and 15.0 years (range 12.1-19.9) at the final assessment. There was a moderate, but not significant rise in fasting glucose throughout the course of the longitudinal study. At oral glucose tolerance testing (oGTT), the area under the curve for glucose rose significantly (p = 0.013) during the period of treatment and returned to the basic value thereafter. Fasting insulin and especially the integrated insulin values (AUCi; area under the curve for insulin) during oGTT increased continuously during treatment, declined after termination of treatment but were still significantly (p = 0.04) higher than before treatment. Considering the fact that in untreated girls with Turner syndrome the fasting insulin and the AUCi increase with age, one can conclude that the insulinaemia returned to age-specific norm after termination of treatment. Thus the effect of a combined growth hormone and oxandrolone growth-promoting treatment on glucose metabolism was fully reversible in these 17 girls with Turner syndrome.

Published
2000

32. [Metabolic control in children and adolescents with diabetes mellitus type I in Berne: a cross-sectional study]

Author

C E, Flück, B V, Kuhlmann, and P E, Mullis

Subjects
Blood Glucose, Glycated Hemoglobin, Male, Adolescent, Puberty, Age Factors, Body Mass Index, Cross-Sectional Studies, Diabetes Mellitus, Type 1, Humans, Insulin, Female, Age of Onset, Child
Abstract

In diabetes mellitus type I, good glycaemic control is crucial in preventing long-term diabetic complications. The aim of this study was to determine the current level of metabolic control in children and adolescents in our diabetes outpatient clinic at the University Children's Hospital, Berne. Furthermore, the impact of different factors such as age, pubertal stage, sex, duration of diabetes and insulin regimen on glycaemic control was studied.In a cross-sectional, prospective study 168 children and adolescents with type I diabetes mellitus (f:m = 87:81; prepubertal 48 [mean age 4.4 years, mean duration of diabetes 2.8 years]; pubertal 120 [mean age 9.4 years; mean duration of diabetes 5.2 years]) were studied for three months. Clinical data and HbA1c levels (latex immunoagglutination test) were recorded, statistically analysed and compared with the international literature.In our type I diabetic children and adolescents the overall HbA1c was 8.07 +/- 1.15% (mean +/- SD; test-specific norm for healthy subjects: 4.1-6.1%). Glycaemic control was significantly worse in the pubertal group compared to the prepubertal (HbA1c 8.22 +/- 1.25% vs. 7.81 +/- 0.87%; p0.01). In addition, we found better metabolic control in patients with duration of diabetes below 2 years in children and adolescents (HbA1c prepubertal2 years: 7.45 +/- 0.67% vs.2 years: 8.05 +/- 0.93%, p0.05; pubertal2 years: 7.62 +/- 0.75% vs.2 years: 8.31 +/- 1.29%, p0.005). Importantly, sex and insulin regimen did not significantly influence glycaemic control.The current level of metabolic control in our children and adolescents with diabetes mellitus type I is comparable to the glycaemic control of the intensively treated adolescent group of the DCCT-study, in whom decreased risk of long-term diabetic complications was found. In contrast, our patients were intensively treated in terms of frequent contacts with the diabetes team, but were not necessarily on an intensified insulin regimen. The impact of biopsychosocial support from multidisciplinary diabetes team on good metabolic control in children and adolescents with type I diabetes mellitus and their families seems to be very important.

Published
1999

33. Aromatase deficiency caused by a novel P450arom gene mutation: impact of absent estrogen production on serum gonadotropin concentration in a boy

Author

J, Deladoëy, C, Flück, M, Bex, N, Yoshimura, N, Harada, and P E, Mullis

Subjects
Male, Heterozygote, Base Sequence, Homozygote, Androstenedione, Infant, Newborn, Estrogens, Luteinizing Hormone, Virilism, Pedigree, Gonadotropin-Releasing Hormone, Pregnancy Complications, Aromatase, Pregnancy, Humans, Female, Testosterone, Follicle Stimulating Hormone, Frameshift Mutation
Abstract

We identified a new point mutation in the CYP19 gene responsible for aromatase (P450arom) deficiency in a 46,XY male infant with unremarkable clinical findings at birth. This boy is homozygote for a 1-bp (C) deletion in exon 5 of the aromatase gene causing a frame-shift mutation. The frame-shift results in a prematurely terminated protein that is inactive due to the absence of the functional regions of the enzyme. Aromatase deficiency was suspected prenatally because of the severe virilization of the mother during the early pregnancy, and the diagnosis was confirmed shortly after birth. Four weeks after birth, the baby boy showed extremely low levels of serum estrogens, but had a normal level of serum free testosterone; in comparison with the high serum concentration of androstenedione at birth, a striking decrease occurred by 4 weeks postnatally. We previously reported elevated basal and stimulated FSH levels in a female infant with aromatase deficiency in the first year of life. In contrast, in the male infant, basal FSH and peak FSH levels after standard GnRH stimulation tests were normal. This finding suggests that the contribution of estrogen to the hypothalamic-pituitary gonadotropin-gonadal feedback mechanism is different in boys and girls during infancy and early childhood. In normal girls, serum estradiol concentrations strongly correlate with circulating inhibin levels, and thus, low inhibin levels may contribute to the striking elevation of FSH in young girls with aromatase deficiency. In contrast, estradiol levels are physiologically about a 7-fold lower in boys than in girls, and serum inhibin levels remain elevated even though levels of FSH, LH, and testosterone are decreased.

Published
1999

34. [What is the value of determining immunoreactive GHRH in acromegaly?]

Author

B, Müller, D, de Marco, U, Bürgi, and P E, Mullis

Subjects
Adult, Male, Acromegaly, Radioimmunoassay, Humans, Female, Insulin-Like Growth Factor I, Middle Aged, Growth Hormone-Releasing Hormone
Abstract

Acromegaly is usually due to autonomous, excessive secretion of growth hormone from a pituitary adenoma. One would expect growth hormone-releasing factor (GHRH) in these patients to be suppressed. In the available literature referring to acromegaly, immunoreactive GHRH levels were determined in 259 acromegalic patients. When growth hormone was measured simultaneously, no correlation was found between serum growth hormone and plasma GHRH concentrations, irrespective of whether the acromegalic patients were treated or not. A possible explanation for this finding might be the lack of a feedback regulation between plasma growth hormone and GHRH. Also, since growth hormone is secreted in a pulsatile fashion the interpretation of single growth hormone values can be difficult. IGF I, which correlates well with mean growth hormone production, may therefore represent a more valuable criterion for the assessment of activity and GHRH plasma levels in acromegalics. However, no study has yet been performed to elucidate the relationship between GHRH and IGF I in acromegaly. To examine this relationship we measured the concentration of plasma GHRH and IGF I in 18 treated patients with acromegaly (age range 32-64 years median 50.5 years; median follow-up 6.5 years, range 3 months to 33 years). All immunoreactive GHRH levels were within the limits described as normal in the literature (mean +/- SD 22.89 +/- 2.72 pg/ml, range 19-28 pg/ml). The IGFI level was 396.78 +/- 224.26 ng/ml (mean +/- SD, range 71-876 ng/ml; reference ranges, age group 25-39 years: 114-492 ng/ml; 40-54 years: 90-360 ng/ml;55 years: 71-290 ng/ml). We found no correlation between IGF I and GHRH concentrations (r = 0.17). We therefore conclude that measuring plasma GHRH is not useful in the evaluation of the activity or therapy of acromegaly but may be helpful in its differential diagnosis since a massive elevation of GHRH is typically associated with the ectopic GHRH syndrome, a rare cause of acromegaly.

Published
1999

35. 'Hot spot' in the PROP1 gene responsible for combined pituitary hormone deficiency

Author

J, Deladoëy, C, Flück, A, Büyükgebiz, B V, Kuhlmann, A, Eblé, P C, Hindmarsh, W, Wu, and P E, Mullis

Subjects
Adult, Homeodomain Proteins, Male, Genome, Polymorphism, Genetic, Human Growth Hormone, Mutation, Missense, Thyrotropin, Luteinizing Hormone, Pedigree, Prolactin, Alternative Splicing, Mice, Pituitary Hormones, Phenotype, Adrenocorticotropic Hormone, Animals, Humans, Female, Follicle Stimulating Hormone, Frameshift Mutation, Gene Deletion, Gonadotropins, Transcription Factors
Abstract

As pituitary function depends on the integrity of the hypothalamic-pituitary axis, any defect in the development and organogenesis of this gland may account for a form of combined pituitary hormone deficiency (CPHD). Although pit-1 was 1 of the first factors identified as a cause of CPHD in mice, many other homeodomain and transcription factors have been characterized as being involved in different developmental stages of pituitary gland development, such as prophet of pit-1 (prop-1), P-Lim, ETS-1, and Brn 4. The aims of the present study were first to screen families and patients suffering from different forms of CPHD for PROP1 gene alterations, and second to define possible hot spots and the frequency of the different gene alterations found. Of 73 subjects (36 families) analyzed, we found 35 patients, belonging to 18 unrelated families, with CPHD caused by a PROP1 gene defect. The PROP1 gene alterations included 3 missense mutations, 2 frameshift mutations, and 1 splice site mutation. The 2 reported frameshift mutations could be caused by any 2-bp GA or AG deletion at either the 148-GGA-GGG-153 or 295-CGA-GAG-AGT-303 position. As any combination of a GA or AG deletion yields the same sequencing data, the frameshift mutations were called 149delGA and 296delGA, respectively. All but 1 mutation were located in the PROP1 gene encoding the homeodomain. Importantly, 3 tandem repeats of the dinucleotides GA at location 296-302 in the PROP1 gene represent a hot spot for CPHD. In conclusion, the PROP1 gene seems to be a major candidate gene for CPHD; however, further studies are needed to evaluate other genetic defects involved in pituitary development.

Published
1999

36. Phenotypic variability in familial combined pituitary hormone deficiency caused by a PROP1 gene mutation resulting in the substitution of Arg--Cys at codon 120 (R120C)

Author

C, Flück, J, Deladoey, K, Rutishauser, A, Eblé, U, Marti, W, Wu, and P E, Mullis

Subjects
Homeodomain Proteins, Male, Infant, Pedigree, Pituitary Hormones, Phenotype, Adrenocorticotropic Hormone, Amino Acid Substitution, Child, Preschool, Mutation, Humans, Female, Child, Codon, Transcription Factors
Abstract

As pituitary function depends on the integrity of the hypothalamic-pituitary axis, any defect in the development and organogenesis of this gland may account for a form of combined pituitary hormone deficiency (CPHD). A mutation in a novel, tissue-specific, paired-like homeodomain transcription factor, termed Prophet of Pit-1 (PROP1), has been identified as causing the Ames dwarf (df) mouse phenotype, and thereafter, different PROP1 gene alterations have been found in humans with CPHD. We report on the follow-up of two consanguineous families (n = 12), with five subjects affected with CPHD (three males and two females) caused by the same nucleotide C to T transition, resulting in the substitution of Arg--Cys in PROP1 at codon 120. Importantly, there is a variability of phenotype, even among patients with the same mutation. The age at diagnosis was dependent on the severity of symptoms, ranging from 9 months to 8 yr. Although in one patient TSH deficiency was the first symptom of the disorder, all patients became symptomatic by exhibiting severe growth retardation and failure to thrive, which was mainly caused by GH deficiency (n = 4). The secretion of the pituitary-derived hormones (GH, PRL, TSH, LH, and FSH) declined gradually with age, following a different pattern in each individual; therefore, the deficiencies developed over a variable period of time. All of the subjects entered puberty spontaneously, and the two females also experienced menarche and periods before a replacement therapy was necessary.

Published
1998

37. Aromatase deficiency in a female who is compound heterozygote for two new point mutations in the P450arom gene: impact of estrogens on hypergonadotropic hypogonadism, multicystic ovaries, and bone densitometry in childhood

Author

P E, Mullis, N, Yoshimura, B, Kuhlmann, K, Lippuner, P, Jaeger, and H, Harada

Subjects
Adult, Male, Heterozygote, Hypogonadism, Ovary, Infant, Newborn, Estrogens, Pedigree, Aromatase, Genes, Bone Density, Pregnancy, Humans, Point Mutation, Female, Follicle Stimulating Hormone, Polycystic Ovary Syndrome, Ultrasonography
Abstract

We report on a female who is compound heterozygote for two new point mutations in the CYP19 gene. The allele inherited from her mother presented a base pair deletion (C) occurring at P408 (CCC, exon 9), causing a frameshift that results in a nonsense codon 111 bp (37 aa) further down in the CYP19 gene. The allele inherited from her father showed a point mutation from G--A at the splicing point (canonical GT to mutational AT) between exon and intron 3. This mutation ignores the splice site and a stop codon 3 bp downstream occurs. Aromatase deficiency was already suspected because of the marked virilization occurring prepartum in the mother, and the diagnosis was confirmed shortly after birth. Extremely low levels of serum estrogens were found in contrast to high levels of androgens. Ultrasonographic follow-up studies revealed persistently enlarged ovaries (19.5-22 mL) during early childhood (2 to 4 yr) which contained numerous large cysts up to 4.8 x 3.7 cm and normal-appearing large tertiary follicles already at the age of 2 yr. In addition, both basal and GnRH-induced FSH levels remained consistently strikingly elevated. Low-dose estradiol (E2) (0.4 mg/day) given for 50 days at the age of 3 6/12 yr resulted in normalization of serum gonadotropin levels, regression of ovarian size, and increase of whole body and lumbar spine (L1-L4) bone mineral density. The FSH concentration and ovarian size returned to pretreatment levels shortly (150 days) after cessation of E2 therapy. Therefore, we recommend that affected females be treated with low-dose E2 in amounts sufficient to result in physiological prepubertal E2 concentrations using an ultrasensitive estrogen assay. However, E2 replacement needs to be adjusted throughout childhood and puberty to ensure normal skeletal maturation and adequate adolescent growth spurt, normal accretion of bone mineral density, and, at the appropriate age, female secondary sex maturation.

Published
1997

38. Extracellular magnesium depletion in pediatric patients with insulin-dependent diabetes mellitus

Author

M J, Husmann, P, Fuchs, A C, Truttmann, R, Laux-End, P E, Mullis, E, Peheim, and M G, Bianchetti

Subjects
Adult, Male, Adolescent, Hydrogen-Ion Concentration, Diabetes Mellitus, Type 1, Reference Values, Cations, Child, Preschool, Humans, Calcium, Female, Magnesium, Child, Extracellular Space, Magnesium Deficiency
Abstract

It is unclear whether insulin-dependent diabetes mellitus is a state of magnesium depletion. This is a relevant question, since magnesium deficiency has been implicated in the pathogenesis of diseases that develop to an increased extent into diabetes mellitus. Total plasma magnesium was not statistically different in 76 pediatric patients with insulin-dependent diabetes mellitus (0.77 [0.73-0.81] mmol/l; median and interquartile range), 59 healthy adults (0.80 [0.77-0.83] mmol/l) and 19 healthy children (0.80 [0.78-0.83] mmol/l). In contrast, plasma ionized magnesium, the most interesting form with respect to physiological and biological properties, was significantly lower in diabetic patients (0.50 [0.48-0.53] mmol/l) when compared with healthy adults (0.53 [0.50-0.56] mmol/l; p0.01) and healthy children (0.54 [0.51-0.56] mmol/l; p0.02). Our report confirms recent findings of reduced circulating ionized magnesium but normal circulating total magnesium in adults with non-insulin-dependent diabetes mellitus.

Published
1997

39. Growth promotion and Turner-specific bone age after therapy with growth hormone and in combination with oxandrolone: when should therapy be started in Turner syndrome?

Author

P.-E. Mullis, C.J. Partsch, E.E. Joss, E.A. Werder, and W.G. Sippell

Subjects
medicine.medical_specialty, Pediatrics, Younger age, medicine.drug_class, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Growth promotion, Turner Syndrome, Growth, Growth hormone, Bone and Bones, Oxandrolone, Endocrinology, Anabolic Agents, Internal medicine, Age Determination by Skeleton, Turner syndrome, medicine, Humans, Child, business.industry, Human Growth Hormone, Age Factors, Bone age, medicine.disease, Body Height, Estrogen, Drug Therapy, Combination, Female, business, Anabolic steroid, medicine.drug
Abstract

The aims of this comparative multicenter study of 67 girls with Turner syndrome (TS) on three different therapeutical regimens were, first, to evaluate the effect of either recombinant human growth hormone (GH) alone or in combination with the anabolic steroid oxandrolone (Oxa) on height velocity and on Turner-specific bone age (BA’TS) and, second, to estimate the gain in final height taking the age at the onset of treatment into account. The mean advancement of BA’TS in 2 years of treatment was 2.5 years/2 years in group 1 (low dose GH: 16 IU/m2/week), 2.8 years/2 years in group 2 (high dose GH: 28 IU/m2/week) and 3.3 years/2 years in group 3 (GH: 24 IU/m2/week + Oxa: 0.06 mg/kg/day) instead of the expected 2 years/2 years advancement in untreated girls with TS. On all treatment regimens the advancement of BA’TS was more pronounced in the younger girls. In many girls with a BA’TS below 9 years at the onset of treatment the increase in height did not outweigh the advancement in BA’TS, suggesting that starting growth-promoting treatment before 9 years would not be the best way to improve final height. In our opinion, the optimal age for starting growth-promoting therapy is at 9 years. A start at a younger age might have no advantage in regard of an ultimate gain in final height. On the other hand, therapy should not be delayed much after the age of 9 years giving the girls with TS the possibility to catch up substantially before estrogen treatment is initiated.

Published
1997

40. Delayed puberty in boys

Author

E E, Joss and P E, Mullis

Subjects
Male, Puberty, Delayed, Humans, Testosterone, Child, Body Height, Growth Disorders
Published
1994

41. [Diabetes in childhood and adolescence]

Author

P E, Mullis and G, Theintz

Subjects
Parents, Patient Care Team, Adolescent, Psychology, Adolescent, Psychology, Child, Hypoglycemia, Hospitalization, Self Care, Diabetes Mellitus, Type 1, Patient Education as Topic, Diet, Diabetic, Humans, Insulin, Child
Published
1994

42. High proximal excretion of sodium during activation of beta 2-adrenoreceptors in humans

Author

G, Duss, M G, Bianchetti, F A, Cattaneo, P E, Mullis, R, Krämer, E, Peheim, and O H, Oetliker

Subjects
Adult, Male, Electrolytes, Heart Rate, Receptors, Adrenergic, beta, Sodium, Humans, Natriuresis, Albuterol, Lithium, Kidney
Abstract

The effects of acute beta 2-type adrenoreceptor activation with intravenous albuterol on plasma and urinary sodium, potassium, calcium, magnesium, phosphate and lithium were investigated in 9 volunteers during acute hydration. When compared with the control infusion with inactive vehicle, beta 2-type adrenoreceptor activation decreased plasma and urinary potassium and phosphate and increased the excretion of calcium and magnesium. In addition, activation of the beta 2 adrenoreceptors did not influence creatinine clearance and plasma level and the net fractional excretion of sodium but increased the fractional clearance of exogenous lithium which measures the fraction of filtered sodium delivered by the proximal tubule. The results indicate that activation of beta 2-type adrenoreceptors decreases the proximal reabsorption of sodium.

Published
1993

43. [Disorders of puberty and gonadal disorders in the child]

Author

P E, Mullis

Subjects
Male, Puberty, Delayed, Adolescent, Humans, Puberty, Precocious, Female, Sexual Maturation, Child, Endocrine System Diseases, Gonadal Steroid Hormones
Abstract

Normal puberty has a characteristic harmony or consonance between the individual modalities of sexual maturation. Thus, the objective description and detailed knowledge of physical pubertal development is the basis of the clinical analysis of pubertal disorders. An aim of the review is to provide details of the visible changes the clinician must note in order to document the normal progression of puberty. Disorders of puberty can be classified by the timing of onset of sexual characteristics into either precocious or delayed puberty. A more useful concept, however, than the abnormalities of timing of puberty is whether the pubertal development is true (consonant) or if there is a pseudo-puberty (absence of consonance). This is of greater significance in relation to the pathophysiology and, therefore, the investigations and therapies which will be required. The use of either well known or new agents that may be used for treatment of pubertal disorders are presented.

Published
1992

44. TURNER'S SYNDROME: EFFECT OF GROWTH HORMONE AND/OR OXANDROLONE ON HEIGHT VELOCITY AND TURNER SPECIFIC BONE AGE TAKING THE AGE OF ONSET OF TREATMENT INTO ACCOUNT

Author

P.-E. Mullis, C.J. Partsch, E.E. Joss, and W.G. Sippell

Subjects
medicine.medical_specialty, business.industry, Growth data, Human growth hormone, Oxandrolone, Bone age, Turner's syndrome, Growth hormone, Endocrinology, Internal medicine, Pediatrics, Perinatology and Child Health, Medicine, Age of onset, business, medicine.drug
Abstract

Girls with Turner's Syndrome (TS) were treated with three different regimens: a) Oxandrolone (Oxa) 0.1 mg/kg/day, b) recombinant human growth hormone (rhGH) 28 U/m2/week and c) rhGH 24 U/m2/week with Oxa 0.06 mg/kg/day (mGH+Oxa). Growth data are presented for the first two years of treatment. None of the girls were given any estrogens. Bone age (BA) was assessed by the TW2-RUS method and expressed in Turner specific bone age (BATS) based on the mean BA data for untreated TS (1). Therefore, in contrast to using BA deriving from non affected girls, the increase in BATS in untreated TS is by definition 1 year/ year at any age.

Published
1993

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