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Dive into the research topics where Michael Oettel is active.

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The Journal of Steroid Biochemistry and Molecular Biology | 1997

Dehydroepiandrosterone stimulates the estrogen response element

Jan M. Bruder; Lothar Sobek; Michael Oettel

Studies suggest that the steroid, dehydroepiandrosterone (DHEA) can exert effects directly, in addition to its indirect role serving as a precursor for other steroids such as androgens and estrogens. Because DHEA is one of the most abundant adrenal steroids secreted in man, we investigated the functional activity of DHEA on the classic estrogen response element (ERE) in the presence of the estrogen receptor (ER) in transiently transfected cells. GT1-7 hypothalamic neuronal cells, devoid of the estrogen receptor, were transiently transfected with the estrogen receptor expression plasmid (HEGO) and the estrogen response element luciferase (ERELUC) reporter vector. As expected, a dose-response stimulation of luciferase activity was observed in cells treated with estradiol. Concentrations of estradiol from 10(-10)-10(-6) M resulted in a 136-195 percent increase in luciferase activity compared with control. A dose-response stimulation was also observed in the cells treated with DHEA. A maximum stimulation of 177 percent increase in luciferase activity compared with control was observed with DHEA at a concentration of 10(-5) M. Both the estradiol and DHEA stimulation of ERE luciferase activity was inhibited by the estrogen receptor antagonist, ICI 182,780. The aromatase inhibitor, formestane in combination with estradiol or DHEA had no effect on luciferase activity, suggesting that the effect of DHEA is independent of its conversion to estradiol. Estradiol levels, as measured by ELISA, were appropriately elevated in the estradiol-treated cells but were not significantly different from the control cells in the DHEA-treated cells. These studies suggest a functional in vitro role of DHEA in activating the ERE in the presence of the classic ER.


Archive | 2006

Pharmaceutical combinations for compensating for a testosterone deficiency in men while simultaneously protecting the prostate

Doris Hubler; Michael Oettel; Lothar Sobek; Walter Elger; Abdul-Abbas Al-Mudhaffar


Archive | 1999

Pharmaceutical preparations for treatment of estrogen deficiency in the central nervous system

Vladimir Patchev; Michael Oettel; Sigfrid Schwarz; Ina Thieme; Wolfgang Roemer


Archive | 1998

Pharmazeutische Kombinationen zum Ausgleich eines Testosteron-Defizits beim Mann mit gleichzeitigem Schutz der Prostata

Doris Dr Huebler; Michael Oettel; Lothar Sobek; Walter Elger; Abdul-Abbas Al-Mudhaffar


Archive | 1999

Use of biogenic estrogen sulfamates for hormone replacement therapy

Walter Elger; Pekka Lähteenmäki; Matti Lehtinen; Gudrun Reddersen; Holger Zimmermann; Michael Oettel; Sigfrid Schwarz


Archive | 1999

Bioadhesive tablet containing testosterone/testosterone ester mixtures and method for producing a predetermined testosterone time-release profile with same

Doris Huebler; Guenter Kaufmann; Michael Oettel; Holger Zimmermann; Michael Dittgen; Sabine Fricke; Manfred Boese; Ralf Ladwig; Sven Claussen; Carsten Timpe


Archive | 2001

Combination preparation for contraception based on natural estrogens

Michael Dittgen; Sabine Fricke; Herbert Prof Dr Hoffmann; Claudia Dr Moore; Michael Oettel; Monika Ostertag


Archive | 2004

Multistage preparation for contraception based on natural estrogens

Michael Dittgen; Sabine Fricke; Herbert Prof Dr Hoffmann; Claudia Dr Moore; Michael Oettel; Monika Oster Wald


Archive | 2002

Use of dehydroepiandrosterone and an estradiol derivative for preparing a medicament for treating postmenopausal climacteric disorders

Sabine Fricke; Doris Hübler; Michael Oettel; Vladimir Prof Dr. Patchev


Archive | 2000

17a-hydroxy-4-androstene-3-one and derivatives thereof

Michael Oettel; Jens Berlau; Wolfgang Römer; Gerhard Schreiber

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