Induction of Human Endometrial Estradiol Dehydrogenase by Progestins

Tseng, Linda; Gurpide, Erlio

doi:10.1210/endo-97-4-825

Cited by 297 publications

(77 citation statements)

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“…This observation is supported by the comparison of the sedimentation patterns of nucleus-bound steroid hormone receptors from normal myometrium in the middle proliferative and early secretory phases and from leiomyoma, and by kinetics of steroid hormone transfer from the cytoplasm to the nucleus under equilibrium conditions. (29,30) and our group (10) on human endometrium have shown, is subject to the inductive effect of the progesterone receptor mechanism. One can only speculate on the cause and pathophysiological significance of the differences in progesterone receptor contents of normal myometrium and leiomyoma: Since, as animal experiments have shown, the progesterone receptor is induced via the estradiol receptor mechanism, and thus represents an end product of the chain of estradiol action, it can be inferred that an alteration at one of the steps sur> sequent to the translpeation of the estradiol receptor (transcription, processing, translation) leads to the "progesterone receptor defect".…”

Section: Discussionmentioning

confidence: 90%

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Estrogen and Progesterone Binding Proteins in Normal Human Myometrium and Leiomyoma Tissue

Pollow¹,

Geilfuss²,

Boquoi³

et al. 1978

Clinical Chemistry and Laboratory Medicine

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Summary: The occurrence and characteristics of macromolecular components of normal human myometrium and leiomyoma which bind [ 3 H]estradiol and [ 3 H]progesterone were investigated, employing dextran coated charcoal, density gradient centrifugation and gel filtration techniques.On sucrose density gradient centrigugation, [ 3 H]progesterone was bound by macromolecules with sedimentation rates of about 4 S and 8 S.The major [ 3 H]progesterone binding component had a sedimentation coefficient of about 4 S, which contained specific and nonspecific binding sites.Sedimentation patterns as well as elution profiles from agarose gel revealed a striking similarity between biochemical properties of the progesterone receptors from normal myometrium and leiomyomas of the same organ.Both progesterone and estradiql receptor change in concentration during the normal menstrual cycle. During the early proliferative phase the number of estradiol receptor binding sites was highest; after ovulation, a rapid decrease of estradiol receptor level was seen. On the other hand, using [ 3 H]progesterone as the ligand, the highest receptor concentration was found at midcycle.The leiomyoma steroid hormone receptor levels were compared with those in normal myometrium. Whereas leiomyoma exhibited higher estradiol binding capacity, the concentration of progesterone receptors was low in fibroid tumors. In normalem Gewebe variieren die Prqgesterqn-sowie Östradiol-Rezeptorkonzentrationen in der Cytoplasmafraktion. Die höchsten Östradiol-Rezeptorbindungsaktivitäten wurden während der frühen Proliferationsphase beobachtet; nach Oviüation kommt es zu einem rapiden Abfall der Östradipl-Rezeptorkohzentration. Die höchsten ProgesteronRezeptorkonzentratipnen zeichneten sich ab in der Mitte des Menstruationszyklus zum Zeitpunkt der Ovulation. Myome waren charakterisiert durch hohe Östradiql-Bindungskäpazität und eine niedrigere Progesteron-Rezeptorkonzentration. Östrogen-und Progesterön-Rezeptören in normalem Human-Myometrium und Myomen

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Section: Discussionmentioning

confidence: 90%

“…The result is that the estradiol receptor mechanism, which is responsible for both its own induction and that of the progesterone receptor, is blocked (10,29,30).…”

Section: Discussionmentioning

confidence: 99%

Estrogen and Progesterone Binding Proteins in Normal Human Myometrium and Leiomyoma Tissue

Pollow¹,

Geilfuss²,

Boquoi³

et al. 1978

Clinical Chemistry and Laboratory Medicine

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“…Although estrone is weakly estrogenic, it exhibits a lower binding affinity for ERs than estradiol, and it diffuses out of the cell more rapidly than estradiol. In the myometrium, the activity of this enzyme is maximal during the early secretory phase because of upregulation by progesterone (Tseng and Gurpide 1973), resulting in a diminished estradiol effect during the second half of the cycle. In leiomyomas, on the other hand, the reduced activity of 17β-hydroxysteroid dehydrogenase may allow for the accumulation of estradiol in the cells during the secretory as well as the proliferative phase of the cycle, thus resulting in continual stimulation by estrogen, with upregulation of both the ERs and PRs, accompanied by the associated growth-promoting effects.…”

Section: Review | Uterine Leiomyomamentioning

confidence: 99%

Etiology and pathogenesis of uterine leiomyomas: a review.

Flake

Andersen

Dixon

2003

Environ Health Perspect

496

392

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Uterine leiomyomas, or fibroids, represent a major public health problem. It is believed that these tumors develop in the majority of American women and become symptomatic in one-third of these women. They are the most frequent indication for hysterectomy in the United States. Although the initiator or initiators of fibroids are unknown, several predisposing factors have been identified, including age (late reproductive years), African-American ethnicity, nulliparity, and obesity. Nonrandom cytogenetic abnormalities have been found in about 40% of tumors examined. Estrogen and progesterone are recognized as promoters of tumor growth, and the potential role of environmental estrogens has only recently been explored. Growth factors with mitogenic activity, such as transforming growth factor-β 3, basic fibroblast growth factor, epidermal growth factor, and insulin-like growth factor-I, are elevated in fibroids and may be the effectors of estrogen and progesterone promotion. These data offer clues to the etiology and pathogenesis of this common condition, which we have analyzed and summarized in this review.

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“…These may change the state of equilibrium between estradiol and estrone to some extent, though from studies on the human placental 17/J-hydroxysteroid dehydrogenase (24,25) it has been shown that under physiological conditions the equilibrium of the reaction lies on the side of estrone. Furthermore it has been shown by supervision experiments with human endometrium (20)(21)(22), that estrone (in contrast to estradiol) is not accumulated in the target cell. This observation seems all the more important since estrone is known to compete for specific estradiol receptor and enzyme binding-sites.…”

Section: Kinetic Analysesmentioning

confidence: 99%

“…an increase in enzyme activity is observed in vitro and in vivo after estrogen pretreatment followed by progesterone application (this can be blocked by inhibitors of protein synthesis); 2. there is a positive correlation between microsomal 17/J-hydroxysteroid dehydrogenase activity and progesterone receptor concentration; and 3. endometrial carcinomas only react to high-dose gestagen therapy with an increase in their 170-hydroxysteroid dehydrogenase activity if they possess adequate levels of progesterone receptors. For human myometrium there is less substantial evidence for a progesterone induced synthesis of the 17β-hydroxysteroid dehydrogenase than for human endometrium (20)(21)(22)(23). Other causes for a postovulatory increase of enzyme activity in human myometrium therefore have to be taken into consideration, such as intracellular proton concentration or the redox state…”

mentioning

confidence: 99%

In Vitro Conversion of Estradiol-17β into Estrone in Normal Human Myometrium und Leiomyoma

Pollow¹,

Sinnecker²,

Boquoi³

et al. 1978

Clinical Chemistry and Laboratory Medicine

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Summary:The specific activity of 170-hydroxysteroid dehydrogenase was measured in normal human myometrium, and in leiomyoma specimens obtained from the same tumor-bearing uterus. In all cases the normal tissue showed greater conversion of estradiol-17/3 into estrone than the neoplastic tissues. In normal myometrium of fertile women, the specific enzyme activity depended on the phase of the menstrual cycle, the highest values of 170-hydroxysteroid dehydrogenase activity being found in the early secretory phase.To determine the intracellular distribution of the 17/3-hydroxysteroid dehydrogenase, purified microsomes, mitochondria, nuclei and cytosol fractions were prepared. The purity of each fraction was monitored by marker enzymes. It was found that the enzyme was mainly located in mitochondria and microsomes. Furthermore it was demonstrated that the microsomal enzyme was bound tightly to the membranes of the endoplasmic reticulum, while the mitochondrial 17j34iydroxysteroid dehydrogenase was mainly associated with the outer membranes of the organelle.Kinetic parameters (K m -values, coenzyme requirements, temperature and pH-optima) of the cytoplasmic, nuclear, mitochondrial and microsomal enzyme of normal and neoplastic tissue were compared. In vitrO'Umwandlung von Östradiol-17ß in Östron in normalem Human-Myometrium und LeiomyomenZusammenfassung: Die spezifische Aktivität der 17|8-Hydroxysteroiddehydrogenase wurde in normalem HumanMyometrium und in Gewebeproben von Leiomyomen vergleichend gemessen. Die Gewebsproben wurden aus dem gleichen Tumor-tragenden Uterus gewonnen. Normalgewebe zeigte einen größeren Umsatz von Östradiol-170 zu Östron als Tumorgewebe. In Normal-Myometrium geschlechtsreifer Frauen variierte die spezifische Enzymaktivität in Abhängigkeit vom Menstruationszyklus: die höchsten Werte wurden in der frühen Sekretionsphase beobachtet.Um die intrazellulare Verteilung der 17|8-Hydroxysteroiddehydrogenase-Aktivität zu untersuchen, wurden hochgereinigte Mikrosomen, Mitochpndrien, Kerne und Cytoplasma präpariert. Der Reinheitsgrad der Fraktion wurde durch Leitenzyme charakterisiert. Die höchsten spezifischen Enzymaktivitäten wurden in Mitochondrien und Mikrosomen lokalisiert. Darüberhinaus wurde beobachtet, daß das mikrosomale Enzym fest mit der Membran des endoplasmatischen Retikulums verbunden ist, während die mitochondriale 17j3-Hydroxysteroiddehydrogenase mit der äußeren Membran der Mitochondrien assoziiert ist.Kinetische Parameter (K m -Werte, Coenzym-Abhängigkeit, Temperatur-und pH-Optima) des cytoplasmatischen, nuklearen, mitochondrialen und mikrosonialen Enzyms aus normalem und neoplastischem Gewebe wurden vergleichend untersucht.

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Induction of Human Endometrial Estradiol Dehydrogenase by Progestins

Cited by 297 publications

References 0 publications

Estrogen and Progesterone Binding Proteins in Normal Human Myometrium and Leiomyoma Tissue

Estrogen and Progesterone Binding Proteins in Normal Human Myometrium and Leiomyoma Tissue

Etiology and pathogenesis of uterine leiomyomas: a review.

In Vitro Conversion of Estradiol-17β into Estrone in Normal Human Myometrium und Leiomyoma

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