Calcium Channel, Ca⁺⁺ mobilization, and Mechanical Reactivity of Estrogen- and Progesterone-Treated Rat Uterus

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Properties of [³H]nitrendipine binding, high K⁺- and Ca⁺⁺-Induced contractions and the inhibition of high K⁺-induced contractions by verapamil were investigated in the uterine preparations isolated from rats treated with estrogen or progesterone or both. In [³H]nitrendipine binding experiments using crude membrane fractions, treatment with estrogen alone or estrogen+progesterone significantly lowered the K_D; There was very little change in the B_max. In the Ca⁺⁺-depleted, high K⁺-containing medium, only the progesterone-, and estrogen→progesterone-treated uteri produced contractions. The estrogen-, estrogen→progestereone-, and estrogen+progesterone-treated uteri showed decreases in concentrations of Ca⁺⁺ required for the maximal contractions. In the estrogen- and estrogen+progesterone-treated uteri, the dose-response curves by verapamil were shifted to the left in a parallel manner. These findngs suggest that estrogen appeared to increase the affinity of calcium channels and increase transmembrane influx of Ca⁺⁺, leading to enhancement of contractions, whereas progesterone might increase the Ca⁺⁺ storage in the intracellular sites.