CHARACTERISTICS OF GLUCOCORTICOID-BINDING SITES OF RAT LIVER: DIFFERENT EFFECTS OF ADRENALECTOMY ON THE BINDING
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概要
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Hydrocortisone (HC) in rat liver cytoplasmic fraction was bound to three different binding sites with high, medium and low affinity. Dissociation constants (K<SUB>d</SUB>) were approx. 2.1, 22 and 208 nM; and the densities of these binding sites were about 40, 50 and 10% of total number of binding sites, respectively. The binding site for dexamethasone (DM) of the cytoplasmic fraction was the medium affinity one among these three components. The maximum number of binding sites (B<SUB>max</SUB>) of HC and DM was significantly increased by adrenalectomy. The B<SUB>max</SUB> of HC was about twice as great as that of DM in normal and adrenalectomized rat liver. DM inhibited <SUP>3</SUP>H-HC binding in a dose-dependent manner but inhibition did not exceed 50% in either normal or adrenalectomized rats. Following adrenalectomy, the B<SUB>max</SUB> of the medium affinity-site for HC was significantly increased, while the high affinity component disappeared. By adding DM to the cytoplasmic fraction of adrenalectomized rat liver in vitro and in vivo, the B<SUB>max</SUB> of the medium affinity-site was significantly decreased, and a high affinity component of HC was revealed with a significant increase in the number of binding sites. These results indicate that the binding site for DM is one component of the HC binding site; and following adrenalectomy, the number of each type of binding site for glucocorticoids increases differently from the others.
- 社団法人 日本薬理学会の論文
著者
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MURAMATSU MAKOTO
Research Center, Taisho Pharmaceutical Co., Ltd.
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TANAKA MAKOTO
Research Center, Taisho Pharmaceutical Co., Ltd.
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OTOMO SUSUMU
Research Center, Taisho Pharmaceutical Co., Ltd.
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AIHARA HIRONAKA
Research Center, Taisho Pharmaceutical Co., Ltd.
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Aihara Hironaka
Research Center Taisho Pharmaceutical Co. Ltd.
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Muramatsu Makoto
Research Center Taisho Pharmaceutical Co. Ltd.
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Muramatsu M
Institute Of Applied Physics University Of Tsukuba
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TANAKA Makoto
Research Center, Taisho Pharmaceutical Co., Ltd
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