Specific binding of 125I-salmon calcitonin to rat brain: Regional variation and calcitonin specificity.
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概要
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Rat brain particulate fraction was found to contain binding sites for <SUP>125</SUP>I-Salmon Calcitonin-I (<SUP>125</SUP>I-SCT). Maximum binding occurred in the physiological pH range of 7.25-7.5. The binding reaction proceeded in a temperature-dependent manner. Binding sites were broadly distributed among the various rat brain regions and considerable regional differences existed in the affinity and density as detected by Scatchard analysis. The highest affinity was recorded in the case of the hypothalamus and the lowest in the case of the cerebellum. The KD (nM) and Bmax (pmole/mg protein) estimated for the binding to four regions were as follows: hypothalamus: 1.4 and 0.19, midbrain, hippocampus plus striatum: 1.5 and 0.08, pons plus medulla oblongata: 3.0 and 0.15 and cerebellum: 8.3 and 0.20. Using a particulate fraction of rat brain void of cerebellum and cortices, a binding assay for calcitonins was developed. Binding of <SUP>125</SUP>I-SCT was inhibited by unlabeled salmon, [Asu<SUP>1, 7</SUP>]-eel and porcine calcitonins in a dose-dependent manner and the IC50s were 2.0, 8.0 and 30 nM, respectively. The IC50s were comparable to those estimated using a kidney particulate fraction. Human calcitonin, β-endorphin and substance P were weak inhibitors of the binding. Other peptides, drugs and putative neurotransmitters tested (totally 23 substances) failed to inhibit the binding at concentrations of 1.0 μM. The physiological significance of brain binding sites for calcitonin, with the possiblity that the brain may possess endogenous ligands for these sites are discussed.
- 公益社団法人 日本薬理学会の論文
著者
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Yajima Haruaki
Faculty Of Pharmaceutical Sciences Kyoto University
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ORLOWSKI Ronald
Armour Pharmaceutical Company
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FURUKAWA Shinichi
Faculty of Pharmaceutical Sciences, Nagasaki University
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SCHLUETER R.
Armour Pharmacertical Company
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Nakamuta Hiromichi
Faculty of Pharmaceutical Sciences, Nagasaki University
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KOIDA Masao
Faculty of Pharmaceutical Sciences, Nagasaki University
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ORLOWSKI Ronald
Armour Pharmacertical Company
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YAJIMA HARUAKI
Faculty of Pharmaceutical Science, Kyoto University
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