Binding Characteristics of a Histamine H<SUB>3</SUB>-Receptor Antagonist, [<SUP>3</SUP>H]S-Methylthioperamide: Comparison with [<SUP>3</SUP>H](<I>R</I>)α-Methylhistamine Binding to Rat Tissues
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概要
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The release and synthesis of neuronal histamine are regulated by histaminergic autoreceptors named as histamine H<SUB>3</SUB> receptors. The development of radiolabeled histamine H<SUB>3</SUB> antagonists is needed to characterize the binding of antagonists to these receptors. Here we describe the binding characteristics of a new histamine H<SUB>3</SUB>-receptor antagonist, [<SUP>3</SUP>H]<I>S</I>-methylthioperamide (SMT), to rat tissues, and compare its binding with that of [<SUP>3</SUP>H](<I>R</I>)α-methylhistamine ((<I>R</I>)αMH), a selective histamine H<SUB>3</SUB>-receptor agonist. The binding of [<SUP>3</SUP>H]SMT to the membranes of rat forebrain was found to be stereoselective, saturable, reversible and temperature-dependent. Saturation binding experiments indicated a single class of high affinity sites for [<SUP>3</SUP>H]SMT in forebrain membranes (K<SUB>D</SUB>=2.1 nM, B<SUB>max</SUB>=24.3 pmol/g of tissue at 4°C). The B<SUB>max</SUB> was approximately 3 times that of [<SUP>3</SUP>H](<I>R</I>)αMH binding to rat forebrain membranes (K<SUB>D</SUB>=2.5 nM, B<SUB>max</SUB>=7.3 pmol/g of tissue at 25°C). Autoradiographic images of [<SUP>3</SUP>H]SMT binding in the brain were essentially the same as those of [<SUP>3</SUP>H](<I>R</I>)αMH. [<SUP>3</SUP>H]SMT also bound appreciably to peripheral tissues (the liver, adrenal, stomach, ileum, kidney, lung and bladder), whereas the [<SUP>3</SUP>H](<I>R</I>)αMH bindings to these peripheral tissues were negligible. These results indicate that [<SUP>3</SUP>H]SMT binds to H<SUB>3</SUB> receptors primarily in the central nervous system, and that it also has high affinity toward non-H<SUB>3</SUB> receptors, probably hemoproteins, in peripheral tissues.
著者
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Ryu Jong
Department Of Life And Nanopharmaceutical Sciences And Department Of Pharmaceutical Science Kyung He
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Iwata Ren
Cyclotron And Radioisotope Center Tohoku University
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Ido Tatsuo
Cyclotron And Radioisotope Center Tohoku University
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Takahashi Toshihiro
Cyclotron And Radioisotope Center Tohoku University
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Watanabe Takehiko
Department Of Mechanical Engineering Niigata University
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IDO Tatsuo
Cyclotron and Radioisotope Center, Tohoku University
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Iwata Ren
Cyclotron and Radioisotope Center, Tohoku University
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Yanai Kazuhiko
Department of Pharmacology I, Tohoku University School of Medicine
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Ryu Jong
Department of Pharmacology I, Tohoku University School of Medicine
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Sakai Naruhiko
Department of Pharmacology I, Tohoku University School of Medicine
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Murakami Kazuki
Green Cross Corporation
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