[I-125] CGP-42112 BINDING REVEALS DIFFERENCES BETWEEN RAT-BRAIN AND ADRENAL AT2-RECEPTOR BINDING-SITES

被引:22
作者
SPETH, RC
机构
[1] Department of Veterinary and Comparative Anatomy, Pharmacology and Physiology, Washington State University, Pullman, WA
关键词
ANGIOTENSIN-II RECEPTOR; LIGAND CGP42112; BETA-MERCAPTOETHANOL; BINDING AFFINITY;
D O I
10.1016/0167-0115(93)90242-Z
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The AT2 angiotensin II receptor selective ligand CGP42112 was radioiodinated and used to study AT2 receptor binding sites in the rat brain (combined olfactory bulb, septum, thalamus and midbrain) and whole adrenal. The [I-125]CGP 42112 binding was of high affinity, saturable and specific in both tissues. Competition studies with nonselective and angiotensin II receptor subtype selective ligands, and evaluation of the effects of the sulfhydryl reducing agent fl-mercaptoethanol, confirmed that [ I-125] CGP 42112 bound selectively to the AT2 angiotensin II receptor subtype. [I-125]CGP 42112 bound with higher affinity in the brain than in the adrenal. Beta-Mercaptoethanol enhanced [I-125]CGP 42112 binding in the brain, but did not alter its binding in the adrenal. A similar difference in binding affinity for [I-125]Sarcosine1,isoleucine8 angiotensin II and enhancement of binding affinity by beta-mercaptoethanol was observed in the rat brain and adrenal. These observations suggest that the AT2 angiotensin II receptor subtypes in the brain and adrenal may differ.
引用
收藏
页码:189 / 197
页数:9
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