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猪、豚鼠、小牛和人类海马体中α1-肾上腺素能受体的亚型:区域差异

Subtypes of alpha 1-adrenoceptors in hippocampus of pigs, guinea-pigs, calves and humans: regional differences.

作者信息

Hoyer D, Jones C R, Ford W, Palacios J M

机构信息

Preclinical Research, Sandoz Ltd., Basel, Switzerland.

出版信息

Eur J Pharmacol. 1990 Jan 23;188(1):9-16. doi: 10.1016/0922-4106(90)90242-p.

Abstract

Radioligand binding studies were performed with membranes of guinea-pig, pig, calf and human hippocampus using [125I]BE 2254 (also known as [125I]HEAT) as the radioligand. [125I]BE 2254 bound with similar high affinity to saturable populations of recognition sites in all four membrane preparations. Competition curves obtained with a variety of ligands (e.g., WB 4101, benoxathian, 5-methyl-urapidil) were biphasic and the profiles of the high- and low-affinity components of [125I]BE 2254 binding were similar in all four membrane preparations. The data suggest that [125I]BE 2254 labels two subtypes of alpha 1-adrenoceptors in the hippocampus of these species. [3H]WB 4101 was used to label alpha 1A recognition sites in pig hippocampus membranes. [3H]WB 4101 recognized with high affinity an apparently homogeneous class of sites, as suggested by monophasic saturation and competition experiments. The rank order of affinity of the compounds for the high-affinity component of [125I]BE 2254 binding was similar to the rank order of affinity of these drugs for [3H]WB 4101 sites. The pharmacological profile of the low-affinity component of [125I]BE 2254 binding was similar to that described recently for the alpha 1B-adrenoceptor cloned from DDT1 cells. In autoradiographic studies with human hippocampal slices, CEC (chloroethylclonidine), an alkylating agent described to show selectivity for alpha 1B-adrenoceptors, displaced preferentially [125I]BE 2254 binding from the molecular layer of the dentate gyrus. In contrast, WB 4101 an alpha 1A-adrenoceptor-selective ligand, displaced preferentially [125I]BE 2254 binding in the hilus and the CA3 region. The data show that 2 subtypes of alpha 1-adrenergic recognition sites can be identified in the hippocampus.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

使用[125I]BE 2254(也称为[125I]HEAT)作为放射性配体,对豚鼠、猪、小牛和人类海马体的膜进行了放射性配体结合研究。[125I]BE 2254以相似的高亲和力与所有四种膜制剂中可饱和的识别位点群体结合。用多种配体(如WB 4101、贝诺沙硫因、5-甲基-乌拉地尔)获得的竞争曲线是双相的,并且在所有四种膜制剂中,[125I]BE 2254结合的高亲和力和低亲和力成分的图谱相似。数据表明,[125I]BE 2254标记了这些物种海马体中α1肾上腺素能受体的两种亚型。[3H]WB 4101用于标记猪海马体膜中的α1A识别位点。单相饱和和竞争实验表明,[3H]WB 4101以高亲和力识别一类明显同质的位点。化合物对[125I]BE 2254结合高亲和力成分的亲和力排序与这些药物对[3H]WB 4101位点的亲和力排序相似。[125I]BE 2254结合低亲和力成分的药理学特征与最近描述的从DDT1细胞克隆的α1B肾上腺素能受体相似。在对人类海马体切片的放射自显影研究中,据描述对α1B肾上腺素能受体具有选择性的烷基化剂CEC(氯乙可乐定)优先取代齿状回分子层中的[125I]BE 2254结合。相反,α1A肾上腺素能受体选择性配体WB 4101优先取代海马门和CA3区域中的[125I]BE 2254结合。数据表明,在海马体中可以识别出两种α1肾上腺素能识别位点亚型。(摘要截断于250字)

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