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外周多巴胺受体亚型的光学显微镜放射自显影术

Light microscope autoradiography of peripheral dopamine receptor subtypes.

作者信息

Amenta F

机构信息

Sezione di Anatomia Umana, Università di Camerino, Italy.

出版信息

Clin Exp Hypertens. 1997 Jan-Feb;19(1-2):27-41. doi: 10.3109/10641969709080802.

Abstract

Radioligand binding assay techniques associated with light microscope autoradiography were used for investigating the pharmacological profile and the micro anatomical localization of peripheral dopamine receptor subtypes. In systemic arteries, the predominant dopamine D1-like receptor belongs to the D5 (or D1B) subtype. It is located within smooth muscle of the tunica media. In pulmonary arteries, dopamine D1-like receptors have primarily an endothelial localization and belong to the dopamine D1 (or D1A) receptor subtype. Both systemic and pulmonary arteries express a dopamine D2-like receptor belonging to the D2 receptor subtype. It has a prejunctional localization in the majority of vascular beds investigated. In cerebral, coronary and mesenteric arteries, it has also an endothelial localization. In the heart, a dopamine D4 receptor was identified. It is expressed by atrial tissue and has a widespread distribution overall atrial musculature. The kidney expresses both dopamine D1-like and D2-like receptors. Renal dopamine D1-like receptors have a vascular and tubular localization. The majority of these sites belongs to the D5 receptor subtype. A smaller D1 receptor population has primarily a tubular localization. Renal dopamine D2-like receptors belong to the dopamine D3 subtype and in lesser amounts to the D2 and D4 receptor subtypes. Renal dopamine D3 receptor has to a greater extent a tubular localization, whereas the D4 receptor is located within glomerular arterioles. The above results suggest that radioligand binding assay and autoradiographic techniques, if performed in the presence of compounds displaying specific receptor subtype selectivity, may contribute to characterize, mainly from a quantitative point of view, peripheral dopamine receptors.

摘要

与光学显微镜放射自显影相关的放射性配体结合测定技术被用于研究外周多巴胺受体亚型的药理学特征和微观解剖定位。在体动脉中,主要的多巴胺D1样受体属于D5(或D1B)亚型。它位于中膜的平滑肌内。在肺动脉中,多巴胺D1样受体主要定位于内皮细胞,属于多巴胺D1(或D1A)受体亚型。体动脉和肺动脉均表达属于D2受体亚型的多巴胺D2样受体。在所研究的大多数血管床中,它具有突触前定位。在脑动脉、冠状动脉和肠系膜动脉中,它也有内皮定位。在心脏中,鉴定出一种多巴胺D4受体。它由心房组织表达,在整个心房肌中广泛分布。肾脏表达多巴胺D1样和D2样受体。肾多巴胺D1样受体具有血管和肾小管定位。这些位点中的大多数属于D5受体亚型。较小的D1受体群体主要定位于肾小管。肾多巴胺D2样受体属于多巴胺D3亚型,少量属于D2和D4受体亚型。肾多巴胺D3受体在更大程度上定位于肾小管,而D4受体位于肾小球小动脉内。上述结果表明,如果在存在显示特定受体亚型选择性的化合物的情况下进行放射性配体结合测定和放射自显影技术,可能有助于主要从定量角度表征外周多巴胺受体。

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