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三种腺苷受体类型的功能特性

Functional characterization of three adenosine receptor types.

作者信息

Gurden M F, Coates J, Ellis F, Evans B, Foster M, Hornby E, Kennedy I, Martin D P, Strong P, Vardey C J

机构信息

Pharmacology Division, Glaxo Group Research, Ware, Hertfordshire.

出版信息

Br J Pharmacol. 1993 Jul;109(3):693-8. doi: 10.1111/j.1476-5381.1993.tb13629.x.

Abstract
  1. The purpose of the present study was to classify adenosine receptors into A1 and A2 subtypes in a wide range of isolated tissues and cell types (rat adipocytes and atria, guinea-pig ileum and atria (A1); guinea-pig aorta, dog coronary artery and human platelets and neutrophils (A2)) using the R- and S-diastereoisomers of N-phenylisopropyladenosine (PIA), N-cyclopentyladenosine (CPA), the novel compound, N-[(1S,trans)-2-hydroxycyclopentyl]adenosine (GR79236), N-[(2-methylphenyl)methyl]adenosine (metrifudil), 2-(phenylamino)adenosine (CV1808), and 2[[2-[4-(2-carboxyethyl)phenyl]ethyl]amino]-N- ethylcarboxamidoadenosine (CGS21680); N-ethylcarboxamidoadenosine (NECA) was used as a standard. 2. Results obtained in all tissue preparations previously reported to contain A1-receptors could be described by a single rank order of agonist potency: CPA > or = GR79236, R-PIA > or = NECA >> S-PAI > or = metrifudil > or = CV1808, CGS21680. 3. In contrast, two distinct rank orders of agonist potency were observed in preparations previously reported to contain A2-receptors. In dog coronary artery, human neutrophils and platelets the rank order of potency was: CV1808, CGS21680 > or = NECA > R-PIA > or = metrifudil > or = CPA > GR79236 S-PIA. However, in guinea-pig aorta the rank order was: NECA > metrifudil > R-PIA, CPA > CV1808, GR79236 > or = S-PIA, CGS21680. 4. The results of this study are consistent with the existence of three types of adenosine receptor: A1-and two subtypes of A2-receptor. The receptor present in dog coronary artery, human platelets and neutrophils, probably corresponds to the A2a subtype, whilst that present in the guinea-pig aorta may be of the A2b subtype.
摘要
  1. 本研究的目的是在多种分离组织和细胞类型(大鼠脂肪细胞和心房、豚鼠回肠和心房(A1);豚鼠主动脉、犬冠状动脉、人血小板和中性粒细胞(A2))中,使用N-苯基异丙基腺苷(PIA)、N-环戊基腺苷(CPA)的R-和S-非对映异构体、新型化合物N-[(1S,反式)-2-羟基环戊基]腺苷(GR79236)、N-[(2-甲基苯基)甲基]腺苷(美曲氟地尔)、2-(苯基氨基)腺苷(CV1808)以及2[[2-[4-(2-羧乙基)苯基]乙基]氨基]-N-乙基羧酰胺腺苷(CGS21680)将腺苷受体分为A1和A2亚型;N-乙基羧酰胺腺苷(NECA)用作标准物。2. 在先前报道含有A1受体的所有组织制剂中获得的结果可用单一的激动剂效价顺序来描述:CPA≥GR79236,R-PIA≥NECA>>S-PAI≥美曲氟地尔≥CV1808,CGS21680。3. 相比之下,在先前报道含有A2受体的制剂中观察到两种不同的激动剂效价顺序。在犬冠状动脉、人中性粒细胞和血小板中,效价顺序为:CV1808,CGS21680≥NECA>R-PIA≥美曲氟地尔≥CPA>GR79236>S-PIA。然而,在豚鼠主动脉中,效价顺序为:NECA>美曲氟地尔>R-PIA,CPA>CV1808,GR79236≥S-PIA,CGS21680。4. 本研究结果与三种类型腺苷受体的存在一致:A1受体以及A2受体的两个亚型。存在于犬冠状动脉、人血小板和中性粒细胞中的受体可能对应于A2a亚型,而存在于豚鼠主动脉中的受体可能是A2b亚型。

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