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腺苷A2受体介导的II型肺上皮细胞中磷脂酰胆碱的分泌

Adenosine A2-receptor-mediated phosphatidylcholine secretion in type II pneumocytes.

作者信息

Griese M, Gobran L I, Douglas J S, Rooney S A

机构信息

Department of Pediatrics, Yale University School of Medicine, New Haven, Connecticut 06510.

出版信息

Am J Physiol. 1991 Feb;260(2 Pt 1):L52-60. doi: 10.1152/ajplung.1991.260.2.L52.

DOI:10.1152/ajplung.1991.260.2.L52
PMID:1996663
Abstract

Adenosine and its analogues stimulate phosphatidylcholine secretion in cultured rat type II pneumocytes. There is evidence that this effect is mediated by A2 receptors. We have now employed the radioligand 5'(N-ethylcarboxyamido)adenosine (NECA) in an attempt to study the adenosine receptor in a membrane fraction of type II cells. Specific binding of [3H]-NECA was saturable with a total binding capacity (Bmax) of 4.91 pmol/mg protein and a dissociation constant (Kd) of 240 nM. The Kd was similar to the concentration of NECA which half-maximally stimulated phosphatidylcholine secretion (EC50, 150 nM). Although the relative potency of adenosine analogues in displacing bound [3H]NECA was consistent with that expected at an A2 receptor, there were discrepancies between binding and function with respect to some agonists as well as the antagonist xanthine amine congener (XAC). This together with the unusually high Bmax suggests that the NECA binding site is not the adenosine receptor mediating phosphatidylcholine secretion. The receptor was further characterized functionally by measuring its antagonist dissociation constant (Kb). KbS for XAC inhibition of the effects of NECA, N6-(L-2-phenylisopropyl)adenosine, and adenosine on phosphatidylcholine secretion were 19 +/- 8, 24 +/- 11, and 6 +/- 12 nM, respectively, suggesting that all three agonists act at the same receptor. The Kb value allowed comparison of the receptor in type II cells with that in other tissues and revealed that it was similar to the A2 receptor previously described in human platelets. These functional data further characterize and are consistent with a physiological role for the adenosine A2 receptor in the regulation of lung surfactant secretion.

摘要

腺苷及其类似物可刺激培养的大鼠II型肺细胞分泌磷脂酰胆碱。有证据表明,这种作用是由A2受体介导的。我们现在使用放射性配体5'(N-乙基甲酰胺基)腺苷(NECA)来研究II型细胞细胞膜组分中的腺苷受体。[3H]-NECA的特异性结合具有饱和性,总结合容量(Bmax)为4.91 pmol/mg蛋白质,解离常数(Kd)为240 nM。该Kd与半最大刺激磷脂酰胆碱分泌的NECA浓度(EC50,150 nM)相似。尽管腺苷类似物在置换结合的[3H]NECA方面的相对效力与A2受体预期的一致,但在一些激动剂以及拮抗剂黄嘌呤胺类似物(XAC)方面,结合和功能之间存在差异。这与异常高的Bmax一起表明,NECA结合位点不是介导磷脂酰胆碱分泌的腺苷受体。通过测量其拮抗剂解离常数(Kb)对该受体进行了进一步的功能表征。XAC抑制NECA、N6-(L-2-苯异丙基)腺苷和腺苷对磷脂酰胆碱分泌作用的KbS分别为19±8、24±11和6±12 nM,表明这三种激动剂作用于同一受体。Kb值允许将II型细胞中的受体与其他组织中的受体进行比较,并表明它与先前在人血小板中描述的A2受体相似。这些功能数据进一步表征了腺苷A2受体在调节肺表面活性物质分泌中的生理作用,且与之相符。

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