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抗过敏药奥沙米特的P2X7受体拮抗剂活性。

P2X7 receptor antagonist activity of the anti-allergic agent oxatomide.

作者信息

Yoshida Kazuki, Ito Masaaki, Matsuoka Isao

机构信息

Laboratory of Pharmacology, Faculty of Pharmacy, Takasaki University of Health and Welfare, 60 Nakaorui-machi, Takasaki-shi, Gunma 370-0033, Japan.

出版信息

Eur J Pharmacol. 2015 Nov 15;767:41-51. doi: 10.1016/j.ejphar.2015.10.002. Epub 2015 Oct 16.

Abstract

Activation of the P2X7 receptor by extracellular ATP is associated with various immune responses including allergic inflammation. Anti-allergic agents, such as H1-antihistamines, are known to inhibit the effects of different chemical mediators such as acetylcholine and platelet-activating factor. Therefore, we hypothesized that some anti-allergic agents might affect P2X7 receptor function. Using N18TG2 and J774 cells, which express functional P2X7 receptors, the effects of several anti-allergic agents on P2X7 receptor function were investigated by monitoring the ATP-induced increase in intracellular Ca(2+) concentrations ([Ca(2+)]i). Among the various agents tested, oxatomide significantly inhibited P2X7 receptor-mediated [Ca(2+)]i elevation in a concentration-dependent manner without affecting the P2Y2 receptor-mediated response in both N18TG2 and J774 cells. Consistently, oxatomide inhibited P2X7 receptor-mediated membrane current and downstream responses such as mitogen-activated protein kinase activation, inflammation-related gene induction, and cell death. In addition, oxatomide inhibited P2X7 receptor-mediated degranulation in mouse bone marrow-derived mast cells. Whole cell patch clamp analyses in HEK293 cells expressing human, mouse, and rat P2X7 receptors revealed that the inhibitory effect of oxatomide on ATP-induced current was most prominent for the human P2X7 receptor and almost non-existent for the rat P2X7 receptor. The potent inhibitory effects of oxatomide on human P2X7 receptor-mediated function were confirmed in RPMI8226 human B cell-like myeloma cells, which endogenously express the P2X7 receptor. Our results demonstrated that the antihistamine oxatomide also acts as a P2X7 receptor antagonist. Future studies should thus evaluate whether P2X7 receptor antagonism contributes to the anti-allergic effects of oxatomide.

摘要

细胞外ATP激活P2X7受体与包括过敏性炎症在内的多种免疫反应相关。抗组胺药等抗过敏药物已知可抑制乙酰胆碱和血小板活化因子等不同化学介质的作用。因此,我们推测一些抗过敏药物可能会影响P2X7受体功能。利用表达功能性P2X7受体的N18TG2和J774细胞,通过监测ATP诱导的细胞内Ca(2+)浓度([Ca(2+)]i)升高,研究了几种抗过敏药物对P2X7受体功能的影响。在测试的各种药物中,奥沙米特以浓度依赖的方式显著抑制P2X7受体介导的[Ca(2+)]i升高,而不影响N18TG2和J774细胞中P2Y2受体介导的反应。同样,奥沙米特抑制P2X7受体介导的膜电流和下游反应,如丝裂原活化蛋白激酶激活、炎症相关基因诱导和细胞死亡。此外,奥沙米特抑制小鼠骨髓来源肥大细胞中P2X7受体介导的脱颗粒。在表达人、小鼠和大鼠P2X7受体的HEK293细胞中进行的全细胞膜片钳分析表明,奥沙米特对ATP诱导电流的抑制作用在人P2X7受体中最为显著,而在大鼠P2X7受体中几乎不存在。奥沙米特对人P2X7受体介导功能的强效抑制作用在内源性表达P2X7受体的RPMI8226人B细胞样骨髓瘤细胞中得到证实。我们的结果表明,抗组胺药奥沙米特也可作为P2X7受体拮抗剂。因此,未来的研究应评估P2X7受体拮抗作用是否有助于奥沙米特的抗过敏作用。

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