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啮齿动物肥大细胞对溶血磷脂酰丝氨酸的不同反应。

Different responses of rodent mast cells to lysophosphatidylserine.

作者信息

Boarato E, Mietto L, Toffano G, Bigon E, Bruni A

出版信息

Agents Actions. 1984 Jun;14(5-6):613-8. doi: 10.1007/BF01978895.

Abstract

The lysophosphatidylserine-induced activation of mast cells has been studied in preparations obtained from different rodents. In mouse and gerbil peritoneal mast cells lysophosphatidylserine behaves as an agonist, inducing noncytotoxic histamine release at 0.2-8 microM. In rat peritoneal and pleural mast cells lysophosphatidylserine is ineffective, but the histamine-releasing activity becomes manifest upon the addition of suboptimal concentrations of other mast cell activators. The common structure-activity relationship shows the link between these effects of lysophosphatidylserine but the calcium requirement indicates differences in the mechanism of action. Histamine release in mouse mast cells is independent of external calcium. Thus, lysophosphatidylserine induces mobilization of endogenous calcium stores in these cells. By contrast, histamine release in gerbil and rat mast cells is dependent on the addition of external calcium indicating that the phospholipid promotes calcium influx. While in gerbil mast cells calcium influx is promoted by lysophosphatidylserine alone, in rat it requires the combined action of the phospholipid and other mast cell agonists. Differently from lysophosphatidylserine, compound 48/80 elicits histamine release in rat and gerbil mast cells. Mouse mast cells are unaffected. Thus, gerbil mast cells are the only preparation in which the action of these two agonists can be observed simultaneously.

摘要

溶血磷脂酰丝氨酸诱导肥大细胞活化的研究已在从不同啮齿动物获得的制剂中展开。在小鼠和沙鼠的腹膜肥大细胞中,溶血磷脂酰丝氨酸表现为一种激动剂,在0.2 - 8微摩尔浓度下诱导无细胞毒性的组胺释放。在大鼠的腹膜和胸膜肥大细胞中,溶血磷脂酰丝氨酸无效,但在添加次优浓度的其他肥大细胞激活剂后,组胺释放活性会显现出来。常见的构效关系显示了溶血磷脂酰丝氨酸这些效应之间的联系,但对钙的需求表明其作用机制存在差异。小鼠肥大细胞中的组胺释放不依赖于细胞外钙。因此,溶血磷脂酰丝氨酸在这些细胞中诱导内源性钙库的动员。相比之下,沙鼠和大鼠肥大细胞中的组胺释放依赖于添加细胞外钙,这表明该磷脂促进钙内流。虽然在沙鼠肥大细胞中,溶血磷脂酰丝氨酸单独就能促进钙内流,但在大鼠中,这需要磷脂和其他肥大细胞激动剂的共同作用。与溶血磷脂酰丝氨酸不同,化合物48/80能在大鼠和沙鼠肥大细胞中引发组胺释放。小鼠肥大细胞不受影响。因此,沙鼠肥大细胞是唯一能同时观察到这两种激动剂作用的制剂。

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