内皮素通过ETB受体亚型收缩小鼠肝小静脉和肝窦。

Y Ito, M Katori, M Majima, A Kakita
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引用次数: 14

摘要

目的:探讨内皮素(ET)-1和ET-3对肝小静脉和肝窦的影响,并鉴定ET受体的亚型。方法:麻醉小鼠肝边缘观察肝小静脉和肝窦。ET-1, ET-3和sarafotoxin (S6c,一种选择性的ETB受体激动剂)局部应用于微血管。结果:ET-1、ET-3和S6c (1 ~ 100 μ m, 30微升)诱导门静脉、窦状静脉和中央静脉呈剂量依赖性收缩。ETs和S6c对这些微血管具有同等效力。BQ-123(一种选择性ETA受体拮抗剂)抑制ET-3(非ET-1)对门静脉和中央小静脉的收缩作用,而对窦状静脉没有抑制作用。结论:在小鼠肝小静脉和肝窦中,ET-1和ET-3诱导的血管收缩主要通过ETB受体亚型介导,部分通过门脉和中央小静脉中未知的bq -123敏感ET受体亚型介导,而仅通过ETB受体亚型介导。
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Constriction of mouse hepatic venules and sinusoids by endothelins through ETB receptor subtype.

Objective: This study was conducted to examine the effects of endothelin (ET)-1 and ET-3 on hepatic venules and sinusoids and to identify the subtypes of ET receptors.

Method: Hepatic venules and sinusoids of anesthetized mice were observed at the edge of the liver. ET-1, ET-3 and sarafotoxin (S6c, a selective ETB receptor agonist) were applied topically over the microvasculature.

Results: ET-1, ET-3 and S6c (1-100 microM, 30 microliters) induced dose-dependent vasoconstriction of the portal venules, the sinusoids and the central venules. The ETs and S6c were equipotent for these microvessels. BQ-123 (a selective ETA receptor antagonist) inhibited the constrictive effects of ET-3 (not of ET-1) on the portal venules and central venules, whereas it had no inhibitory effect on the sinusoids.

Conclusions: In mouse hepatic venules and sinusoids, the vasoconstriction induced by ET-1 and ET-3 was mediated mainly through the ETB receptor subtype and partly through an unknown BQ-123-sensitive ET receptor subtype in the portal and central venules, and only through the ETB receptor subtype in the sinusoids.

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