Insulin preincubation effects on rat vessel contractile responses: role of the endothelium.

Endothelium-journal of Endothelial Cell Research Pub Date : 2001-01-01 DOI:10.3109/10623320109090804

A. Rebolledo, G. Rinaldi, V. Milesi, A. Gómez Alvis, A. O. Grassi de Gende

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引用次数: 3

Abstract

The effect of contractions elicited with ET1 and AVP after preincubating rat aortic and tail artery rings with a hyperinsulinemic dose (3 nM) of insulin were studied. Insulin preincubation (120 min), in the presence of 0.1 mM L-NAME, depressed contraction of aortic rings to 0.01 microM ET1 (132 +/- 6 vs. 161 +/- 9 mg/mm2 in control, n = 25; p < 0.05) and to 1 microM AVP (84 +/- 7 vs. 110 +/- 9 mg/mm2 in control, n = 16; p < 0.05), but did not modify 45Ca influx to the cell. Insulin-induced relaxation was inhibited by indomethacin 10 microM, an antagonist of prostaglandin synthesis, and also by blockade of insulin receptors with 30 microM genistein. A short insulin preincubation (15 min) did not modify ET1 contractions. In rat tail artery, insulin preincubation (120 min) increased the force developed by ET1 (847 +/- 45 vs. 596 +/- 99 mgF/mgW in controls, n = 14) by stimulating TXA2 release and/or actions. In summary, the present results suggest that endothelial factors are involved in both the vasoconstrictor and vasodilator effects of insulin on rat vessels.

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胰岛素对大鼠血管收缩反应的影响:内皮细胞的作用。

研究了高胰岛素剂量(3 nM)胰岛素预孵育大鼠主动脉和尾动脉环后，ET1和AVP诱导的收缩作用。胰岛素预孵育(120分钟)，在0.1 mM L-NAME存在的情况下，将主动脉环收缩降至0.01微米ET1(对照组为132 +/- 6，对照组为161 +/- 9 mg/mm2, n = 25;p < 0.05)和1 μ m AVP(对照组为84 +/- 7，对照组为110 +/- 9 mg/mm2, n = 16;p < 0.05)，但不改变45Ca向细胞内流。吲哚美辛(一种前列腺素合成拮抗剂)可抑制胰岛素诱导的松弛，染料木素(30 microM)可阻断胰岛素受体。短胰岛素预孵育(15分钟)没有改变ET1收缩。在大鼠尾动脉中，胰岛素预培养(120分钟)通过刺激TXA2释放和/或作用，增加了ET1产生的力(对照组为847 +/- 45，对照组为596 +/- 99 mg /mgW, n = 14)。综上所述，目前的结果表明，内皮因子参与了胰岛素对大鼠血管的收缩和扩张作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Endothelium-journal of Endothelial Cell Research

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