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将血管活性肠肽包裹于脂质体中:对体内血管舒张的影响。

Encapsulation of vasoactive intestinal peptide into liposomes: effects on vasodilation in vivo.

作者信息

Suzuki H, Noda Y, Paul S, Gao X P, Rubinstein I

机构信息

Department of Medicine, University of Illinois at Chicago, USA.

出版信息

Life Sci. 1995;57(15):1451-7. doi: 10.1016/0024-3205(95)02108-u.

Abstract

The purpose of this study was to determine whether encapsulation of vasoactive intestinal peptide (VIP) into liposomes potentiated its vasorelaxant effects in vivo. Using intravital microscopy, we measured the diameter of second-order arterioles (53 +/- 1 microns) in the hamster cheek pouch before, during and after suffusion of VIP, liposomes and VIP encapsulated into liposomes for 7 min. We found that VIP (0.05, 0.1 & 1.0 nmol) induced significant, time- and concentration-dependent vasodilation (9 +/- 1%, 13 +/- 3% and 14 +/- 1% increase from baseline values, respectively; mean +/- SEM; n = 12; p < 0.05). Arteriolar diameter returned to baseline values within 1-4 min after suffusion was stopped. These effects were significantly potentiated when VIP (0.05, 0.1 & 1.0 nmol) was encapsulated into liposomes (26 +/- 6%, 38 +/- 7% and 34 +/- 3% increase from baseline values, respectively; n = 12; p < 0.05). In addition, arteriolar diameter returned to baseline values 5-13 min after suffusion was stopped. Suffusion of liposomes alone had no significant effects on arteriolar diameter (n = 12; p > 0.5). We conclude that encapsulation of VIP into liposomes potentiates and prolongs of its vasorelaxant effects in the peripheral microcirculation in vivo.

摘要

本研究的目的是确定将血管活性肠肽(VIP)包裹于脂质体中是否会增强其在体内的血管舒张作用。利用活体显微镜,我们在灌注VIP、脂质体以及包裹于脂质体中的VIP 7分钟之前、期间和之后,测量了仓鼠颊囊内二级小动脉(直径53±1微米)的直径。我们发现,VIP(0.05、0.1和1.0纳摩尔)可诱导显著的、时间和浓度依赖性的血管舒张(分别比基线值增加9±1%、13±3%和14±1%;平均值±标准误;n = 12;p < 0.05)。停止灌注后1 - 4分钟内,小动脉直径恢复至基线值。当VIP(0.05、0.1和1.0纳摩尔)包裹于脂质体中时,这些作用显著增强(分别比基线值增加26±6%、38±7%和34±3%;n = 12;p < 0.05)。此外,停止灌注后5 - 13分钟,小动脉直径恢复至基线值。单独灌注脂质体对小动脉直径无显著影响(n = 12;p > 0.5)。我们得出结论,将VIP包裹于脂质体中可增强并延长其在体内外周微循环中的血管舒张作用。

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