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改变细胞外钙浓度及使用钙通道阻滞剂维拉帕米对仓鼠颊囊微血管渗漏部位和右旋糖酐清除率的影响。

The effect of altering the external calcium concentration and a calcium channel blocker, verapamil, on microvascular leaky sites and dextran clearance in the hamster cheek pouch.

作者信息

Mayhan W G, Joyner W L

出版信息

Microvasc Res. 1984 Sep;28(2):159-79. doi: 10.1016/0026-2862(84)90015-3.

Abstract

The role of calcium in contractile mechanisms has been well documented. Since the formation of intraendothelial gaps may be due to a contractile process, these studies were initiated to describe the effects of altering the external calcium concentration and a calcium blocker, verapamil, on the development of leaky sites and clearance of dextran in the hamster cheek pouch under normal and histamine-stimulated conditions. Adult Syrian hamsters were anesthetized and tracheostomized, and the femoral vein was cannulated for injecting the FITC-Dextran-70K. In all hamsters, a removable plastic chamber was placed in the cheek pouch to observe and collect suffusate from the microvasculature. In one series of experiments, suffusion was begun with either "normal" calcium (1.5 mM) or a calcium-free, Ringer's bicarbonate (pH 7.4, 36 degrees) buffer. After a 30-min period, fluorescein-labeled dextran (FITC-Dextran-70K) was given intravenously and the number of leaky sites and dextran clearance determined for 30-45 min. Two 5-min periods of stimulation with histamine (10(-7) and 10(-6) M) followed by a 30-min equilibration were completed while the above measurements were repeated. Then, the suffusate was switched to the opposite calcium buffer and the same sequence repeated. A similar protocol was followed using either the "normal" buffer or a high (4.5 mM)-calcium buffer. In another series of experiments, similar measurements were completed with and without verapamil (10(-4) M) using a "normal" calcium buffer and histamine-stimulated conditions. In the control, nonstimulated state, there was a significant increase in the leaky sites while suffusing with low-calcium buffer; however, there were no changes in leaky sites while suffusing with the high-calcium buffer. In the histamine-stimulated state, the increase in the number of leaky sites and dextran clearance was attenuated with the low-calcium buffer and potentiated with the high-calcium buffer. While suffusing with the verapamil buffer, there was an increase in the control number of leaky sites and in the histamine-stimulated state there was an attenuation of the histamine-stimulated response. These results indicate that external calcium influences and modulates microvascular leaky sites in normal and stimulated states and that the formation of leaky sites and dextran clearance after histamine stimulation require the transmembrane flux of calcium. Also, the formation of leaky sites was coupled directly to the clearance of dextran.

摘要

钙在收缩机制中的作用已有充分记载。由于内皮间隙的形成可能归因于收缩过程,因此开展了这些研究,以描述改变细胞外钙浓度以及一种钙阻滞剂维拉帕米,在正常和组胺刺激条件下对仓鼠颊囊渗漏部位的形成和葡聚糖清除的影响。成年叙利亚仓鼠麻醉后行气管切开术,股静脉插管用于注射异硫氰酸荧光素标记的葡聚糖-70K(FITC-Dextran-70K)。在所有仓鼠中,将一个可移除的塑料腔室置于颊囊中,以观察并收集来自微血管的灌流液。在一系列实验中,灌流开始时使用“正常”钙(1.5 mM)或无钙的碳酸氢盐林格氏液(pH 7.4,36℃)缓冲液。30分钟后,静脉注射荧光素标记的葡聚糖(FITC-Dextran-70K),并在30 - 45分钟内测定渗漏部位的数量和葡聚糖清除率。在重复上述测量的同时,完成两个5分钟的组胺(10⁻⁷和10⁻⁶ M)刺激期,随后进行30分钟的平衡期。然后,将灌流液换成相反的钙缓冲液,并重复相同的序列。使用“正常”缓冲液或高钙(4.5 mM)缓冲液遵循类似的方案。在另一系列实验中,在使用“正常”钙缓冲液和组胺刺激条件下,分别在有和没有维拉帕米(10⁻⁴ M)的情况下完成类似测量。在对照的非刺激状态下,用低钙缓冲液灌流时渗漏部位显著增加;然而,用高钙缓冲液灌流时渗漏部位没有变化。在组胺刺激状态下,低钙缓冲液可减弱渗漏部位数量的增加和葡聚糖清除率,而高钙缓冲液则增强之。在用维拉帕米缓冲液灌流时,对照状态下渗漏部位数量增加,在组胺刺激状态下组胺刺激反应减弱。这些结果表明,细胞外钙在正常和刺激状态下影响并调节微血管渗漏部位,组胺刺激后渗漏部位的形成和葡聚糖清除需要钙的跨膜通量。此外,渗漏部位的形成与葡聚糖的清除直接相关。

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