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形态学上不同的平滑肌细胞类型对血管活性激动剂的不同电反应。

Different electrical responses to vasoactive agonists in morphologically distinct smooth muscle cell types.

作者信息

Neylon C B, Avdonin P V, Dilley R J, Larsen M A, Tkachuk V A, Bobik A

机构信息

Baker Medical Research Institute, Prahran, Victoria, Australia.

出版信息

Circ Res. 1994 Oct;75(4):733-41. doi: 10.1161/01.res.75.4.733.

Abstract

Vascular smooth muscle cells (SMCs) in the blood vessel wall are frequently heterogeneous in nature, differing in their gross morphology, size, and shape, subcellular organelles, cytoskeleton, and contractile protein composition. In adult rat arterial vessels, two populations of SMCs have been shown to predominate: elongated bipolar cells, representing the majority of cells, and epithelial-like SMCs. We examined the ionic responses of these two types of SMCs, isolated by multiple subculture, to vasoactive stimuli. Elevations in intracellular Na+ and Ca2+ were measured with SBFI and fura 2, respectively, and changes in membrane potential were measured using the potential-sensitive fluorescent probe bis-oxonol. The resting membrane potential of the elongated bipolar cells was less negative than that of the epithelial-like SMCs. Exposure of the elongated SMCs to endothelin 1, alpha-thrombin, or arginine vasopressin induced elevations in [Ca2+]i and [Na+]i and membrane depolarization. Depolarization occurred because of entry of both Na+ and Ca2+, and pharmacological blockade of Cl- or K+ channels did not attenuate the depolarization. In contrast, when [Ca2+]i was elevated by the same agonists in the epithelial-like SMCs there was a pronounced hyperpolarization that appeared to be the consequence of enhanced activity of charybdotoxin-sensitive Ca(2+)-activated K+ channels because it was abolished by charybdotoxin (20 nmol/L), partially attenuated by tetraethylammonium chloride (10 mmol/L), and unaffected by apamin (1 mumol/L), glibenclamide (1 mumol/L), or 4-aminopyridine (5 mmol/L). Chelation of [Ca2+]i also abolished the hyperpolarization; instead, a small depolarization was observed.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

血管壁中的血管平滑肌细胞(SMC)本质上通常是异质性的,在总体形态、大小和形状、亚细胞器、细胞骨架以及收缩蛋白组成方面存在差异。在成年大鼠动脉血管中,已显示有两种主要的SMC群体:细长的双极细胞,占大多数细胞,以及上皮样SMC。我们研究了通过多次传代培养分离出的这两种类型SMC对血管活性刺激的离子反应。分别用SBFI和fura 2测量细胞内Na⁺和Ca²⁺的升高,并使用电位敏感荧光探针双羟萘酚测量膜电位的变化。细长双极细胞的静息膜电位比上皮样SMC的静息膜电位负性小。将细长的SMC暴露于内皮素1、α-凝血酶或精氨酸加压素会导致[Ca²⁺]i和[Na⁺]i升高以及膜去极化。去极化是由于Na⁺和Ca²⁺的内流引起的,Cl⁻或K⁺通道的药理学阻断并未减弱去极化。相反,当相同的激动剂使上皮样SMC中的[Ca²⁺]i升高时,会出现明显的超极化,这似乎是由于对藜芦毒素敏感的Ca²⁺激活K⁺通道活性增强所致,因为它被藜芦毒素(20 nmol/L)消除,被氯化四乙铵(10 mmol/L)部分减弱,并且不受蜂毒明肽(1 μmol/L)、格列本脲(1 μmol/L)或4-氨基吡啶(5 mmol/L)的影响。[Ca²⁺]i的螯合也消除了超极化;相反,观察到了小的去极化。(摘要截断于250字)

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