Archer S L, Huang J M, Reeve H L, Hampl V, Tolarová S, Michelakis E, Weir E K
Cardiovascular Section, VA Medical Center, Minneapolis, MN 55417, USA.
Circ Res. 1996 Mar;78(3):431-42. doi: 10.1161/01.res.78.3.431.
The cellular mechanisms that determine differences in reactivity of arteries of varying size and origin are unknown. We evaluated the hypothesis that there is diversity in the distribution of K+ channels between vascular smooth muscle (VSM) cells within a single segment of the pulmonary arteries (PAs) and that there are differences in the prevalence of these cell types between conduit and resistance arteries, which contribute to segmental differences in the vascular response to NO and hypoxia. Three types of VSM cells can be identified in rat PAs on the basis of their whole-cell electrophysiological properties- current density and the pharmacological dissection of whole-cell K+ current(I(K))-and morphology. Cells are referred to as "K(Ca), K(Dr), or mixed," acknowledging the type of K+ channel that dominates the IK: the Ca2+-sensitive (K(Ca)) channel, delayed rectifier (K(Dr)) channel, or a mixture of both. The three cell types were identified by light and electron microscopy. K(Ca) cells are large and elongated, and they have low current density and currents that are inhibited by tetraethylammonium (5 mmol/L) or charybdotoxin (100 nmol/L). K(Dr) cells are smaller, with a perinuclear bulge, but have high current density and currents that are inhibited by 4-aminopyridine (5 mmol/L). Conduit arteries contain significant numbers of K(Ca) cells, whereas resistance arteries have a majority of K(Dr) cells and few K(Ca) cells. NO rapidly and reversibly increases I(K) and hyperpolarizes K(Ca) cells because of an increase in open probability of a 170-pS K(Ca) channel. Hypoxia depolarizes K(Dr) cells by rapidly and reversibly inhibiting one or more of the tonically active K(Dr) channels (including a 37-pS channel) that control resting membrane potential. The effects of both hypoxia and NO on K+ channels are evident at negative membrane potentials, supporting their physiological relevance. The functional correlate of this electrophysiological diversity is that K(Dr)-enriched resistance vessels constrict to hypoxia, whereas conduit arteries have a biphasic response predominated by relaxation. Although effective in both segments, NO relaxes conduit more than resistance rings, in both cases by a cGMP-dependent mechanism. We conclude that regional electrophysiological diversity among smooth muscle cells is a major determinant of segmental differences in vascular reactivity.
决定不同大小和来源的动脉反应性差异的细胞机制尚不清楚。我们评估了以下假设:在肺动脉(PA)单个节段内的血管平滑肌(VSM)细胞之间,钾通道的分布存在差异,并且在导管动脉和阻力动脉之间,这些细胞类型的患病率存在差异,这导致血管对一氧化氮(NO)和缺氧反应的节段性差异。根据大鼠PA的全细胞电生理特性——电流密度和全细胞钾电流(I(K))的药理学剖析以及形态学,可以识别出三种类型的VSM细胞。根据主导IK的钾通道类型,细胞被称为“K(Ca)、K(Dr)或混合型”:钙敏感(K(Ca))通道、延迟整流器(K(Dr))通道或两者的混合物。通过光学和电子显微镜鉴定了这三种细胞类型。K(Ca)细胞大且细长,电流密度低,其电流可被四乙铵(5 mmol/L)或蝎毒素(100 nmol/L)抑制。K(Dr)细胞较小,有核周隆起,但电流密度高,其电流可被4-氨基吡啶(5 mmol/L)抑制。导管动脉含有大量的K(Ca)细胞,而阻力动脉中大多数是K(Dr)细胞,K(Ca)细胞很少。NO通过增加170-pS K(Ca)通道的开放概率,迅速且可逆地增加I(K)并使K(Ca)细胞超极化。缺氧通过迅速且可逆地抑制一个或多个控制静息膜电位的持续性活动的K(Dr)通道(包括一个37-pS通道),使K(Dr)细胞去极化。缺氧和NO对钾通道的影响在负膜电位时很明显,这支持了它们的生理相关性。这种电生理多样性的功能关联是,富含K(Dr)的阻力血管对缺氧收缩,而导管动脉有以舒张为主的双相反应。尽管在两个节段中都有效,但NO对导管环的舒张作用比对阻力环更强,在两种情况下都是通过依赖环磷酸鸟苷(cGMP)的机制。我们得出结论:平滑肌细胞之间的区域电生理多样性是血管反应性节段性差异的主要决定因素。
