Differential activation of ion channels by inositol 1,4,5-trisphosphate (IP(3))- and ryanodine-sensitive calcium stores in rat basilar artery vasomotion.

Haddock RE; Hill CE

首页> 外文期刊>The Journal of Physiology >Differential activation of ion channels by inositol 1,4,5-trisphosphate (IP(3))- and ryanodine-sensitive calcium stores in rat basilar artery vasomotion.

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Differential activation of ion channels by inositol 1,4,5-trisphosphate (IP(3))- and ryanodine-sensitive calcium stores in rat basilar artery vasomotion.

机译：肌醇1,4,5-三磷酸（IP（3））-和ryanodine敏感的钙储存在大鼠基底动脉血管运动中的离子通道的差异激活。

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Spontaneous, rhythmical contractions, or vasomotion, can be recorded from cerebral vessels under both normal physiological and pathophysiological conditions. Using electrophysiology to study changes in membrane potential, the ratiometric calcium indicator Fura-2 AM to study changes in [Ca(2+)](i) in both the arterial wall and in individual smooth muscle cells (SMCs), and video microscopy to study changes in vessel diameter, we have investigated the cellular mechanisms underlying vasomotion in the juvenile rat basilar artery. During vasomotion, rhythmical oscillations in both membrane potential and [Ca(2+)](i) were found to precede rhythmical contractions. Nifedipine depolarized SMCs and abolished rhythmical contractions and depolarizations. [Ca(2+)](i) oscillations in the arterial wall became reduced and irregular, while [Ca(2+)](i) oscillations in adjacent SMCs were no longer synchronized. BAPTA-AM, thapsigargin and U73122 hyperpolarized SMCs, relaxed the vessel, decreased basal calcium levels and abolished vasomotion. Chloride substitution abolished rhythmical activity, depolarized SMCs, increased basal calcium levels and constricted the vessel, while niflumic acid and DIDS abolished vasomotion. Ryanodine, charybdotoxin and TRAM-34, but not iberiotoxin, 4-aminopyridine or apamin, each depolarized SMCs and increased the frequency of rhythmical depolarizations and [Ca(2+)](i) oscillations. We conclude that vasomotion in the basilar artery depends on the release of intracellular calcium from IP(3) (inositol 1,4,5,-trisphosphate)-sensitive stores which activates calcium-dependent chloride channels to depolarize SMCs. Depolarization in turn activates voltage-dependent calcium channels, synchronizing contractions of adjacent cells through influx of extracellular calcium. Subsequent calcium-induced calcium release from ryanodine-sensitive stores activates an intermediate conductance potassium channel, hyperpolarizing the SMCs and providing a negative feedback pathway for regeneration of the contractile cycle.

机译：在正常生理和病理生理条件下，都可以从脑血管中记录自发性节律性收缩或血管运动。使用电生理学研究膜电位的变化，比例钙指示剂Fura-2 AM研究动脉壁和单个平滑肌细胞（SMC）中[Ca（2 +）]（i）的变化，并通过视频显微镜观察为了研究血管直径的变化，我们研究了幼年大鼠基底动脉血管运动背后的细胞机制。在血管舒缩过程中，发现膜电位和[Ca（2 +）]（i）的节律性振荡都在节律性收缩之前。硝苯地平使SMCs去极化，并取消了节律性收缩和去极化。 [Ca（2 +）]（i）的动脉壁振荡变得减少和不规则，而[Ca（2 +）]（i）的SMC中的振荡不再同步。 BAPTA-AM，thapsigargin和U73122超极化SMC可放松血管，降低基础钙水平并消除血管舒张功能。氯化物取代消除了节律性活动，使SMCs去极化，增加了基础钙水平并收缩了血管，而尼氟酸和DIDS消除了血管舒张功能。 Ryanodine，charybdotoxin和TRAM-34，但不是iberiotoxin，4-氨基吡啶或apapamin，均使SMCs去极化，并增加了节律性去极化和[Ca（2 +）]（i）振荡的频率。我们得出的结论是，基底动脉中的血管舒张取决于IP（3）（肌醇1,4,5，-三磷酸）敏感存储区中细胞内钙的释放，从而激活钙依赖性氯离子通道使SMCs去极化。去极化反过来又激活了电压依赖性钙通道，通过细胞外钙的流入使相邻细胞的收缩同步。随后，钙诱导的钙从精氨酸的敏感存储中释放，激活了一个中等电导的钾通道，使SMC超极化并为收缩循环的再生提供了负反馈途径。

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《The Journal of Physiology》 |2002年第2期|共13页
作者
Haddock RE; Hill CE;
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正文语种 eng
中图分类基础医学;
关键词
Calcium; vasomotion; Calcium measurement; Ryanodine; Arteries; 钙; 兰尼碱; 动脉;

机译：Calcium;vasomotion;Calcium measurement;Ryanodine;Arteries;钙;兰尼碱;动脉;

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1. Differential activation of ion channels by inositol 1,4,5-trisphosphate (IP(3))- and ryanodine-sensitive calcium stores in rat basilar artery vasomotion. [J] . Haddock RE, Hill CE The Journal of Physiology . 2002,第Pta2期

机译：肌醇1,4,5-三磷酸（IP（3））-和ryanodine敏感的钙储存在大鼠基底动脉血管运动中的离子通道的差异激活。
2. 2-Aminoethoxydiphenyl borate (2-APB) antagonises inositol 1,4,5-trisphosphate-induced calcium release, inhibits calcium pumps and has a use-dependent and slowly reversible action on store-operated calcium entry channels. [J] . Peppiatt CM, Collins TJ, Mackenzie L, Cell Calcium: The International Interdisciplinary Forum for Research on Calcium . 2003,第1期

机译：2-氨基乙氧基二苯基硼酸酯（2-APB）拮抗肌醇1,4,5-三磷酸酯诱导的钙释放，抑制钙泵，对储存液操作的钙进入通道具有依赖于使用且缓慢可逆的作用。
3. Activation of store-mediated calcium entry by secretion-like coupling between the inositol 1,4,5-trisphosphate receptor type II and human transient receptor potential (hTrp1) channels in human platelets [J] . Rosado JA., Sage SO. The Biochemical Journal . 2001,第Pta1期

机译：II型肌醇1,4,5-三磷酸受体与人类血小板中人类瞬态受体电位（hTrp1）通道之间的分泌样偶联激活存储介导的钙进入
4. A model of inositol 1,4,5-trisphosphate and calcium dynamics in single cells following metabotropic receptor activation [C] . Greg Lemon, William G. Gibson, Max R. Bennett Computational neuroscience meeting . 2003

机译：代谢受体激活后单细胞肌醇1,4,5-三磷酸盐和钙动力学模型
5. Identification of intracellular calcium receptors (Inositol 1,4,5 -trisphosphate and ryanodine) during maturation in bovine oocytes. [D] . Wang, Lin. 2000

机译：鉴定牛卵母细胞成熟过程中的细胞内钙受体（肌醇1,4,5-三磷酸和ryanodine）。
6. Differential activation of ion channels by inositol 145-trisphosphate (IP3)- and ryanodine-sensitive calcium stores in rat basilar artery vasomotion [O] . R E Haddock, C E Hill 2002

机译：大鼠基底动脉血管运动中肌醇145-三磷酸（IP3）和ryanodine敏感的钙库对离子通道的差异激活
7. Differential activation of ion channels by inositol 1,4,5-trisphosphate (IP3)- and ryanodine-sensitive calcium stores in rat basilar artery vasomotion [O] . Haddock, R E, Hill, C E 2002

机译：大鼠基底动脉血管运动中肌醇1,4,5-三磷酸（IP3）和ryanodine敏感的钙库对离子通道的差异激活

Differential activation of ion channels by inositol 1,4,5-trisphosphate (IP(3))- and ryanodine-sensitive calcium stores in rat basilar artery vasomotion.

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