首页>
外文期刊>The Journal of general physiology
>Injection of inositol trisphosphorothioate into Limulus ventral photoreceptors causes oscillations of free cytosolic calcium.
【24h】
Injection of inositol trisphosphorothioate into Limulus ventral photoreceptors causes oscillations of free cytosolic calcium.
Limulus ventral photoreceptors contain calcium stores sensitive to release by D-myo-inositol 1,4,5 trisphosphate (InsP3) and a calcium-activated conductance that depolarizes the cell. Mechanisms that terminate the response to InsP3 were investigated using nonmetabolizable DL-myo-inositol 1,4,5 trisphosphorothioate (InsPS3). An injection of 1 mM InsPS3 into a photoreceptor's light-sensitive lobe caused an initial elevation of cytosolic free calcium ion concentration (Cai) and a depolarization lasting only 1-2 s. A period of densensitization followed, during which injections of InsPS3 were ineffective. As sensitivity recovered, oscillations of membrane potential began, continuing for many minutes with a frequency of 0.07-0.3 Hz. The activity of InsPS3 probably results from the D-stereoisomer, since L-InsP3 was much less effective than InsP3. Injections of 1 mM InsP3 caused an initial depolarization and a period of densensitization similar to that caused by 1 mM InsPS3, but no sustained oscillations of membrane potential. The initial response to InsPS3 or InsP3 may therefore be terminated by densensitization, rather than by metabolism. Metabolism of InsP3 may prevent oscillations of membrane potential after sensitivity has recovered. The InsPS3-induced oscillations of membrane potential accompanied oscillations of Cai and were abolished by injection of ethyleneglycol-bis (beta-aminoethyl ether)-N,N'-tetraacetic acid. Removal of extracellular calcium reduced the frequency of oscillation but not its amplitude. Under voltage clamp, oscillations of inward current were observed. These results indicate that periodic bursts of calcium release underly the oscillations of membrane potential. After each burst, the sensitivity of the cell to injected InsP3 was greatly reduced, recovering during the interburst interval. The oscillations may, therefore, result in part from a periodic variation in sensitivity to a constant concentration of InsPS3. Prior injection of calcium inhibited depolarization by InsPS3, suggesting that feedback inhibition of InsPS3-induced calcium release by elevated Cai may mediate desensitization between bursts and after injections of InsPS3.
展开▼
机译:腹侧光感受器包含对D-肌醇1,4,5三磷酸(InsP3)释放敏感的钙存储和钙激活的电导,使细胞去极化。使用不可代谢的DL-肌醇1,4,5三硫代硫代磷酸酯(InsPS3)研究了终止对InsP3应答的机制。将1 mM InsPS3注入到感光器的光波瓣中会引起细胞内游离钙离子浓度(Cai)的最初升高,去极化仅持续1-2 s。随后是一段致敏期,在此期间InsPS3注射无效。随着灵敏度的恢复,膜电位的振荡开始,以0.07-0.3 Hz的频率持续几分钟。 InsPS3的活性可能来自D-立体异构体,因为L-InsP3的效力远不及InsP3。注射1 mM InsP3会引起初始去极化和一段时间的脱敏作用,类似于1 mM InsPS3引起的去极化作用,但没有膜电位的持续振荡。因此,对InsPS3或InsP3的初始反应可以通过致敏作用而不是通过代谢来终止。恢复敏感性后,InsP3的代谢可能会阻止膜电位的振荡。 InsPS3引起的膜电位振荡伴随着Cai的振荡,并通过注入乙二醇双(β-氨基乙基醚)-N,N'-四乙酸消除。去除细胞外钙降低了振荡的频率,但没有降低其振幅。在电压钳制下,观察到内向电流的振荡。这些结果表明钙的周期性爆发在膜电位的振荡之下释放。每次爆发后,细胞对注入的InsP3的敏感性大大降低,在爆发间隔期间恢复。因此,振荡可能部分是由于对InsPS3浓度恒定的灵敏度的周期性变化引起的。事先注射钙会抑制InsPS3的去极化作用,这表明InsPS3引起的Cas升高对InsPS3诱导的钙释放的反馈抑制作用可能会介导猝发之间和注射InsPS3之后的脱敏。
展开▼
