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首页> 外文期刊>The Journal of general physiology >Inositol 1,4,5-Trisphosphate (InsP3) and Calcium Interact to Increase the Dynamic Range of InsP3 Receptor-dependent Calcium Signaling

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Inositol 1,4,5-Trisphosphate (InsP3) and Calcium Interact to Increase the Dynamic Range of InsP3 Receptor-dependent Calcium Signaling

机译：肌醇1,4,5-三磷酸（InsP3）与钙相互作用可增加InsP3受体依赖性钙信号的动态范围

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The inositol 1,4,5-trisphosphate (InsP3)-gated Ca channel in cerebellum is tightly regulated by Ca (Bezprozvanny, I., J. Watras, and B.E. Ehrlich. 1991. Nature (Lond.). 351:751–754; Finch, E.A., T.J. Turner, and S.M. Goldin. 1991. Science (Wash. DC). 252:443–446; Hannaert-Merah, Z., J.F. Coquil, L. Combettes, M. Claret, J.P. Mauger, and P. Champeil. 1994. J. Biol. Chem. 269:29642–29649; Iino, M. 1990. J. Gen. Physiol. 95:1103–1122; Marshall, I., and C. Taylor. 1994. Biochem. J. 301:591–598). In previous single channel studies, the Ca dependence of channel activity, monitored at 2 μM InsP3, was described by a bell-shaped curve (Bezprozvanny, I., J. Watras, and B.E. Ehrlich. 1991. Nature (Lond.). 351:751–754). We report here that, when we used lower InsP3 concentrations, the peak of the Ca-dependence curve shifted to lower Ca concentrations. Unexpectedly, when we used high InsP3 concentrations, channel activity persisted at Ca concentrations as high as 30 μM. To explore this unexpected response of the channel, we measured InsP3 binding over a broad range of InsP3 concentrations. We found the well-characterized high affinity InsP3 binding sites (with K d 1 and 50 nM) (Maeda, N., M. Niinobe, and K. Mikoshiba. 1990. EMBO ( Eur. Mol. Biol. Organ.) J. 9:61–67; Mignery, G., T.C. Sudhof, K. Takei, and P. De Camilli. 1989. Nature (Lond.). 342:192–195; Ross, C.A., J. Meldolesi, T.A. Milner, T. Satoh, S. Supattapone, and S.H. Snyder. 1989. Nature (Lond.). 339:468–470) and a low affinity InsP3 binding site ( K d = 10 μM). Using these InsP3 binding sites, we developed a new model that accounts for the shift in the Ca-dependence curve at low InsP3 levels and the maintained channel activity at high Ca and InsP3 levels. The observed Ca dependence of the InsP3-gated Ca channel allows the cell to abbreviate the rise of intracellular Ca in the presence of low levels of InsP3, but also provides a means of maintaining high intracellular Ca during periods of prolonged stimulation.

机译：小脑中的肌醇1,4,5-三磷酸（InsP3）门控的Ca通道受到Ca的严格调控（Bezprozvanny，I.，J.Watras和BE Ehrlich。1991. Nature（Lond。）。351：751-754 ; Finch，EA，TJ Turner，and SM Goldin。1991. Science（Wash。DC）。252：443-446; Hannaert-Merah，Z.，JF Coquil，L.Combettes，M.Claret，JP Mauger，and P Champeil。1994. J. Biol。Chem。269：29642–29649; Iino，M. 1990. J. Gen. Physiol。95：1103-1122; Marshall，I.和C. Taylor。1994. Biochem。J. 301：591–598）。在以前的单通道研究中，通过钟形曲线描述了在2μMInsP3下监测的通道活性的Ca依赖性（Bezprozvanny，I.，J. Watras和BE Ehrlich。1991. Nature（Lond。）。351 ：751–754）。我们在这里报告说，当我们使用较低的InsP3浓度时，Ca依赖性曲线的峰值将移至较低的Ca浓度。出乎意料的是，当我们使用高InsP3浓度时，通道活性在Ca浓度高达30μM时仍然存在。为了探索通道的这种意外响应，我们在很宽的InsP3浓度范围内测量了InsP3的结合。我们发现了特征明确的高亲和力InsP3结合位点（K d <1和50 nM）（前田，北田，M。Niinobe和K.Mikoshiba。1990年。EMBO（欧洲分子生物学器官），J 9：61–67; Mignery，G.，TC Sudhof，K. Takei和P. De Camilli。1989. Nature（Lond。）342：192-195; Ross，CA，J. Meldolesi，TA Milner， T. Satoh，S。Supattapone和SH Snyder。1989. Nature（伦敦）。339：468-470）和低亲和力的InsP3结合位点（K d = 10μM）。使用这些InsP3结合位点，我们开发了一个新模型，该模型解释了在低InsP3水平下Ca依赖性曲线的移动以及在高Ca和InsP3水平下维持的通道活性。观察到的对InsP3门控的Ca通道的Ca依赖性使得细胞可以在低水平的InsP3存在的情况下简化细胞内Ca的升高，但也提供了在长时间刺激期间维持高细胞内Ca的方法。

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《The Journal of general physiology》 |1997年第5期|共10页
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Edward J. Kaftan; Barbara E. Ehrlich; James Watras;
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2. Regulation of Type 1 Inositol 1,4,5-Trisphosphate–gated Calcium Channels by InsP3 and Calcium [J] . I.I. Moraru, E.J. Kaftan, B.E. Ehrlich, The Journal of general physiology . 1999,第6期

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3. Inositol (1,4,5)-trisphosphate (InsP3)-gated Ca channels from cerebellum: conduction properties for divalent cations and regulation by intraluminal calcium. [J] . I Bezprozvanny, B E Ehrlich The Journal of general physiology . 1994,第5期

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