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同源性小鼠5-羟色胺3A受体的开放概率取决于亚基占有率。

Open probability of homomeric murine 5-HT3A serotonin receptors depends on subunit occupancy.

作者信息

Mott D D, Erreger K, Banke T G, Traynelis S F

机构信息

Department of Pharmacology, Emory University School of Medicine, Atlanta, GA 30322-3090, USA.

出版信息

J Physiol. 2001 Sep 1;535(Pt 2):427-43. doi: 10.1111/j.1469-7793.2001.00427.x.

Abstract
  1. The time course of macroscopic current responses of homomeric murine serotonin 5-HT3A receptors was studied in whole cells and excised membrane patches under voltage clamp in response to rapid application of serotonin. 2. Serotonin activated whole cell currents with an EC(50) value for the peak response of 2 microM and a Hill slope of 3.0 (n = 12), suggesting that the binding of at least three agonist molecules is required to open the channel. 3. Homomeric 5-HT3A receptors in excised membrane patches had a slow activation time course (mean +/- S.E.M. 10-90 % rise time 12.5 +/- 1.6 ms; n = 9 patches) for 100 microM serotonin. The apparent activation rate was estimated by fitting an exponential function to the rising phase of responses to supramaximal serotonin to be 136 s(-1). 4. The 5-HT3A receptor response to 100 microM serotonin in outside-out patches (n = 19) and whole cells (n = 41) desensitized with a variable rate that accelerated throughout the experiment. The time course for desensitization was described by two exponential components (for patches tau(slow) 1006 +/- 139 ms, amplitude 31 %; tau(fast) 176 +/- 25 ms, amplitude 69 %). 5. Deactivation of the response following serotonin removal from excised membrane patches (n = 8) and whole cells (n = 29) was described by a dual exponential time course with time constants similar to those for desensitization (for patches tau(slow) 838 +/- 217 ms, 55 % amplitude; tau(fast) 213 +/- 44 ms, 45 % amplitude). 6. In most patches (6 of 8), the deactivation time course in response to a brief 1-5 ms pulse of serotonin was similar to or slower than desensitization. This suggests that the continued presence of agonist can induce desensitization with a similar or more rapid time course than agonist unbinding. The difference between the time course for deactivation and desensitization was voltage independent over the range -100 to -40 mV in patches (n = 4) and -100 to +50 mV in whole cells (n = 4), suggesting desensitization of these receptors in the presence of serotonin does not reflect a voltage-dependent block of the channel by agonist. 7. Simultaneously fitting the macroscopic 5-HT3A receptor responses in patches to submaximal (2 microM) and maximal (100 microM) concentrations of serotonin to a variety of state models suggests that homomeric 5-HT3A receptors require the binding of three agonists to open and possess a peak open probability greater than 0.8. Our modelling also suggests that channel open probability varies with the number of serotonin molecules bound to the receptor, with a reduced open probability for fully liganded receptors. Increasing the desensitization rate constants in this model can generate desensitization that is more rapid than deactivation, as observed in a subpopulation of our patches.
摘要
  1. 在电压钳制下,于全细胞和切除的膜片上研究了同源性小鼠5-羟色胺5-HT3A受体对快速施加的5-羟色胺的宏观电流响应的时间进程。2. 5-羟色胺激活全细胞电流,其峰值响应的EC(50)值为2 microM,希尔系数为3.0(n = 12),这表明至少需要三个激动剂分子结合才能打开通道。3. 切除的膜片中同源性5-HT3A受体对100 microM 5-羟色胺具有缓慢的激活时间进程(平均±标准误,10 - 90%上升时间为12.5 ± 1.6 ms;n = 9个膜片)。通过将指数函数拟合到对超最大浓度5-羟色胺响应的上升阶段,估计表观激活速率为136 s(-1)。4. 外向膜片中(n = 19)和全细胞中(n = 41)100 microM 5-羟色胺的5-HT3A受体响应以可变速率脱敏,且在整个实验过程中加速。脱敏的时间进程由两个指数成分描述(对于膜片,tau(慢) 1006 ± 139 ms,幅度31%;tau(快) 176 ± 25 ms,幅度69%)。5. 从切除的膜片(n = 8)和全细胞(n = 29)中去除5-羟色胺后响应的失活由双指数时间进程描述,时间常数与脱敏的相似(对于膜片,tau(慢) 838 ± 217 ms,幅度55%;tau(快) 213 ± 44 ms,幅度45%)。6. 在大多数膜片(8个中的6个)中,对5-羟色胺1 - 5 ms短暂脉冲的响应失活时间进程与脱敏相似或更慢。这表明激动剂的持续存在可诱导脱敏,其时间进程与激动剂解离相似或更快。在膜片(n = 4)中-100至-40 mV范围内以及全细胞(n = 4)中-100至+50 mV范围内,失活和脱敏的时间进程差异与电压无关,这表明在5-羟色胺存在下这些受体的脱敏并不反映激动剂对通道的电压依赖性阻断。7. 将膜片中5-HT3A受体对亚最大浓度(2 microM)和最大浓度(100 microM)5-羟色胺的宏观响应同时拟合到各种状态模型表明,同源性5-HT3A受体需要三个激动剂结合才能打开,且具有大于0.8的峰值开放概率。我们的模型还表明,通道开放概率随与受体结合的5-羟色胺分子数量而变化,完全结合配体的受体开放概率降低。在该模型中增加脱敏速率常数可产生比失活更快的脱敏,正如在我们部分膜片中观察到的那样。

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