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豚鼠黏膜下神经元短期培养物中烟碱型和P2X通道之间的功能相互作用。

Functional interactions between nicotinic and P2X channels in short-term cultures of guinea-pig submucosal neurons.

作者信息

Barajas-López C, Espinosa-Luna R, Zhu Y

机构信息

Intestinal Disease Research Program, Department of Biomedical Sciences, McMaster University, Hamilton, Ontario, Canada.

出版信息

J Physiol. 1998 Dec 15;513 ( Pt 3)(Pt 3):671-83. doi: 10.1111/j.1469-7793.1998.671ba.x.

Abstract
  1. Functional interactions between nicotinic and P2X receptors in submucosal neurons were investigated. Whole-cell currents induced by ACh (IACh) and ATP (IATP) were blocked by hexamethonium and PPADS), respectively. Currents induced by simultaneous application of the two transmitters (IACh+ATP) were only as large as the current induced by the most effective of these substances. This current occlusion indicates that activation of nicotinic and P2X channels is not independent. 2. Kinetic parameters of IACh+ATP indicate that they are carried through channels activated by either substance. In agreement with this interpretation, both IACh and IATP amplitudes were decreased when ATP and ACh were applied simultaneously, whereas no cross-desensitization was observed when nicotinic and P2X receptors were desensitized individually. 3. Current occlusion was observed at membrane potentials of -60 and +10 mV, when IACh and IATP were inward. However, when these currents were outward (at +40 mV), current occlusion was not observed. Current occlusion was still observed at +40 mV in experiments in which the reversal potential of these currents had been adjusted to more positive values. 4. Current occlusion occurred as soon as currents were detected (< 5 ms), was still present in the absence of Ca2+, Na+ or Mg2+, and after adding staurosporine, genistein, K-252a, or N-ethylmaleimide to the pipette solution. Similar observations were noted after substituting alpha, beta-methylene ATP for ATP, or GTP for GTP-gamma-S in the pipette and in experiments carried out at 36, 23 and 9 C. 5. We propose that nicotinic and P2X channels are in functional clusters of at least two, and that the influx of ions through one activates (through allosteric interactions) a mechanism that inhibits the other channel.
摘要
  1. 研究了黏膜下神经元中烟碱型受体与P2X受体之间的功能相互作用。乙酰胆碱(ACh)诱导的全细胞电流(IACh)和ATP诱导的全细胞电流(IATP)分别被六甲铵和PPADS阻断。同时施加这两种递质诱导的电流(IACh+ATP)仅与这两种物质中最有效的一种诱导的电流一样大。这种电流叠加表明烟碱型通道和P2X通道的激活并非相互独立。2. IACh+ATP的动力学参数表明,它们是通过由任何一种物质激活的通道传导的。与此解释一致的是,当同时施加ATP和ACh时,IACh和IATP的幅度均降低,而当烟碱型受体和P2X受体分别脱敏时,未观察到交叉脱敏现象。3. 当IACh和IATP为内向电流时,在-60和+10 mV的膜电位下观察到电流叠加。然而,当这些电流为外向电流时(在+40 mV),未观察到电流叠加。在将这些电流的反转电位调整到更正的值的实验中,在+40 mV时仍观察到电流叠加。4. 一旦检测到电流(<5毫秒)就会出现电流叠加,在没有Ca2+、Na+或Mg2+的情况下以及在向移液管溶液中添加星形孢菌素、染料木黄酮、K-252a或N-乙基马来酰亚胺后,电流叠加仍然存在。在用α,β-亚甲基ATP替代ATP,或用GTP替代移液管中的GTP-γ-S以及在36、23和9℃下进行的实验中也观察到了类似的现象。5. 我们提出,烟碱型通道和P2X通道至少以两个为功能簇,并且通过一个通道的离子内流通过变构相互作用激活一种抑制另一个通道的机制。

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