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人类T淋巴细胞中的电压门控钾离子通道:在有丝分裂中起作用?

Voltage-gated K+ channels in human T lymphocytes: a role in mitogenesis?

作者信息

DeCoursey T E, Chandy K G, Gupta S, Cahalan M D

出版信息

Nature. 1984;307(5950):465-8. doi: 10.1038/307465a0.

Abstract

Membrane receptors and ion transport mechanisms probably have an important role in lymphocyte activation leading to T-lymphocyte proliferation in the immune response. Here we have applied a gigaohm-seal patch clamp technique to reveal the identity and properties of ion channels in human T lymphocytes. A voltage-dependent potassium channel bearing a resemblance to the delayed rectifier of nerve and muscle cells was found to be the predominant ion channel in these cells. In the whole cell recording conformation, the channels open with sigmoid kinetics during depolarizing voltage steps, reaching a maximum K+ conductance of 3-5 nS. The current subsequently becomes almost completely inactivated during a long-lasting depolarization. Currents through single K+ channels recorded in whole cell and outside-out patch recording conformations reveal a unitary channel conductance of about 16 pS in normal Ringer solution. Thus, the peak current corresponds to approximately 200-300 conducting K+ channels per cell. Phytohaemagglutinin (PHA), at concentrations that produce mitogenesis, alters K+ channel gating within 1 min of addition to the bathing solution, causing channels to open more rapidly and at more negative membrane potentials. 3H-thymidine incorporation by T lymphocytes following PHA stimulation is inhibited by the 'classical' K+ channel blockers tetraethylammonium and 4-aminopyridine, and also by quinine, at doses found to block the K+ channel in voltage-clamped T lymphocytes, suggesting that K+ channels may play a part in mitogenesis.

摘要

膜受体和离子转运机制可能在免疫应答中淋巴细胞活化导致T淋巴细胞增殖过程中发挥重要作用。在此,我们应用千兆欧封接膜片钳技术来揭示人类T淋巴细胞中离子通道的特性。发现一种与神经和肌肉细胞的延迟整流器相似的电压依赖性钾通道是这些细胞中的主要离子通道。在全细胞记录模式下,通道在去极化电压阶跃期间以S形动力学开放,达到最大K+电导为3 - 5 nS。随后,电流在长时间去极化期间几乎完全失活。在全细胞和外向膜片记录模式下记录的单个K+通道电流显示,在正常林格溶液中单位通道电导约为16 pS。因此,峰值电流对应于每个细胞约200 - 300个导通的K+通道。在产生有丝分裂作用的浓度下,植物血凝素(PHA)在加入浴液后1分钟内改变K+通道门控,使通道在更负的膜电位下更快速地开放。PHA刺激后T淋巴细胞的3H - 胸腺嘧啶核苷掺入受到“经典”K+通道阻滞剂四乙铵和4 - 氨基吡啶的抑制,以及奎宁的抑制,在发现能阻断电压钳制的T淋巴细胞中K+通道的剂量下,这表明K+通道可能在有丝分裂中起作用。

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