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Role of the activation gate in determining the extracellular potassium dependency of block of HERG by trapped drugs

机译:激活门在被困药物确定HERG阻滞的细胞外钾依赖性中的作用

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Drug induced long QT syndrome (diLQTS) results primarily from block of the cardiac potassium channel HERG (human-ether-a-go-go related gene). In some cases long QT syndrome can result in the lethal arrhythmia torsade de pointes, an arrhythmia characterized by a rapid heart rate and severely compromised cardiac output. Many patients requiring medication present with serum potassium abnormalities due to a variety of conditions including gastrointestinal dysfunction, renal and endocrine disorders, diuretic use, and aging. Extracellular potassium influences HERG channel inactivation and can alter block of HERG by some drugs. However, block of HERG by a number of drugs is not sensitive to extracellular potassium. In this study, we show that block of WT HERG by bepridil and terfenadine, two drugs previously shown to be trapped inside the HERG channel after the channel closes, is insensitive to extracellular potassium over the range of 0 mM to 20 mM. We also show that bepridil block of the HERG mutant D540K, a mutant channel that is unable to trap drugs, is dependent on extracellular potassium, correlates with the permeant ion, and is independent of HERG inactivation. These results suggest that the lack of extracellular potassium dependency of block of HERG by some drugs may in part be related to the ability of these drugs to be trapped inside the channel after the channel closes.
机译:药物诱发的长QT综合征(diLQTS)主要是由于心脏钾通道HERG(人类以太的相关基因)受阻所致。在某些情况下,长时间QT综合征可能导致致命的心律失常扭转性扭转性心律失常,这种心律失常的特征是心律过快和严重的心输出量降低。由于各种疾病,包括胃肠功能障碍,肾脏和内分泌疾病,利尿剂使用和衰老,许多需要药物治疗的患者血清钾异常。细胞外钾会影响HERG通道的失活,并可能通过某些药物改变HERG的阻滞作用。但是,许多药物对HERG的阻滞对细胞外钾不敏感。在这项研究中,我们显示了贝普地尔和特非那定对WT HERG的阻滞作用,这两种药物先前显示在通道关闭后被困在HERG通道内,对0 mM至20 mM范围内的细胞外钾不敏感。我们还显示,HERG突变体D540K(无法捕获药物的突变体通道)的贝普地尔阻滞依赖于细胞外钾,与渗透离子相关,并且与HERG失活无关。这些结果表明,某些药物缺乏对HERG阻断的细胞外钾依赖性,可能与这些药物在通道关闭后被困在通道内的能力有关。

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