Nguyen A, Kath J C, Hanson D C, Biggers M S, Canniff P C, Donovan C B, Mather R J, Bruns M J, Rauer H, Aiyar J, Lepple-Wienhues A, Gutman G A, Grissmer S, Cahalan M D, Chandy K G
Department of Physiology and Biophysics, University of California, Irvine 92717, USA.
Mol Pharmacol. 1996 Dec;50(6):1672-9.
The nonpeptide agent CP-339,818 (1-benzyl-4-pentylimino-1,4-dihydroquinoline) and two analogs (CP-393,223 and CP-394,322) that differ only with respect to the type of substituent at the N1 position, potently blocked the Kv1.3 channel in T lymphocytes. A fourth compound (CP-393,224), which has a smaller and less-lipophilic group at N1, was 100-200-fold less potent, suggesting that a large lipophilic group at this position is necessary for drug activity. CP-339,818 blocked Kv1.3 from the outside with a IC50 value of approximately 200 nM and 1:1 stoichiometry and competitively inhibited 125I-charybdotoxin from binding to the external vestibule of Kv1.3. This drug inhibited Kv1.3 in a use-dependent manner by preferentially blocking the C-type inactivated state of the channel. CP-339,818 was a significantly less potent blocker of Kv1.1, Kv1.2, Kv1.5, Kv1.6, Kv3.1-4, and Kv4.2; the only exception was Kv1.4, a cardiac and neuronal A-type K+ channel. CP-339,818 had no effect on two other T cell channels (I(CRAC) and intermediate-conductance K(Ca)) implicated in T cell mitogenesis. This drug suppresses human T cell activation, suggesting that blockade of Kv1.3 alone is sufficient to inhibit this process.
非肽类药物CP-339,818(1-苄基-4-戊基亚氨基-1,4-二氢喹啉)及其仅在N1位取代基类型上不同的两种类似物(CP-393,223和CP-394,322)能有效阻断T淋巴细胞中的Kv1.3通道。第四种化合物(CP-393,224)在N1位具有较小且亲脂性较低的基团,其效力低100 - 200倍,这表明该位置的大亲脂性基团是药物活性所必需的。CP-339,818从外部阻断Kv1.3,IC50值约为200 nM,化学计量比为1:1,并竞争性抑制125I-蝎毒素与Kv1.3外部前庭结合。该药物以使用依赖性方式抑制Kv1.3,优先阻断通道的C型失活状态。CP-339,818对Kv1.1、Kv1.2、Kv1.5、Kv1.6、Kv3.1 - 4和Kv4.2的阻断效力明显较低;唯一的例外是Kv1.4,一种心脏和神经元A型钾通道。CP-339,818对另外两种与T细胞有丝分裂相关的T细胞通道(I(CRAC)和中电导K(Ca))没有影响。该药物抑制人T细胞活化,表明单独阻断Kv1.3足以抑制这一过程。
