Chromaffin cell catecholamine secretion: bisindolylmaleimide compounds exhibit novel and potent antagonist effects at the nicotinic cholinergic receptor in pheochromocytoma cells.

Mahata M; Mahapatra NR; OConnor DT; Mahata SK

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Chromaffin cell catecholamine secretion: bisindolylmaleimide compounds exhibit novel and potent antagonist effects at the nicotinic cholinergic receptor in pheochromocytoma cells.

机译：嗜铬细胞中儿茶酚胺的分泌：双辛基马来酰亚胺化合物对嗜铬细胞瘤细胞的烟碱胆碱能受体表现出新颖而有效的拮抗作用。

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Activation of protein kinase C (PKC) stimulates nicotine-induced catecholamine secretion. PKC down-regulation by prolonged pretreatment with phorbol 12-myristate 13-acetate diminished nicotine-induced catecholamine secretion only slightly (approximately 16%), suggesting substantial PKC independence of nicotinic receptor activation. However, we found that bisindolylmaleimide compounds (which are also putative PKC chemical inhibitors) dramatically inhibited nicotine-induced catecholamine secretion (IC(50) values of approximately 24-37 nM). This inhibition was specific for the nicotinic cholinergic receptor. Catecholamine secretion induced by other nicotinic agonists (such as epibatidine, anatoxin, or cytisine) was also powerfully antagonized by bisindolylmaleimide II (IC(50) values of approximately 60-90 nM). Even high-dose nicotinic agonists failed to overcome the inhibition by bisindolylmaleimide II, suggesting noncompetitive nicotinic antagonism by this class of compounds. Nicotinic inhibition by bisindolylmaleimide seemed not to be readily reversible. Structure-activity studies of bisindolylmaleimide compounds revealed that bisindolylmaleimides I through III are the most potent nicotinic antagonists at the nicotinic cholinergic receptor in PC-12 cells (IC(50) < or =37 nM), whereas bisindolylmaleimide IV and V have far less nicotinic antagonist activity (IC(50) >1 microM); the active compounds I through III have cationic tails at an indole nitrogen, whereas the least potent compounds IV and V do not. By contrast, a free NH within the maleimide ring is crucial for PKC inhibition by this class of compounds. We conclude that bisindolylmaleimides I through III are some of the most potent noncompetitive neuronal nicotinic antagonists, indeed the most potent such antagonists we have observed in PC-12 cells. Nicotinic antagonism of these compounds seems to be independent of PKC inhibition.

机译：蛋白激酶C（PKC）的激活刺激了尼古丁诱导的儿茶酚胺分泌。通过用佛波醇12-肉豆蔻酸酯13-乙酸酯进行长时间预处理可以使PKC下调，尼古丁诱导的儿茶酚胺分泌仅略微降低（约16％），这表明烟碱样受体激活对PKC的依赖性很大。但是，我们发现，bisindolylmaleimide化合物（也是推定的PKC化学抑制剂）大大抑制了尼古丁引起的儿茶酚胺分泌（IC（50）值约为24-37 nM）。这种抑制作用对烟碱胆碱能受体具有特异性。由其他烟碱激动剂（如依巴替丁，抗毒素或胱氨酸）诱导的儿茶酚胺分泌也被比辛多基马来酰亚胺II（IC（50）值约为60-90 nM）强烈拮抗。甚至大剂量的烟碱激动剂也未能克服双辛基基马来酰亚胺II的抑制作用，这表明这类化合物的非竞争性烟碱拮抗作用。 bisindolylmaleimide对烟碱的抑制作用似乎不容易逆转。 bisindolylmaleimide化合物的结构活性研究表明，bisindolylmaleimide I至III是PC-12细胞中烟碱胆碱能受体最有效的烟碱拮抗剂（IC（50）<或= 37 nM），而bisindolylmaleimide IV和V的烟碱含量要低得多拮抗剂活性（IC（50）> 1 microM）;活性化合物I至III在吲哚氮上具有阳离子尾，而效力最低的化合物IV和V没有。相反，马来酰亚胺环内的游离NH对于这类化合物对PKC的抑制至关重要。我们得出的结论是，bisindolylmaleimide I至III是一些最有效的非竞争性神经元烟碱拮抗剂，实际上是我们在PC-12细胞中观察到的最有效的此类拮抗剂。这些化合物的烟碱拮抗作用似乎与PKC抑制无关。

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《Molecular pharmacology.》 |2002年第6期|共8页
作者
Mahata M; Mahapatra NR; OConnor DT; Mahata SK;
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正文语种 eng
中图分类药学;
关键词
Protein Kinase C; Process of secretion; Catecholamines; bisindolylmaleimide; 蛋白激酶C; 儿茶酚胺类;

机译：Protein Kinase C;Process of secretion;Catecholamines;bisindolylmaleimide;蛋白激酶C;儿茶酚胺类;

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1. Chromaffin cell catecholamine secretion: bisindolylmaleimide compounds exhibit novel and potent antagonist effects at the nicotinic cholinergic receptor in pheochromocytoma cells. [J] . Mahata M, Mahapatra NR, OConnor DT, Molecular pharmacology. . 2002,第6期

机译：嗜铬细胞中儿茶酚胺的分泌：双辛基马来酰亚胺化合物对嗜铬细胞瘤细胞的烟碱胆碱能受体表现出新颖而有效的拮抗作用。
2. omega-Conotoxin GVIA blocks nicotine-induced catecholamine secretion by blocking the nicotinic receptor-activated inward currents in bovine chromaffin cells. [J] . Fernandez JM, Granja R, Izaguirre V, Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences . 1995,第1a2期

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3. Catecholamine secretion in trout chromaffin cells experiencing nicotinic receptor desensitization is maintained by non-cholinergic neurotransmission [J] . McNeill B, Montpetit CJ, Perry SF The Journal of Experimental Biology . 2003,第23期

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4. TEA EXTRACTS CONFER ITS ANTIPROLIFERATING EFFECTS THROUGH INHIBITION OF NICOTINE- AND ESTROGEN-INDUCED 9-NICOTINIC ACETYLCHOLINE RECEPTOR UPREGULATION IN HUMAN BREAST CANCER CELLS [C] . Yuan-Soon Ho, Min-Hsiung Pan International Flavor Conference . 2013

机译：茶提取物通过抑制尼古丁和雌激素诱导的9-烟碱乙酰胆碱受体上调在人乳腺癌细胞中赋予其抗增殖效果
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6. Mixed nicotinic and muscarinic features of cholinergic receptor coupled to secretion in bovine chromaffin cells. [O] . M H Shirvan, H B Pollard, E Heldman 1991

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7. Mixed nicotinic and muscarinic features of cholinergic receptor coupled to secretion in bovine chromaffin cells. [O] . Shirvan, M H, Pollard, H B, Heldman, E 1991

机译：胆碱能受体的混合烟碱和毒蕈碱特性与牛嗜铬细胞的分泌有关。

Chromaffin cell catecholamine secretion: bisindolylmaleimide compounds exhibit novel and potent antagonist effects at the nicotinic cholinergic receptor in pheochromocytoma cells.

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