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Reversal and inhibition of cholera toxin-induced secretion in isolated rabbit ileum.

机译:霍乱毒素诱导的兔回肠分泌物的逆转和抑制。

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摘要

1. Cholera toxin (1 microgram/ml) abolished net fluid absorption by everted sacs of rabbit ileum, leading to net fluid secretion. This action occurred via the toxin-catalysed ADP ribosylation of the stimulatory GTP-binding protein Gs which is linked to adenylate cyclase. Nicotinamide (10 mM), a reaction product of ADP ribosylation, reversed cholera toxin-induced secretion, restoring absorption. Lower concentrations of nicotinamide induced partial reversal. 2. Nicotinamide (1 mM) blocked the secretory action of cholera toxin applied to ileal sacs. This inhibitory action was more effective in the presence of methionine (1 mM). 3. Other inhibitors of ADP ribosylation, benzamide and adenine, blocked the secretory action of cholera toxin. Hypoxanthine, an analogue and metabolite of adenine, was similarly effective. 4. Nicotinamide was not, however, effective in blocking or reversing the secretory action of theophylline (10 mM) or of heat-stable E. coli enterotoxin STa. This indicates that nicotinamide has a highly specific action against ADP ribosylating toxins. 5. It is proposed that nicotinamide reverses the secretory action of cholera toxin by reversing ADP ribosylation, simply by the law of mass action. This counters the established idea that the effects of cholera and other ADP-ribosylating toxins are irreversible under physiological conditions.
机译:1.霍乱毒素(1微克/毫升)消除了兔回肠外翻囊的净液体吸收,导致净液体分泌。该作用通过刺激性GTP结合蛋白Gs的毒素催化的ADP核糖基化而发生,该蛋白与腺苷酸环化酶连接。烟酰胺(10 mM)是ADP核糖基化反应的产物,可逆转霍乱毒素诱导的分泌,恢复吸收。较低浓度的烟酰胺可引起部分逆转。 2.烟酰胺(1 mM)阻止了应用于回肠囊的霍乱毒素的分泌作用。在蛋氨酸(1 mM)存在下,这种抑制作用更为有效。 3.其他ADP核糖基化抑制剂,苯甲酰胺和腺嘌呤可阻断霍乱毒素的分泌作用。次黄嘌呤是腺嘌呤的类似物和代谢产物,同样有效。 4.然而,烟酰胺不能有效阻止或逆转茶碱(10 mM)或热稳定的大肠杆菌肠毒素STa的分泌作用。这表明烟酰胺对ADP核糖基化毒素具有高度特异性的作用。 5.提出烟酰胺可以通过简单地根据质量作用定律逆转ADP核糖基化来逆转霍乱毒素的分泌作用。这与已确立的思想相反,即在生理条件下霍乱和其他ADP-核糖基化毒素的作用是不可逆的。

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