驱虫药阿苯达唑在体内影响大鼠脑微管的动力学和去酪氨酸-酪氨酸循环。

H D Solana, M T Teruel, R Najle, C E Lanusse, J A Rodríguez
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引用次数: 0

摘要

阿苯达唑(ABZ)是一种广泛应用于人畜医学的驱虫药。ABZ对哺乳动物和寄生虫微管蛋白均有结合亲和力。在目前的工作中,我们进行了体外实验和体内实验,在实验中,大鼠口服ABZ,以更好地表征药物对大鼠脑微管聚合的作用,以及对α -微管蛋白cooh末端发生的去酪氨酸/酪氨酸循环的作用。结果表明,ABZ在体外抑制脑微管聚合,并在体内显著延迟微管组装。体外酪氨酸化反应周期不受影响;然而,在口服药物的大鼠中,与模拟治疗的对照组相比,体外酪氨酸化水平降低。这些结果表明,这种明显的抑制可能是由于ABZ的解聚作用和随后在完整的大脑中内源性酪氨酸的酪氨酸化引起的底物数量的减少。综上所述,ABZ对体内和体外微管蛋白动力学都有强烈的影响。这些实验的结果有助于理解苯并咪唑类化合物抗小管作用的分子机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The anthelmintic albendazole affects in vivo the dynamics and the detyrosination-tyrosination cycle of rat brain microtubules.

Albendazole (ABZ) is an anthelmintic benzimidazole drug widely used in human and veterinary medicine. ABZ has binding affinity to both mammalian and helminth parasite tubulin. In the current work, we have performed in vitro assays and in vivo experiments in which rats were given ABZ orally to better characterize the action of the drug on the polymerization of rat brain microtubules and on the detyrosination/tyrosination cycle that occurs on the COOH-terminal end of alpha-tubulin. The results showed that ABZ inhibits brain microtubule polymerization in vitro, and significantly delayed microtubule assembly in vivo. The tyrosination reaction cycle was not affected in vitro; however, in rats to which the drug was administered orally, the levels of in vitro tyrosination were reduced when compared to the controls with mock treatment. These results suggest that this apparent inhibition would be due to a decrease in the amount of substrate caused by the depolymerizing effect of ABZ and the subsequent tyrosination in the intact brain with endogenous tyrosine. In conclusion, ABZ strongly affects tubulin dynamics both in vivo and in vitro. The outcome of these experiments is a contribution to the understanding of the molecular mechanisms involved in the antimicrotubular action of benzimidazole compounds.

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