阐明化疗策略,开发针对致命疾病--内皮利什曼病--的有效药物。

Awanish Kumar
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摘要

在没有有效疫苗的情况下,控制内脏利什曼病(VL)主要依靠化疗。然而,现有的抗利什曼病药物数量有限,存在毒性问题、不良反应、低效和抗利什曼病耐药性。据报道,与五价抗锑药物(90 年前发现的最值得推荐的抗利什曼病药物)的常规治疗相比,疗效明显下降(剂量和疗程增加了约十倍)。两性霉素 B 是第二线治疗药物,但因其价格昂贵而限制了其广泛使用。喷他脒是另一种抗 VL 药物,但其疗效在不同地区已显著下降。由于治疗失败的比例显著增加,这些治疗 VL 的传统疗法几乎已经过时。因此,寻找有效的未来抗 VL 药物的工作已持续了数十年,而在当前形势下,这种药物的需求量很大。一些传统疗法经过改良,但也不尽如人意。因此,本文旨在讨论传统疗法和改良疗法,同时强调抗 VL 的创新化疗措施,以加快抗利什曼病药物的缓慢步伐,并在未来克服耐药性问题。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Articulate Chemotherapeutic Strategies for the Development of Effective Drugs against a Fatal Disease, Visceral Leishmaniasis.

Visceral Leishmaniasis (VL) control relies mainly on chemotherapy in the absence of no effective vaccines. However, available anti-VL drugs are limited in number, having toxicity issues, adverse reactions, low efficacy, and resistance observed against antileishmanial. A significant decrease in efficacy (~tenfold increase in dosage and duration) was reported against the usual treatment with Pentavalent antimonials (the most recommended antileishmanial drug discovered 90 years ago). Amphotericin B is the second line of treatment but limits wider use due to its high cost. Pentamidine is another anti-VL drug, but its therapeutic efficacy has decreased significantly in different areas. These conventional therapeutics for VL have become almost outdated due to a significant increase in therapeutic failure in terms of percentage. Due to this, the search for an effective future anti-VL drug spans several decades, and now it is in high demand in the current situation. Some conventional therapeutics are modified, but they are also not satisfactory. Therefore, this article aimed to discuss conventional and modified therapeutics while emphasizing innovative chemotherapeutic measures against VL that could speed up the slow pace of antileishmanial drugs and overcome the drug resistance problem in the future.

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