谷胱甘肽触发原药:设计策略、潜在应用和前景。

IF 10.9 1区 医学 Q1 CHEMISTRY, MEDICINAL
Jintao Zhao, Xinming Li, Tao Ma, Bingbing Chang, Baoxin Zhang, Jianguo Fang
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引用次数: 0

摘要

蓬勃发展的原药策略为提高细胞毒性药物的疗效和特异性提供了一条大有可为的途径。细胞内谷胱甘肽(GSH)水平升高一直被认为是肿瘤细胞的标志和肿瘤微环境的特征。考虑到谷胱甘肽(GSH)升高在肿瘤发生过程中的关键作用,人们开发出了多种多样的谷胱甘肽(GSH)触发原药用于癌症治疗,以减轻传统化疗药物的有害副作用和/或取得更有效的治疗效果。这些原药制剂包含一系列结构,从小分子到聚合物和有机-无机纳米材料结构。尽管人们对 GSH 触发的原药越来越感兴趣,但仍缺乏对该领域进展的全面回顾。为了填补这一空白,本综述根据这些分子的不同识别单元(即二硫化物、二硒化物、迈克尔受体和磺酰胺/磺酸盐)对其进行了分类,并在此基础上对值得关注的研究工作进行了回顾性分析。本综述还着重解释了在设计这些原药制剂时采用各种化学结构策略的独特优势。此外,我们还强调了通过结合多种靶向共轭物、治疗实体和组合治疗模式实现协同功能的潜力,所有这些都依赖于 GSH 触发。总之,本综述对这一新兴领域进行了广泛概述,强调了未来的障碍和机遇。我们的总体目标是为未来开发更有效的 GSH 触发原药提供方法指导。通过评估现有 GSH 触发原药的优缺点,我们希望这篇综述能成为原药设计的重要参考文献,并为改进原药的特性和发现构建 GSH 触发原药的新型触发支架提供指导。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Glutathione-triggered prodrugs: Design strategies, potential applications, and perspectives

The burgeoning prodrug strategy offers a promising avenue toward improving the efficacy and specificity of cytotoxic drugs. Elevated intracellular levels of glutathione (GSH) have been regarded as a hallmark of tumor cells and characteristic feature of the tumor microenvironment. Considering the pivotal involvement of elevated GSH in the tumorigenic process, a diverse repertoire of GSH-triggered prodrugs has been developed for cancer therapy, facilitating the attenuation of deleterious side effects associated with conventional chemotherapeutic agents and/or the attainment of more efficacious therapeutic outcomes. These prodrug formulations encompass a spectrum of architectures, spanning from small molecules to polymer-based and organic–inorganic nanomaterial constructs. Although the GSH-triggered prodrugs have been gaining increasing interests, a comprehensive review of the advancements made in the field is still lacking. To fill the existing lacuna, this review undertakes a retrospective analysis of noteworthy research endeavors, based on a categorization of these molecules by their diverse recognition units (i.e., disulfides, diselenides, Michael acceptors, and sulfonamides/sulfonates). This review also focuses on explaining the distinct benefits of employing various chemical architecture strategies in the design of these prodrug agents. Furthermore, we highlight the potential for synergistic functionality by incorporating multiple-targeting conjugates, theranostic entities, and combinational treatment modalities, all of which rely on the GSH-triggering. Overall, an extensive overview of the emerging field is presented in this review, highlighting the obstacles and opportunities that lie ahead. Our overarching goal is to furnish methodological guidance for the development of more efficacious GSH-triggered prodrugs in the future. By assessing the pros and cons of current GSH-triggered prodrugs, we expect that this review will be a handful reference for prodrug design, and would provide a guidance for improving the properties of prodrugs and discovering novel trigger scaffolds for constructing GSH-triggered prodrugs.

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来源期刊
CiteScore
29.30
自引率
0.00%
发文量
52
审稿时长
2 months
期刊介绍: Medicinal Research Reviews is dedicated to publishing timely and critical reviews, as well as opinion-based articles, covering a broad spectrum of topics related to medicinal research. These contributions are authored by individuals who have made significant advancements in the field. Encompassing a wide range of subjects, suitable topics include, but are not limited to, the underlying pathophysiology of crucial diseases and disease vectors, therapeutic approaches for diverse medical conditions, properties of molecular targets for therapeutic agents, innovative methodologies facilitating therapy discovery, genomics and proteomics, structure-activity correlations of drug series, development of new imaging and diagnostic tools, drug metabolism, drug delivery, and comprehensive examinations of the chemical, pharmacological, pharmacokinetic, pharmacodynamic, and clinical characteristics of significant drugs.
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