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寻找圣杯——用于靶向癌症治疗的高效桥连内过氧化物

Searching for the Holy Grail - Highly Potent Bridged Endoperoxides for Targeted Cancer Therapy.

作者信息

Tiwari Mohit K, Goslinski Tomasz

机构信息

Chair and Department of Chemical Technology of Drugs, Poznan University of Medical Sciences, ul. Rokietnicka 3, 60-806, Poznań, Poland.

Chair and Department of Chemical Technology of Drugs, Poznan University of Medical Sciences, ul. Rokietnicka 3, 60-806, Poznań, Poland.

出版信息

Bioorg Chem. 2024 Dec;153:107893. doi: 10.1016/j.bioorg.2024.107893. Epub 2024 Oct 18.

DOI:10.1016/j.bioorg.2024.107893
PMID:39454496
Abstract

The International Agency for Research on Cancer (IARC) recently estimated the global cancer burden in 2050. The statistics are startling, with a 77% hike and 35 million new cancer cases per year. The present discoveries have recommended plant-derived bridged endoperoxides or artemisinin-based semisynthetic analogues as safe, well-tolerated and powerful substitutes that could be effectively utilized as a warhead to fight against global enemies like cancer. In addition, artemisinin-based drug repositioning crucially can reduce overriding drug development expenditures and establish accessibility of approved drugs with low risk to patients. Hence, the present review article provides a comprehensive account of the recent chemical and synthetic advancement of diverse cytotoxic artemisinin derivatives such as C-O, C, N, S linked artemisinin analogues, artemisinin-derived metal complexes, artemisinin-derived hybrids/conjugates with other pharmaceutically active substances, and artemisinin-derived dimers, trimers and tetramers perceived during the last three decades (1997-2024). Moreover, the current preclinical and clinical anticancer application prospects of artemisinin derivatives with other defined drugs and their utilization in combination therapy and also nanoformulation approaches for targeted drug delivery have been discussed.

摘要

国际癌症研究机构(IARC)最近对2050年全球癌症负担进行了估计。统计数据令人震惊,癌症病例将增加77%,每年新增3500万例。目前的研究发现,植物来源的桥连内过氧化物或青蒿素类半合成类似物是安全、耐受性良好且强效的替代品,可有效地用作对抗癌症等全球“敌人”的“武器”。此外,基于青蒿素的药物重新定位至关重要的是可以减少高昂的药物开发支出,并使患者能够使用风险较低的已批准药物。因此,本文综述全面介绍了近三十年来(1997 - 2024年)各种具有细胞毒性的青蒿素衍生物的化学和合成进展,如C - O、C、N、S连接的青蒿素类似物、青蒿素衍生的金属配合物、青蒿素与其他药物活性物质的杂化物/缀合物,以及青蒿素衍生的二聚体、三聚体和四聚体。此外,还讨论了青蒿素衍生物与其他特定药物的当前临床前和临床抗癌应用前景、它们在联合治疗中的应用以及用于靶向给药的纳米制剂方法。

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