Trace elements and metal nanoparticles: mechanistic approaches to mitigating chemotherapy-induced toxicity-a review of literature evidence.

IF 4.1 3区 生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Ademola C Famurewa, Mina Y George, Cletus A Ukwubile, Sachindra Kumar, Mehta V Kamal, Vijetha S Belle, Eman M Othman, Sreedhara Ranganath K Pai
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引用次数: 0

Abstract

Anticancer chemotherapy (ACT) remains a cornerstone in cancer treatment, despite significant advances in pharmacology over recent decades. However, its associated side effect toxicity continues to pose a major concern for both oncology clinicians and patients, significantly impacting treatment protocols and patient quality of life. Current clinical strategies to mitigate ACT-induced toxicity have proven largely unsatisfactory, leaving a critical unmet need to block toxicity mechanisms without diminishing ACT's therapeutic efficacy. This review aims to document the molecular mechanisms underlying ACT toxicity and highlight research efforts exploring the protective effects of trace elements (TEs) and their nanoparticles (NPs) against these mechanisms. Our literature review reveals that the primary driver of ACT toxicity is redox imbalance, which triggers oxidative inflammation, apoptosis, endoplasmic reticulum stress, mitochondrial dysfunction, autophagy, and dysregulation of signaling pathways such as PI3K/mTOR/Akt. Studies suggest that TEs, including zinc, selenium, boron, manganese, and molybdenum, and their NPs, can potentially counteract ACT-induced toxicity by inhibiting oxidative stress-mediated pathways, including NF-κB/TLR4/MAPK/NLRP3, STAT-3/NLRP3, Bcl-2/Bid/p53/caspases, and LC3/Beclin-1/CHOP/ATG6, while also upregulating protective signaling pathways like Sirt1/PPAR-γ/PGC-1α/FOXO-3 and Nrf2/HO-1/ARE. However, evidence regarding the roles of lncRNA and the Wnt/β-catenin pathway in ACT toxicity remains inconsistent, and the impact of TEs and NPs on ACT efficacy is not fully understood. Further research is needed to confirm the protective effects of TEs and their NPs against ACT toxicity in cancer patients. In summary, TEs and their NPs present a promising avenue as adjuvant agents for preventing non-target organ toxicity induced by ACT.

微量元素和金属纳米颗粒:减轻化疗毒性的机理方法--文献证据综述。
尽管近几十年来药理学取得了重大进展,但抗癌化疗(ACT)仍是癌症治疗的基石。然而,与之相关的副作用毒性仍然是肿瘤临床医生和患者的一大担忧,严重影响了治疗方案和患者的生活质量。事实证明,目前减轻 ACT 引起的毒性的临床策略在很大程度上并不令人满意,因此,在不降低 ACT 疗效的前提下阻断毒性机制的关键需求尚未得到满足。本综述旨在记录 ACT 毒性的分子机制,并重点介绍探索微量元素 (TE) 及其纳米颗粒 (NP) 对这些机制的保护作用的研究工作。我们的文献综述显示,ACT毒性的主要驱动因素是氧化还原失衡,它会引发氧化性炎症、细胞凋亡、内质网应激、线粒体功能障碍、自噬以及 PI3K/mTOR/Akt 等信号通路的失调。研究表明,包括锌、硒、硼、锰和钼在内的 TE 及其 NPs 有可能通过抑制氧化应激介导的途径来抵消 ACT 诱导的毒性、包括NF-κB/TLR4/MAPK/NLRP3、STAT-3/NLRP3、Bcl-2/Bid/p53/caspases和LC3/Beclin-1/CHOP/ATG6,同时还能上调保护性信号通路,如Sirt1/PPAR-γ/PGC-1α/FOXO-3和Nrf2/HO-1/ARE。然而,有关 lncRNA 和 Wnt/β-catenin 通路在 ACT 毒性中的作用的证据仍不一致,而且 TEs 和 NPs 对 ACT 疗效的影响也不完全清楚。要证实 TEs 及其 NPs 对癌症患者 ACT 毒性的保护作用,还需要进一步的研究。总之,TEs 及其 NPs 是一种很有前景的辅助药物,可用于预防 ACT 引起的非靶器官毒性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Biometals
Biometals 生物-生化与分子生物学
CiteScore
5.90
自引率
8.60%
发文量
111
审稿时长
3 months
期刊介绍: BioMetals is the only established journal to feature the important role of metal ions in chemistry, biology, biochemistry, environmental science, and medicine. BioMetals is an international, multidisciplinary journal singularly devoted to the rapid publication of the fundamental advances of both basic and applied research in this field. BioMetals offers a forum for innovative research and clinical results on the structure and function of: - metal ions - metal chelates, - siderophores, - metal-containing proteins - biominerals in all biosystems. - BioMetals rapidly publishes original articles and reviews. BioMetals is a journal for metals researchers who practice in medicine, biochemistry, pharmacology, toxicology, microbiology, cell biology, chemistry, and plant physiology who are based academic, industrial and government laboratories.
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