Explorations on the antiviral potential of zinc and magnesium salts against chikungunya virus: implications for therapeutics

Frontiers in Cellular and Infection Microbiology Pub Date : 2024-06-04 DOI:10.3389/fcimb.2024.1335189

K. Davuluri, Shridhar Shukla, M. Kakade, Sarah Cherian, K. Alagarasu, D. Parashar

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Abstract

Chikungunya virus (CHIKV), which causes chikungunya fever, is an arbovirus of public health concern with no approved antiviral therapies. A significant proportion of patients develop chronic arthritis after an infection. Zinc and magnesium salts help the immune system respond effectively against viral infections. This study explored the antiviral potential of zinc sulphate, zinc acetate, and magnesium sulphate against CHIKV infection.The highest non-toxic concentration of the salts (100 µM) was used to assess the prophylactic, virucidal, and therapeutic anti-CHIKV activities. Dose-dependent antiviral effects were investigated to find out the 50% inhibitory concentration of the salts. Entry bypass assay was conducted to find out whether the salts affect virus entry or post entry stages. Virus output in all these experiments was estimated using a focus-forming unit assay, real-time RT-PCR, and immunofluorescence assay.Different time- and temperature-dependent assays revealed the therapeutic antiviral activity of zinc and magnesium salts against CHIKV. A minimum exposure of 4 hours and treatment initiation within 1 to 2 hours of infection are required for inhibition of CHIKV. Entry assays revealed that zinc salt affected virus-entry. Entry bypass assays suggested that both salts affected post-entry stages of CHIKV. In infected C57BL6 mice orally fed with zinc and magnesium salts, a reduction in viral RNA copy number was observed.The study results suggest zinc salts exert anti-CHIKV activity at entry and post entry stages of the virus life cycle, while magnesium salt affect CHIKV at post entry stages. Overall, the study highlights the significant antiviral potential of zinc sulphate, zinc acetate, and magnesium sulphate against CHIKV, which can be exploited in designing potential therapeutic strategies for early treatment of chikungunya patients, thereby reducing the virus-associated persistent arthritis.

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锌盐和镁盐对基孔肯雅病毒抗病毒潜力的探索：对治疗学的启示

导致基孔肯雅热的基孔肯雅病毒（CHIKV）是一种引起公共卫生问题的虫媒病毒，目前还没有获得批准的抗病毒疗法。相当一部分患者在感染后会出现慢性关节炎。锌和镁盐有助于免疫系统有效应对病毒感染。本研究探讨了硫酸锌、醋酸锌和硫酸镁对 CHIKV 感染的抗病毒潜力。研究人员使用最高无毒浓度（100 µM）的盐来评估其预防、杀病毒和治疗抗 CHIKV 活性。研究了剂量依赖性抗病毒效果，以找出盐类的 50% 抑制浓度。还进行了病毒进入旁路试验，以确定盐类是否会影响病毒进入或进入后阶段。所有这些实验中的病毒输出量都是通过病灶形成单位检测、实时 RT-PCR 和免疫荧光检测来估算的。对 CHIKV 的抑制需要至少 4 小时的暴露和在感染后 1 至 2 小时内开始治疗。进入试验表明，锌盐会影响病毒的进入。进入旁路试验表明，两种盐都会影响 CHIKV 的进入后阶段。研究结果表明，锌盐在病毒生命周期的进入和进入后阶段具有抗 CHIKV 活性，而镁盐则在进入后阶段影响 CHIKV。总之，该研究强调了硫酸锌、醋酸锌和硫酸镁对 CHIKV 的显著抗病毒潜力，可用于设计早期治疗基孔肯雅病患者的潜在治疗策略，从而减少与病毒相关的持续性关节炎。

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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Frontiers in Cellular and Infection Microbiology

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