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霍楠酚和α-倒捻子素通过不同机制抑制马雅罗病毒复制。

Honokiol and Alpha-Mangostin Inhibit Mayaro Virus Replication through Different Mechanisms.

机构信息

Grupo de Biología Celular y Molecular de Arbovirus, Instituto Conmemorativo Gorgas de Estudios de la Salud, Panama City 0816-02593, Panama.

Programa de Maestría en Microbiología Ambiental, Universidad de Panamá, Panama City 0824-03366, Panama.

出版信息

Molecules. 2022 Oct 29;27(21):7362. doi: 10.3390/molecules27217362.

Abstract

Mayaro virus (MAYV) is an emerging arbovirus with an increasing circulation across the Americas. In the present study, we evaluated the potential antiviral activity of the following natural compounds against MAYV and other arboviruses: Sanguinarine, (R)-Shikonin, Fisetin, Honokiol, Tanshinone IIA, and α-Mangostin. Sanguinarine and Shikonin showed significant cytotoxicity, whereas Fisetin, Honokiol, Tanshinone IIA, and α-Mangostin were well tolerated in all the cell lines tested. Honokiol and α-Mangostin treatment protected Vero-E6 cells against MAYV-induced damage and resulted in a dose-dependent reduction in viral progeny yields for each of the MAYV strains and human cell lines assessed. These compounds also reduced MAYV viral RNA replication in HeLa cells. In addition, Honokiol and α-Mangostin disrupted MAYV infection at different stages of the virus life cycle. Moreover, Honokiol and α-Mangostin decreased Una, Chikungunya, and Zika viral titers and downmodulated the expression of E1 and nsP1 viral proteins from MAYV, Una, and Chikungunya. Finally, in Honokiol- and α-Mangostin-treated HeLa cells, we observed an upregulation in the expression of type I interferon and specific interferon-stimulated genes, including , β, , , , , , and IL-1β, which may promote an antiviral cellular state. Our results indicate that Honokiol and α-Mangostin present potential broad-spectrum activity against different arboviruses through different mechanisms.

摘要

马亚罗病毒(MAYV)是一种新兴的虫媒病毒,其在美洲的传播范围不断扩大。在本研究中,我们评估了以下天然化合物对 MAYV 和其他虫媒病毒的潜在抗病毒活性:血根碱、(R)-紫草素、非瑟酮、和厚朴酚、丹参酮 IIA 和 α-倒捻子素。血根碱和紫草素表现出显著的细胞毒性,而非瑟酮、和厚朴酚、丹参酮 IIA 和 α-倒捻子素在所有测试的细胞系中均耐受良好。和厚朴酚和 α-倒捻子素处理可保护 Vero-E6 细胞免受 MAYV 诱导的损伤,并导致每种 MAYV 株和评估的人细胞系的病毒子代产量呈剂量依赖性降低。这些化合物还可抑制 HeLa 细胞中的 MAYV 病毒 RNA 复制。此外,和厚朴酚和 α-倒捻子素在病毒生命周期的不同阶段破坏 MAYV 感染。此外,和厚朴酚和 α-倒捻子素降低了 Una、基孔肯雅热和寨卡病毒滴度,并下调了 MAYV、Una 和基孔肯雅热的 E1 和 nsP1 病毒蛋白的表达。最后,在和厚朴酚和 α-倒捻子素处理的 HeLa 细胞中,我们观察到 I 型干扰素和特定干扰素刺激基因的表达上调,包括 、 、 、 、 、 和 IL-1β,这可能促进抗病毒的细胞状态。我们的结果表明,和厚朴酚和 α-倒捻子素通过不同机制对不同的虫媒病毒具有潜在的广谱活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3386/9659048/951609b1e506/molecules-27-07362-g001.jpg

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