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蜜蜂肽作为山羊痘病毒DNA指导的RNA聚合酶潜在抑制剂的计算机模拟分析

In Silico Analysis of Honey Bee Peptides as Potential Inhibitors of Capripoxvirus DNA-Directed RNA Polymerase.

作者信息

Mustafa Ghulam, Mahrosh Hafiza Salaha, Salman Mahwish, Ali Muhammad, Arif Rawaba, Ahmed Sibtain, Ebaid Hossam

机构信息

Department of Biochemistry, Government College University Faisalabad, Faisalabad 38060, Pakistan.

Department of Biochemistry, University of Agriculture Faisalabad, Faisalabad 38040, Pakistan.

出版信息

Animals (Basel). 2023 Jul 12;13(14):2281. doi: 10.3390/ani13142281.

Abstract

The genus Capripoxvirus belongs to the Poxviridae family. The sheeppox, goatpox, and lumpy skin disease viruses are three species of this genus with 96% identity in their genomes. These are financially devastating viral infections among cattle, which cause a reduction in animal products and lead to a loss in livestock industries. In the current study, the phylogenetic analysis was carried out to reveal the evolutionary relationships of Capripoxvirus species (i.e., sheeppox virus (SPPV), goatpox virus (GTPV), and lumpy skin disease virus (LSDV)) with other viruses from the Poxviridae family with >96% query coverage to find the similarity index among all members. The three viruses (i.e., SPPV, GTPV, and LSDV) joined the clade of Capripoxvirus of the Poxviridae family in the phylogenetic tree and exhibited close evolutionary relationships. The multiple sequence alignment using ClustalOmega revealed significant variations in the protein sequences of the DNA-dependent RNA polymerase of SPPV, GTPV, and LSDV. The three-dimensional structures of five selected bee peptides and DNA-directed RNA polymerase of SPPV, GTPV, and LSDV were predicted using trRosetta and I-TASSER and used for molecular docking and simulation studies. The protein-protein docking was carried out using HADDOCK server to explore the antiviral activity of peptides as honey bee proteins against SPPV, GTPV, and LSDV. In total, five peptides were docked to DNA-directed RNA polymerase of these viruses. The peptides mellitin and secapin-1 displayed the lowest binding scores (-106.9 +/- 7.2 kcal/mol and -101.4 +/- 11.3 kcal/mol, respectively) and the best patterns with stable complexes. The molecular dynamics simulation indicated that the complex of protein DNA-dependent RNA polymerase and the peptide melittin stayed firmly connected and the peptide binding to the receptor protein was stable. The findings of this study provide the evidence of bee peptides as potent antimicrobial agents against sheeppox, goatpox, and lumpy skin disease viruses with no complexity.

摘要

山羊痘病毒属属于痘病毒科。绵羊痘病毒、山羊痘病毒和结节性皮炎病毒是该属的三个物种,它们的基因组具有96%的同一性。这些病毒感染对养牛业造成了巨大的经济损失,会导致动物产品减少,给畜牧业带来损失。在本研究中,进行了系统发育分析,以揭示山羊痘病毒属物种(即绵羊痘病毒(SPPV)、山羊痘病毒(GTPV)和结节性皮炎病毒(LSDV))与痘病毒科中查询覆盖率>96%的其他病毒之间的进化关系,以找出所有成员之间的相似性指数。这三种病毒(即SPPV、GTPV和LSDV)在系统发育树中加入了痘病毒科山羊痘病毒属的进化枝,并显示出密切的进化关系。使用ClustalOmega进行的多序列比对揭示了SPPV、GTPV和LSDV的依赖DNA的RNA聚合酶蛋白质序列存在显著差异。使用trRosetta和I-TASSER预测了五种选定的蜜蜂肽以及SPPV、GTPV和LSDV的依赖DNA的RNA聚合酶的三维结构,并将其用于分子对接和模拟研究。使用HADDOCK服务器进行蛋白质-蛋白质对接,以探索作为蜜蜂蛋白质的肽对SPPV、GTPV和LSDV的抗病毒活性。总共将五种肽与这些病毒的依赖DNA的RNA聚合酶进行对接。蜂毒肽和secapin-1显示出最低的结合分数(分别为-106.9±7.2千卡/摩尔和-101.4±11.3千卡/摩尔)以及具有稳定复合物的最佳模式。分子动力学模拟表明,依赖蛋白质DNA的RNA聚合酶与蜂毒肽的复合物保持牢固连接,并且肽与受体蛋白的结合是稳定的。本研究结果提供了证据,证明蜜蜂肽是对抗绵羊痘、山羊痘和结节性皮炎病毒的有效抗菌剂,且不复杂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d7ae/10376589/b5b3b1910610/animals-13-02281-g001.jpg

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