Seif Elias Jorge Muniz, Junior Pedro Ismael Silva
Postgraduate Program of Molecular Biology, Biophysics and Biochemistry Department, Federal University of São Paulo, São Paulo, SP CEP 04021-001, Brazil; Laboratory of Applied Toxicology, Center of Toxins, Immune-Response and Cell Signaling - CeT-ICS/CEPID, Butantan Institute São Paulo, São Paulo, SP CEP 05503-900, Brazil.
Laboratory of Applied Toxicology, Center of Toxins, Immune-Response and Cell Signaling - CeT-ICS/CEPID, Butantan Institute São Paulo, São Paulo, SP CEP 05503-900, Brazil; Postgraduate Program Interunits in Biotechnology, USP/IPT/IBU, São Paulo, SP, Brazil.
Colloids Surf B Biointerfaces. 2025 Apr;248:114472. doi: 10.1016/j.colsurfb.2024.114472. Epub 2024 Dec 22.
Irresponsible and wholesale use of antimicrobial agents is the principal cause of the emergence of strains of resistant microorganisms to traditional drugs. Oligoventin is a neutral peptide isolated from spider eggs of Phoneutria nigriventer, with antimicrobial activity against Gram-positive, Gram-negative, and yeast organisms. However, the molecular target and pathways of antimicrobial activity are still unknown. Thus, the aim of the present study is to prospect receptors associated with the antimicrobial activity of Oligoventin using in silico tools.
The PharmMapper and PDB server was used to prospect targets originating from microorganisms. Additionally, the PatchDock server was utilized to perform molecular docking between Oligoventin and the targets. Subsequently, the I-TASSER server was adopted to predict the ligand site. Finally, the docking results and predicted sites were compared with literature sites of each target.
Over 100 potential receptors for oligoventin have been identified. Among these, enoyl-ACP reductase (Id1LXC) and thymidylate synthase ThyX (Id 1O28) from bacteria and N-acetylglucosamine phosphate mutase (Id 2DKD) showed superior interaction with oligoventin, exhibiting colocalization between docked residues and cofactor/active sites. These enzymes play a crucial role in fatty acid and DNA biosynthesis in prokaryotes and in cell wall synthesis in yeast.
Therefore, in silico results suggest that Oligoventin can impair fatty acid DNA, cell wall synthesis, thereby reducing microbial proliferation and causing microorganism death.
不负责任且大规模地使用抗菌剂是导致微生物菌株对传统药物产生耐药性的主要原因。寡聚缬菌素是一种从黑腹捕鸟蛛的蜘蛛卵中分离出的中性肽,对革兰氏阳性菌、革兰氏阴性菌及酵母菌具有抗菌活性。然而,其抗菌活性的分子靶点和途径仍不清楚。因此,本研究的目的是使用计算机工具探寻与寡聚缬菌素抗菌活性相关的受体。
利用PharmMapper和PDB服务器探寻源自微生物的靶点。此外,使用PatchDock服务器进行寡聚缬菌素与靶点之间的分子对接。随后,采用I-TASSER服务器预测配体位点。最后,将对接结果和预测位点与每个靶点的文献位点进行比较。
已鉴定出100多种寡聚缬菌素的潜在受体。其中,来自细菌的烯酰-ACP还原酶(Id1LXC)和胸苷酸合酶ThyX(Id 1O28)以及N-乙酰葡糖胺磷酸变位酶(Id 2DKD)与寡聚缬菌素表现出较强的相互作用,对接残基与辅因子/活性位点之间存在共定位。这些酶在原核生物的脂肪酸和DNA生物合成以及酵母的细胞壁合成中起关键作用。
因此,计算机模拟结果表明,寡聚缬菌素可损害脂肪酸、DNA及细胞壁合成,从而减少微生物增殖并导致微生物死亡。
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