通过体外和计算机方法鉴定口腔疾病的新型蓝藻化合物

Vijayakumar Madhumathi, Suburamaniyan Vijayakumar
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引用次数: 2

摘要

在本研究中,我们对铜绿微囊藻和灰磷进行了生物活性化合物筛选对接研究。采用薄层色谱(TLC)和气相色谱-质谱(GC-MS)分析了两种蓝绿藻中生物活性物质的化学性质。所鉴定的抗菌化合物有酚类、生物碱、类固醇等。本研究报道了铜绿假单胞菌凝乳提取物中含有生物活性化合物Microginins,而从铜绿假单胞菌中检测到Cyalobolide B。对M. aeruginosa (Microginins)进行植物化学分析,提供乙烷酸、辛烷酸、3,7,11-三甲基-1,6,10-十二烷基-3-醇(神经胶质)、单甲基肼和甲酸。这些植物化学物质的累积效应为抑制微生物生长提供了更有效的抗菌化合物。Cyalobolide B的植物化学分析显示:乙烷酸、二氢二plodiide、3,7,11 -三甲基- 1,6,10 -十二烷基-3-醇(神经胶质)、1-十二烷醇、1-十六烷醇(CAS)和纳米酸。这些化合物在抑制微生物生长方面表现出更有效的抗菌物质。一个群落的哪些成员与自身以及与白色念珠菌和变形链球菌的不同宿主结构和成分相互作用。这种口腔感染的发病机制是一个多因素的过程,导致口腔念珠菌病的严重退行性疾病。本研究以SAP(分泌的天冬氨酸蛋白酶在毒力和发病机制中的作用)为个案研究分子,了解各种药物对口腔念珠菌病的高反应性反应。将这些药物与白色念珠菌的SAP和变形链球菌的细胞表面抗原SpaP基因进行比较。SAP和SpaP通过对接方式与甲酸、神经胶质、辛醇和壬酸相互作用。如果能够达到足够的准确性,计算方法的指数级增长速度使得在药物发现的早期阶段更广泛的应用具有吸引力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Identification of novel cyanobacterial compounds for oral disease through in vitro and insilico approach

In this research, we have conducted docking study to screen bioactive compounds from Microcystis aeruginosa and Phormidium corium. Among the two blue-green algal species were analyzed for chemical nature of bioactive substances using TLC and GC-MS methods. The antimicrobial compounds identified were phenolics, alkaloids, steroids. In the present study as reported that M. aeruginosa curde extract contained the bioactive compound Microginins, while Cyalobolide B was detected from P. corium. The phytochemical analysis of M. aeruginosa (Microginins), provided ethaneloic acid, Octanal, 3,7,11-Trimethyl-1,6,10-dodecatrien-3-ol (nerolidal), Monomethyl hydrazine and formic acid. The cumulative effect of these phytochemical provided more effective antimicrobial compound in inhibiting microbial growth. The phytochemical analysis of P. corium (Cyalobolide B) exhibited Ethaneloic acid, Dihydrodiplodialide, 3, 7, 11-Trimethyl-1, 6, 10-dodecatrien-3-ol (nerolidal), 1-Dodecanol, 1-Hexadecanol (CAS) and nanonic acid. These compounds together exhibited more effective antimicrobial substance in inhibiting microbial growth. Which members of a community interact with themselves as well as with different host structures and components of Candida albicans and Streptococcus mutans. The pathogenesis of this dental infection is a multi factorial process that results in a serious degenerative disease of the Oral candidiasis. In the present study SAP (secreted aspartyl proteinases in virulence and pathogenesis) is taken as a case study molecule to understand high reactive responses of various drugs administered for the oral candidiasis. The drugs are being compared with the SAP from C. albicans and SpaP (cell surface antigen SpaP gene) from S. mutans. The SAP and SpaP interacted with formic acid, nerolidal, octanol and nonanoic acid using docking methods. The exponentially increasing speed of computational methods makes a more extensive use in the early stages of drug discovery attractive if sufficient accuracy can be achieved.

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