An in silico study involving Mangiferin, 7-Epiclusianone, Fukugetin, Lapachol, Plumbagin and Guttiferone-A against C. albicans proteins

A. Barros, Leonardo Pereira de Araújo, N. Silveira, B. Santos
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引用次数: 1

Abstract

It is notorious that since the beginnings of spacetime, the human being lives with microorganisms of countless forms, be it in a positive way as in case of Bacteroidetes present in the intestine’s microbiota or negative way as in case of recent epidemic of Sars-Cov-2. So, the negative impacts caused by microorganisms are objects of study in the whole world, for instance, Candida albicans, which is a fungus that lives in the human body symbiotically and assists in the maintenance of body homeostasis, but the same can present an invasive features that become harmful to the human health, mainly in people who present some kind of immunodeficiency, causing its proliferation to become exacerbated, may cause the death. Said that, the use of drugs to control C. albicans is very important, being the nystatin and fluconazole that are the ones that are currently used. However, the updating of such medicines as time goes by becomes ineffective to some kinds of strains, since the capacity of the fungus in evolution creates resistance to medicines. So, the Discovery of new drugs is necessary and natural products are an excellent research source for the same. Therefore, this study made the methodology in silico of molecular docking to investigate the forms of connection of the natural compounds fukugetin, guttiferone-A, lapachol, mangiferin, plumbagin and 7-epiclusianone in potential molecular targets of fungus Candida albicans.
一项涉及芒果苷、7-依壁鸠鲁酮、福古苷、拉帕恰尔、白莲花苷和古提铁酮- a抗白色念珠菌蛋白的计算机研究
众所周知,从时空开始,人类就与无数形式的微生物生活在一起,无论是正面的方式,如肠道微生物群中存在的拟杆菌门,还是负面的方式,如最近流行的Sars-Cov-2。因此,微生物造成的负面影响是全世界研究的对象,例如,白色念珠菌,它是一种真菌,共生生活在人体中,帮助维持人体稳态,但同样可以呈现出侵入性的特征,对人体健康有害,主要是在出现某种免疫缺陷的人身上,使其增殖加剧,可能导致死亡。说,使用药物控制白色念珠菌是非常重要的,制霉菌素和氟康唑是目前使用的药物。然而,随着时间的推移,这些药物的更新对某些菌株无效,因为真菌在进化中的能力产生了对药物的耐药性。因此,新药的发现是必要的,天然产物是一个很好的研究来源。因此,本研究采用分子对接的方法,研究天然化合物fukugetin、guttiferone-A、lapachhol、mangiferin、plumbagin和7-epiclusianone在白色念珠菌潜在分子靶点中的连接形式。
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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