Natália Gonçalves Ribeiro Araujo, Francisco Carlos da Silva Junior, Lizandra Vitória de Souza Santos, Silvia Regina Batistuzzo de Medeiros, Israel Felzenszwalb, Carlos Fernando Araújo-Lima
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Further than this, the molecular docking was performed. The compounds present in the aqueous extract of <i>C. glutiniferum</i> were identified by UHPLC-MS/MS, finding Arbutin, Caffeic acid 4-O-glucoside, and Dihydroformononetin as the three most abundant molecules. The evaluation of the gastrointestinal absorption of Dihydroformononetin is given as high, also managing to cross the blood-brain barrier, while Arbutin can only be absorbed by the gastrointestinal tract and Caffeic acid 4-O-glucoside had very low absorption. Further analysis showed that Arbutin and Dihydroformononetin are possible leading molecules for drug synthesis, according to the prediction. Toxicological aspects were analysed, and no adverse effects were noted, but there were divergences in the mutagenic prediction of Arbutin and Dihydroformononetin, having different results in the used platforms, demonstrating that a cautious analysis and data insertion is needed in these tools to optimize them. The analysis of the differentially expressed genes predicted that the compounds can regulate several genes, including some genes associated with carcinogenesis and inflammation. The Molecular docking analysis showed high binding affinities of the molecules with different proteins. Therefore, <i>C. glutiniferum</i> demonstrates the potential to be used as a phytotherapeutic. 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引用次数: 0
摘要
兰属,兰科植物,因其治疗结核、脓肿、泌尿系统感染和感冒的特性而被广泛使用。C. glutiniferum是该属的一种,是巴西特有的,主要用于草药。因此,认识它的组成和在其中发现的分子的性质是非常有趣的。本研究在pKCSM、SwissADME、LAZAR、CLC-pred、ToxTree、DIGEPred、STRING和Cytoscape等平台上对黄姜中的主要化合物进行了硅晶分析。在此基础上,进行了分子对接。采用高效液相色谱-质谱联用技术对其进行鉴定,发现熊果苷、咖啡酸4- o -葡萄糖苷和二氢芒柄花素为含量最多的3种化合物。二氢刺芒柄花素的胃肠道吸收评价高,也能通过血脑屏障,熊果苷只能通过胃肠道吸收,咖啡酸4- o -葡萄糖苷的吸收率很低。进一步分析表明,熊果苷和二氢芒柄花素可能是药物合成的先导分子。毒理学方面进行了分析,未发现不良反应,但熊果苷和双氢芒柄花素的致突变性预测存在分歧,在所使用的平台上有不同的结果,表明这些工具需要谨慎分析和数据插入以优化它们。对差异表达基因的分析预测,这些化合物可以调节几种基因,包括一些与致癌和炎症有关的基因。分子对接分析表明,这些分子与不同的蛋白质具有较高的结合亲和力。因此,谷草具有作为植物治疗药物的潜力。通过对兰花中发现的三种化合物的计算机分析也得出了同样的结论,它们显示出良好的个体潜力。
Molecular docking and in silico analysis of the pharmacokinetics, toxicological profile and differential gene expression of bioactive compounds from Cyrtopodium glutiniferum.
The genus Cyrtopodium, from the Orchidaceae family, is widely used for its therapeutic properties in the treatment of tuberculosis, abscesses, urinary infection, and colds. C. glutiniferum, one of the species of this genus, is endemic in Brazil and largely used in herbal medicine. Thus, it is of great interest to recognize its composition, the properties of the molecules found in it. This study aimed to perform the in silico analysis of the main compounds from C. glutiniferum, on the platforms pKCSM, SwissADME, LAZAR, CLC-pred, ToxTree, DIGEPred, STRING, and Cytoscape. Further than this, the molecular docking was performed. The compounds present in the aqueous extract of C. glutiniferum were identified by UHPLC-MS/MS, finding Arbutin, Caffeic acid 4-O-glucoside, and Dihydroformononetin as the three most abundant molecules. The evaluation of the gastrointestinal absorption of Dihydroformononetin is given as high, also managing to cross the blood-brain barrier, while Arbutin can only be absorbed by the gastrointestinal tract and Caffeic acid 4-O-glucoside had very low absorption. Further analysis showed that Arbutin and Dihydroformononetin are possible leading molecules for drug synthesis, according to the prediction. Toxicological aspects were analysed, and no adverse effects were noted, but there were divergences in the mutagenic prediction of Arbutin and Dihydroformononetin, having different results in the used platforms, demonstrating that a cautious analysis and data insertion is needed in these tools to optimize them. The analysis of the differentially expressed genes predicted that the compounds can regulate several genes, including some genes associated with carcinogenesis and inflammation. The Molecular docking analysis showed high binding affinities of the molecules with different proteins. Therefore, C. glutiniferum demonstrates the potential to be used as a phytotherapeutic. The same was given through the in silico analysis of the three compounds found in the orchid, that show good individual potential.
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