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阿福花科马鲁若塔次生代谢产物对 SARS-CoV-2 药物靶点表现出多效性:对弗林抑制的体外验证。

Aframomum melegueta secondary metabolites exhibit polypharmacology against SARS-CoV-2 drug targets: in vitro validation of furin inhibition.

机构信息

Chemo-Genomics Research Unit, Department of Biochemistry, Adekunle Ajasin University, Akungba, Nigeria.

Chemoinformatics Unit, Mols & Sims, Ado Ekiti, Nigeria.

出版信息

Phytother Res. 2021 Feb;35(2):908-919. doi: 10.1002/ptr.6843. Epub 2020 Sep 22.

Abstract

COVID-19 pandemic is currently decimating the world's most advanced technologies and largest economies and making its way to the continent of Africa. Weak medical infrastructure and over-reliance on medical aids may eventually predict worse outcomes in Africa. To reverse this trend, Africa must re-evaluate the only area with strategic advantage; phytotherapy. One of the many plants with previous antiviral potency is against RNA viruses is Aframomum melegueta. In this study, one hundred (100) A. melegueta secondary metabolites have been mined and computational evaluated for inhibition of host furin, and SARS-COV-2 targets including 3C-like proteinase (M /3CL ), 2'-O-ribose methyltransferase (nsp16) and surface glycoprotein/ACE2 receptor interface. Silica-gel column partitioning of A. melegueta fruit/seed resulted in 6 fractions tested against furin activity. Diarylheptanoid (Letestuianin A), phenylpropanoid (4-Cinnamoyl-3-hydroxy-spiro[furan-5,2'-(1'H)-indene]-1',2,3'(2'H,5H)-trione), flavonoids (Quercetin, Apigenin and Tectochrysin) have been identified as high-binding compounds to SARS-COV-2 targets in a polypharmacology manner. Di-ethyl-ether (IC = 0.03 mg/L), acetone (IC = 1.564 mg/L), ethyl-acetate (IC = 0.382 mg/L) and methanol (IC = 0.438 mg/L) fractions demonstrated the best inhibition in kinetic assay while DEF, ASF and MEF completely inhibited furin-recognition sequence containing Ebola virus-pre-glycoprotein. In conclusion, A. melegueta and its secondary metabolites have potential for addressing the therapeutic needs of African population during the COVID-19 pandemic.

摘要

COVID-19 大流行正在摧毁世界上最先进的技术和最大的经济体,并蔓延到非洲大陆。薄弱的医疗基础设施和过度依赖医疗援助可能最终导致非洲出现更糟糕的结果。为了扭转这一趋势,非洲必须重新评估其唯一具有战略优势的领域;植物疗法。许多具有先前抗病毒效力的植物之一是针对 RNA 病毒的 Aframomum melegueta。在这项研究中,已经挖掘并计算评估了 100 种 A. melegueta 次生代谢产物,以抑制宿主弗林蛋白酶和 SARS-COV-2 靶标,包括 3C 样蛋白酶(M/3CL)、2'-O-核糖甲基转移酶(nsp16)和表面糖蛋白/ACE2 受体界面。A. melegueta 果实/种子的硅胶柱分馏得到了 6 个馏分,用于测试对弗林酶活性的抑制作用。二芳基庚烷(Letestuianin A)、苯丙素(4-肉桂酰-3-羟基-螺[furan-5,2'-(1'H)-indene]-1',2,3'(2'H,5H)-trione)、类黄酮(槲皮素、芹菜素和 tectochrysin)已被鉴定为通过多药理学方式与 SARS-COV-2 靶标结合的高结合化合物。二乙基醚(IC = 0.03 mg/L)、丙酮(IC = 1.564 mg/L)、乙酸乙酯(IC = 0.382 mg/L)和甲醇(IC = 0.438 mg/L)馏分在动力学测定中显示出最佳抑制作用,而 DEF、ASF 和 MEF 则完全抑制了含有埃博拉病毒前糖蛋白的弗林识别序列。总之,A. melegueta 及其次生代谢产物具有在 COVID-19 大流行期间满足非洲人口治疗需求的潜力。

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