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大蒜的抗糖化、抗氧化和蛋白质结构稳定性潜力的生物物理、生物化学和分子对接研究。

Biophysical, Biochemical, and Molecular Docking Investigations of Anti-Glycating, Antioxidant, and Protein Structural Stability Potential of Garlic.

机构信息

Department of Chemistry, College of Sciences, University of Ha'il, Ha'il 2440, Saudi Arabia.

Department of Biology, College of Sciences, University of Ha'il, Ha'il 2440, Saudi Arabia.

出版信息

Molecules. 2022 Mar 14;27(6):1868. doi: 10.3390/molecules27061868.

Abstract

Garlic has been reported to inhibit protein glycation, a process that underlies several disease processes, including chronic complications of diabetes mellitus. Biophysical, biochemical, and molecular docking investigations were conducted to assess anti-glycating, antioxidant, and protein structural protection activities of garlic. Results from spectral (UV and fluorescence) and circular dichroism (CD) analysis helped ascertain protein conformation and secondary structure protection against glycation to a significant extent. Further, garlic showed heat-induced protein denaturation inhibition activity (52.17%). It also inhibited glycation, advanced glycation end products (AGEs) formation as well as lent human serum albumin (HSA) protein structural stability, as revealed by reduction in browning intensity (65.23%), decrease in protein aggregation index (67.77%), and overall reduction in cross amyloid structure formation (33.26%) compared with positive controls (100%). The significant antioxidant nature of garlic was revealed by FRAP assay (58.23%) and DPPH assay (66.18%). Using molecular docking analysis, some of the important garlic metabolites were investigated for their interactions with the HSA molecule. Molecular docking analysis showed quercetin, a phenolic compound present in garlic, appears to be the most promising inhibitor of glucose interaction with the HSA molecule. Our findings show that garlic can prevent oxidative stress and glycation-induced biomolecular damage and that it can potentially be used in the treatment of several health conditions, including diabetes and other inflammatory diseases.

摘要

大蒜已被报道能抑制蛋白质糖基化,这一过程是多种疾病的基础,包括糖尿病的慢性并发症。本研究通过生物物理、生物化学和分子对接研究评估了大蒜的抗糖基化、抗氧化和蛋白质结构保护活性。光谱(紫外和荧光)和圆二色性(CD)分析的结果有助于确定蛋白质构象,并在很大程度上保护二级结构免受糖基化的影响。此外,大蒜表现出热诱导的蛋白质变性抑制活性(52.17%)。它还能抑制糖基化、晚期糖基化终产物(AGEs)的形成以及人血清白蛋白(HSA)的蛋白质结构稳定性,这表现为褐变强度的降低(65.23%)、蛋白质聚集指数的降低(67.77%)以及交叉淀粉样结构形成的总体减少(33.26%),与阳性对照(100%)相比。FRAP 测定法(58.23%)和 DPPH 测定法(66.18%)显示大蒜具有显著的抗氧化性质。通过分子对接分析,研究了一些重要的大蒜代谢物与 HSA 分子的相互作用。分子对接分析表明,大蒜中存在的一种酚类化合物槲皮素,似乎是抑制葡萄糖与 HSA 分子相互作用的最有前途的抑制剂。我们的研究结果表明,大蒜可以防止氧化应激和糖基化诱导的生物分子损伤,并且它可能被用于治疗几种健康状况,包括糖尿病和其他炎症性疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fbac/8950752/18ea66af5faf/molecules-27-01868-g001.jpg

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