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甘草素:一种用于治疗勃起功能障碍的潜在药物候选物。

Isoliquiritigenin: a potential drug candidate for the management of erectile dysfunction.

机构信息

Department of Zoology, Mangaldai College, Mangaldai, Assam 784125, India.

Department of Zoology, Tihu College, Tihu, Assam 781371, India.

出版信息

J Pharm Pharmacol. 2024 Aug 2;76(8):1065-1077. doi: 10.1093/jpp/rgae054.

DOI:10.1093/jpp/rgae054
PMID:38865360
Abstract

OBJECTIVE

This study aimed to assess the erectogenic properties of isoliquiritigenin taking sildenafil (SDF) as the standard.

METHODS

The binding affinity of isoliquiritigenin (ISL) with the erectile marker proteins (endothelial nitric oxide synthase [eNOS] and enzyme phosphodiesterase type 5 [PDE5]) was investigated using Autodock Vina, which was validated using molecular dynamics simulation. Furthermore, the effect of ISL on the eNOS and PDE5 messenger ribonucleic acid (mRNA) expression and the sexual behavior of mice was investigated, along with the assessment of the pharmacokinetics of ISL.

KEY FINDINGS

The results revealed that the binding affinity of ISL-eNOS/PDE5 and SDF-eNOS/PDE5 was in the range of -7.5 to -8.6 kcal/mol. The ISL-eNOS/PDE5 complexes remained stable throughout the 100 ns simulation period. Root mean square deviation, Rg, SASA, hydrogen, and hydrophobic interactions were similar between ISL-eNOS/PDE5 and SDF-eNOS/PDE5. Analysis of mRNA expressions in paroxetine (PRX)-induced ED mice showed that the co-administration of PRX with ISL reduced PDE5 and increased eNOS mRNA expression, similar to the co-administered group (PRX+SDF). The sexual behavior study revealed that the results of PRX+ISL were better than those of the PRX+SDF group. Pharmacokinetic evaluation further demonstrated that ISL possesses drug-like properties.

CONCLUSIONS

The results showed that ISL is equally potent as SDF in terms of binding affinity, specific pharmacological properties, and modulating sexual behavior.

摘要

目的

本研究旨在评估异甘草素(ISL)的勃起性能,以西地那非(SDF)作为标准。

方法

使用 Autodock Vina 研究 ISL 与勃起标志物蛋白(内皮型一氧化氮合酶[eNOS]和酶磷酸二酯酶 5 [PDE5])的结合亲和力,并使用分子动力学模拟进行验证。此外,还研究了 ISL 对 eNOS 和 PDE5 信使核糖核酸(mRNA)表达的影响以及对小鼠性行为的影响,并评估了 ISL 的药代动力学。

主要发现

结果表明,ISL-eNOS/PDE5 和 SDF-eNOS/PDE5 的结合亲和力在-7.5 至-8.6 kcal/mol 范围内。在整个 100 ns 模拟期间,ISL-eNOS/PDE5 复合物保持稳定。均方根偏差(Rg)、SASA、氢键和疏水性相互作用在 ISL-eNOS/PDE5 和 SDF-eNOS/PDE5 之间相似。在帕罗西汀(PRX)诱导的 ED 小鼠中分析 mRNA 表达显示,PRX 与 ISL 联合给药可降低 PDE5 并增加 eNOS mRNA 表达,与联合给药组(PRX+SDF)相似。性行为研究表明,PRX+ISL 的结果优于 PRX+SDF 组。药代动力学评价进一步表明,ISL 具有类药性。

结论

结果表明,ISL 在结合亲和力、特定药理学特性和调节性行为方面与 SDF 一样有效。

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