Xiang Boyu, An Jinshun, Li Dongjie
Department of Urology, Andrology Center, Xiangya Hospital, Central South University, Changsha 410008, P.R. China.
Institute of Andrology, Central South University, Changsha 410008, P.R. China.
Sex Med. 2025 Jun 2;13(3):qfaf039. doi: 10.1093/sexmed/qfaf039. eCollection 2025 Jun.
Growing evidence suggests that alterations in the gut microbiota may contribute to the pathogenesis of erectile dysfunction (ED).
To investigate the potential causal relationship between specific gut microbial taxa and ED, identify key microbial metabolites and their associated target genes, and evaluate their therapeutic potential through computational drug screening.
Genome-wide association study (GWAS) summary statistics for gut microbiota and ED were obtained from the MiBioGen, IEU OpenGWAS, and FinnGen databases. Mendelian randomization (MR) analysis was performed using the TwoSampleMR package to assess potential causal relationships. A microbiota-metabolite-target gene network was constructed using data from GutMGene, Super-PRED, and GeneCards databases to explore the microbiota-host interaction axis. The DeepPurpose machine learning framework was utilized to predict drug-target binding affinities, and top-ranking drug-gene pairs were validated by molecular docking to assess binding free energies and confirm interaction stability.
The study aimed to identify specific gut microbiota, metabolites, and target genes associated with ED and evaluate their therapeutic potential.
MR analysis revealed a negative association between ED and the gut microbial genera , , and , suggesting a potential protective role. Machine learning predictions indicated strong binding affinities between target genes (, , ) and bile acid derivatives (Tauroursodeoxycholic acid and Taurochenodeoxycholic acid). Molecular docking confirmed high binding affinities of to Tauroursodeoxycholic acid (-9.81 kcal/mol) and Taurochenodeoxycholic acid (-9.35 kcal/mol).
These findings suggest that gut microbiota and their metabolites could serve as potential therapeutic targets for ED interventions.
The study provides novel insights into the gut microbiota-ED relationship by integrating multi-omics data and advanced computational methods. However, validation in preclinical or clinical studies is needed to translate these findings into therapeutic applications.
Specific gut microbiota, through metabolites and associated target genes, may influence the onset of ED. These findings highlight potential therapeutic targets and provide a basis for future interventions in ED treatment.
越来越多的证据表明,肠道微生物群的改变可能有助于勃起功能障碍(ED)的发病机制。
研究特定肠道微生物分类群与ED之间的潜在因果关系,识别关键微生物代谢产物及其相关靶基因,并通过计算药物筛选评估其治疗潜力。
从MiBioGen、IEU OpenGWAS和FinnGen数据库中获取肠道微生物群和ED的全基因组关联研究(GWAS)汇总统计数据。使用TwoSampleMR软件包进行孟德尔随机化(MR)分析,以评估潜在的因果关系。利用来自GutMGene、Super-PRED和GeneCards数据库的数据构建微生物群-代谢产物-靶基因网络,以探索微生物群与宿主的相互作用轴。利用DeepPurpose机器学习框架预测药物与靶标的结合亲和力,并通过分子对接验证排名靠前的药物-基因对,以评估结合自由能并确认相互作用稳定性。
该研究旨在识别与ED相关的特定肠道微生物群、代谢产物和靶基因,并评估其治疗潜力。
MR分析显示ED与肠道微生物属、和之间存在负相关,表明其可能具有保护作用。机器学习预测表明靶基因(、和)与胆汁酸衍生物(牛磺熊去氧胆酸和牛磺鹅去氧胆酸)之间具有很强的结合亲和力。分子对接证实与牛磺熊去氧胆酸(-9.81 kcal/mol)和牛磺鹅去氧胆酸(-9.35 kcal/mol)具有高结合亲和力。
这些发现表明肠道微生物群及其代谢产物可能作为ED干预的潜在治疗靶点。
该研究通过整合多组学数据和先进的计算方法,为肠道微生物群与ED的关系提供了新的见解。然而,需要在临床前或临床研究中进行验证,才能将这些发现转化为治疗应用。
特定的肠道微生物群可能通过代谢产物和相关靶基因影响ED的发病。这些发现突出了潜在的治疗靶点,并为未来ED治疗干预提供了依据。
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