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多队列分析揭示了治疗高尿酸血症和痛风的新型微生物靶点。

Multi-cohort analysis unveils novel microbial targets for the treatment of hyperuricemia and gout.

作者信息

Qie Jinlong, Cao Man, Xu Min, Zhang Yingjie, Luo Liangen, Sun Chuqing, Ke Dongxian, Yuan Songjian, Jia Wenting, Qiu Tianhua, Li Tianhua, Du Xiaoman, Xiao Chuanxing, Hong Zhenqiang, Zhang Bangzhou

机构信息

School of Pharmacy, Fujian University of Traditional Chinese Medicine, Fuzhou, China.

School of Traditional Chinese Medicine, Fujian University of Traditional Chinese Medicine, Fuzhou, China.

出版信息

mSystems. 2025 Sep 17:e0109125. doi: 10.1128/msystems.01091-25.

Abstract

The gut microbiota plays a crucial role in the development of hyperuricemia (HUA) and gout. However, the variability in study designs and analytical methods has led to inconsistent conclusions across different studies. Here, we conducted a comprehensive analysis of the gut microbiota associated with HUA and gout by examining 368 16S rRNA sequencing data from four Chinese cohorts, including 159 healthy controls (HC), 136 HUA patients, and 73 gout patients. Our findings indicate that there were significant differences in the gut microbiota composition between the three groups. Specifically, the HUA and gout groups demonstrated an increased abundance of pro-inflammatory bacteria, such as and , while beneficial bacteria known for their anti-inflammatory properties and metabolic benefits, including R-7 group, and , are relatively reduced. Additionally, we developed a predictive model using microbial markers that achieved a high accuracy (area under the curve [AUC] > 0.8) in distinguishing between the HC, HUA, and gout groups. Notably, further metagenomic analysis identified a species-level genome bin (SGB), designated as , belonging to the order . For the first time, we discovered that this SGB carries a uric acid metabolic gene cluster and possesses enzymes associated with purine metabolism, suggesting its potential role in uric acid metabolism. Overall, our study deepens the understanding of the gut microbiota's role in HUA and gout and lays a foundation for developing innovative therapeutic strategies to effectively control uric acid levels through gut microbiota modulation.In this study, we conducted a comprehensive analysis of gut microbiota across multiple cohorts, identifying distinct microbial signatures in healthy controls, hyperuricemia (HUA), and gout patients. We observed an increase in pro-inflammatory bacteria and a decrease in beneficial bacteria for host metabolism in both the HUA and gout groups. Additionally, we developed a predictive model with high accuracy (area under the curve [AUC] > 0.8) based on microbial markers and discovered a novel species with potential for uric acid metabolism, providing new therapeutic targets for HUA and gout.

摘要

肠道微生物群在高尿酸血症(HUA)和痛风的发展中起着至关重要的作用。然而,研究设计和分析方法的差异导致不同研究得出的结论不一致。在此,我们通过检查来自四个中国队列的368个16S rRNA测序数据,对与HUA和痛风相关的肠道微生物群进行了全面分析,其中包括159名健康对照(HC)、136名HUA患者和73名痛风患者。我们的研究结果表明,三组之间肠道微生物群组成存在显著差异。具体而言,HUA组和痛风组中促炎细菌(如 和 )的丰度增加,而具有抗炎特性和代谢益处的有益细菌(包括R-7组、 和 )相对减少。此外,我们使用微生物标志物开发了一种预测模型,该模型在区分HC组、HUA组和痛风组方面具有较高的准确性(曲线下面积[AUC]>0.8)。值得注意的是,进一步的宏基因组分析鉴定出一个物种水平的基因组 bins(SGB),命名为 ,属于 目。我们首次发现该SGB携带尿酸代谢基因簇并拥有与嘌呤代谢相关的酶,表明其在尿酸代谢中的潜在作用。总体而言,我们的研究加深了对肠道微生物群在HUA和痛风中作用的理解,并为通过调节肠道微生物群有效控制尿酸水平开发创新治疗策略奠定了基础。在本研究中,我们对多个队列的肠道微生物群进行了全面分析,确定了健康对照、高尿酸血症(HUA)和痛风患者中不同的微生物特征。我们观察到HUA组和痛风组中促炎细菌增加,对宿主代谢有益的细菌减少。此外,我们基于微生物标志物开发了一种具有高准确性(曲线下面积[AUC]>0.8)的预测模型,并发现了一种具有尿酸代谢潜力的新物种,为HUA和痛风提供了新的治疗靶点。

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