Feiyan Zhao , Ning Tie , Lai-Yu Kwok , Teng Ma , Jing Wang , Dafu Man , Xiangzheng Yuan , Huiyun Li , Lixia Pang , Hui Shi , Shuiming Ren , Zhongjie Yu , Xin Shen , Hongbin Li , Heping Zhang
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Based on achieving a target sUA level (360 μmol/L) after the intervention, the probiotic group was further subdivided into probiotic-responsive (ProA; n = 54) and probiotic-unresponsive (ProB; n = 66) subgroups. Post-intervention clinical indicators, metagenomic, and metabolomic changes in the ProB and placebo groups were similar, but differed from those in the ProA group, which exhibited significantly lower levels of acute gout attack, gout impact score, serum indicators (UA, XOD, hypoxanthine, and IL-1β), and fecal gene abundances of UA-producing pathways (KEGG orthologs of K13479 and K01487; gut metabolic modules for formate conversion and lactose and galactose degradation). Additionally, the ProA group showed significantly higher levels (<em>P</em> < 0.05) of gut SCFAs-producing bacteria and UA-related metabolites (xanthine, hypoxanthine, bile acids) after the intervention. Finally, we established a gout metagenomic classifier to predict probiotic responsiveness based on subjects’ baseline gut microbiota composition. 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引用次数: 0
摘要
痛风的特点是尿酸(UA)代谢失调,而肠道微生物群可能是一个调节靶点。这项为期两个月的随机、双盲、安慰剂对照试验旨在研究在服用非布索坦的同时服用普罗比奥-X的额外益处。共有160名痛风患者被随机分配到益生菌组(n = 120;Probio-X [1 ×1011 CFU/天] 与非布司他)或安慰剂组(n = 40;安慰剂材料与非布司他)。同时服用 Probio-X 可显著降低血清 UA 水平和痛风急性发作率(P < 0.05)。根据干预后达到目标 sUA 水平(360 μmol/L)的情况,益生菌组又进一步细分为益生菌有反应(ProA;n = 54)和益生菌无反应(ProB;n = 66)两组。ProB组和安慰剂组干预后的临床指标、元基因组和代谢组变化相似,但与ProA组不同,ProA组的痛风急性发作水平、痛风影响评分、血清指标(UA、XOD、次黄嘌呤和IL-1β)以及粪便中产生UA通路的基因丰度(KEGG直向同源物K13479和K01487;甲酸盐转化以及乳糖和半乳糖降解的肠道代谢模块)均显著降低。此外,干预后,ProA 组的肠道 SCFAs 产生菌和 UA 相关代谢物(黄嘌呤、次黄嘌呤、胆汁酸)水平明显更高(P < 0.05)。最后,我们建立了痛风元基因组分类器,根据受试者的基线肠道微生物群组成预测益生菌的反应性。我们的研究结果表明,益生菌驱动的治疗反应具有很强的个体差异性,具有益生菌反应的受试者群可从联合服用益生菌中显著获益。
Baseline gut microbiome as a predictive biomarker of response to probiotic adjuvant treatment in gout management
Gout is characterized by dysregulation of uric acid (UA) metabolism, and the gut microbiota may serve as a regulatory target. This two-month randomized, double-blind, placebo-controlled trial aimed to investigate the additional benefits of coadministering Probio-X alongside febuxostat. A total of 160 patients with gout were randomly assigned to either the probiotic group (n = 120; Probio-X [1 ×1011 CFU/day] with febuxostat) or the placebo group (n = 40; placebo material with febuxostat). Coadministration of Probio-X significantly decreased serum UA levels and the rate of acute gout attacks (P < 0.05). Based on achieving a target sUA level (360 μmol/L) after the intervention, the probiotic group was further subdivided into probiotic-responsive (ProA; n = 54) and probiotic-unresponsive (ProB; n = 66) subgroups. Post-intervention clinical indicators, metagenomic, and metabolomic changes in the ProB and placebo groups were similar, but differed from those in the ProA group, which exhibited significantly lower levels of acute gout attack, gout impact score, serum indicators (UA, XOD, hypoxanthine, and IL-1β), and fecal gene abundances of UA-producing pathways (KEGG orthologs of K13479 and K01487; gut metabolic modules for formate conversion and lactose and galactose degradation). Additionally, the ProA group showed significantly higher levels (P < 0.05) of gut SCFAs-producing bacteria and UA-related metabolites (xanthine, hypoxanthine, bile acids) after the intervention. Finally, we established a gout metagenomic classifier to predict probiotic responsiveness based on subjects’ baseline gut microbiota composition. Our results indicate that probiotic-driven therapeutic responses are highly individual, with the probiotic-responsive cohort benefitting significantly from probiotic coadministration.
期刊介绍:
Pharmacological Research publishes cutting-edge articles in biomedical sciences to cover a broad range of topics that move the pharmacological field forward. Pharmacological research publishes articles on molecular, biochemical, translational, and clinical research (including clinical trials); it is proud of its rapid publication of accepted papers that comprises a dedicated, fast acceptance and publication track for high profile articles.