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这种益生菌可增强供体微生物群的稳定性,并提高粪便微生物群移植治疗结肠炎的疗效。

The probiotic enhances donor microbiota stability and improves the efficacy of fecal microbiota transplantation for treating colitis.

作者信息

Fan Jingjing, Wu Ying, Wang Xing, Ullah Habib, Ling Zhenmin, Liu Pu, Wang Yu, Feng Pengya, Ji Jing, Li Xiangkai

机构信息

Ministry of Education Key Laboratory of Cell Activities and Stress Adaptations, School of Life Sciences, Lanzhou University, Lanzhou, Gansu 730000, PR China.

Nutrition and Health Research Center, Lanzhou University, Lanzhou, Gansu 730000, PR China.

出版信息

J Adv Res. 2025 Mar 13. doi: 10.1016/j.jare.2025.03.017.

Abstract

INTRODUCTION

The stability and metabolic functionality of donor microbiota are critical determinants of fecal microbiota transplantation (FMT) efficacy in inflammatory bowel disease (IBD). While probiotics show potential to enhance microbiota resilience, their role in optimizing donor microbiota for FMT remains underexplored.

OBJECTIVES

This study investigated whether pretreatment of donor microbiota with L. plantarum GR-4 could improve FMT outcomes in a DSS-induced colitis model by modulating microbial stability, metabolic activity, and host-microbiome interactions.

METHODS

Donor mice received L. plantarum GR-4 for 3 weeks to generate modified FMT (MFMT). DSS-colitis mice were treated with MFMT, conventional FMT, or 5-aminosalicylic acid (5-ASA). Multi-omics analyses and functional assays (stress resistance, engraftment efficiency) were used to evaluate therapeutic mechanisms.

RESULTS

GR-4 pretreatment conferred three key advantages to donor microbiota: Ecological stabilization: 1. GR-4-driven acidification (pH 3.97 vs. 4.59 for LGG, p < 0.0001) enriched butyrogenic Butyricicoccus (73 % butyrate increase, p < 0.05) and improved stress resistance to bile acids/gastric conditions (1.25 × survival vs. FMT). 2. Metabolic reprogramming: GR-4 metabolized 25.3 % of tryptophan (vs. 10.3 % for LGG) to generate immunomodulatory indoles (ILA, IAA), activating aryl hydrocarbon receptor (AHR) signaling and upregulating anti-inflammatory IL-10/IL-22. 3. Bile acid remodeling: MFMT restored sulfolithocholic acid and β-MCA levels, outperforming FMT in resolving DSS-induced dysregulation. MFMT achieved an 83 % remission rate (vs. 50 % for FMT), enhanced gut barrier integrity, and reversed colitis-associated metabolic dysregulation (e.g., elevated spermidine, 7-sulfocholic acid). Probiotic preconditioning improved donor engraftment by 1.25 × and enriched success-associated taxa (Sporobacter, Butyricimonas), while suppressing pathogens (Clostridium papyrosolvens).

CONCLUSIONS

L. plantarum GR-4 optimizes donor microbiota via pH-driven niche engineering, immunometabolic reprogramming, and bile acid modulation, addressing key limitations of conventional FMT. The multi-targeted efficacy of MFMT, evidenced by superior remission rates and metabolic restoration, establishes this approach as a translatable strategy for IBD therapy. This study establishes probiotic-enhanced FMT as a paradigm for precision microbiome interventions.

摘要

引言

供体微生物群的稳定性和代谢功能是炎症性肠病(IBD)中粪便微生物群移植(FMT)疗效的关键决定因素。虽然益生菌显示出增强微生物群恢复力的潜力,但其在优化FMT供体微生物群方面的作用仍未得到充分探索。

目的

本研究调查了用植物乳杆菌GR-4对供体微生物群进行预处理是否可以通过调节微生物稳定性、代谢活性和宿主-微生物组相互作用来改善DSS诱导的结肠炎模型中的FMT结果。

方法

供体小鼠接受植物乳杆菌GR-4处理3周以产生改良FMT(MFMT)。DSS结肠炎小鼠接受MFMT、传统FMT或5-氨基水杨酸(5-ASA)治疗。采用多组学分析和功能测定(抗应激能力、植入效率)来评估治疗机制。

结果

GR-4预处理赋予供体微生物群三个关键优势:生态稳定:1. GR-4驱动的酸化(pH 3.97 vs. LGG的4.59,p < 0.0001)使产丁酸的丁酸球菌富集(丁酸盐增加73%,p < 0.05),并提高了对胆汁酸/胃部环境的抗应激能力(存活率是FMT的1.25倍)。2. 代谢重编程:GR-4将25.3%的色氨酸(vs. LGG的10.3%)代谢生成免疫调节性吲哚(ILA、IAA),激活芳烃受体(AHR)信号并上调抗炎性IL-10/IL-22。3. 胆汁酸重塑:MFMT恢复了牛磺石胆酸和β-MCA水平,在解决DSS诱导的失调方面优于FMT。MFMT实现了83%的缓解率(vs. FMT的50%),增强了肠道屏障完整性,并逆转了结肠炎相关的代谢失调(例如,亚精胺、7-磺胆酸升高)。益生菌预处理使供体植入率提高了1.25倍,并富集了与成功相关的分类群(芽孢杆菌、丁酸单胞菌),同时抑制了病原体(纸状梭菌)。

结论

植物乳杆菌GR-4通过pH驱动的生态位工程、免疫代谢重编程和胆汁酸调节来优化供体微生物群,解决了传统FMT的关键局限性。MFMT的多靶点疗效通过更高的缓解率和代谢恢复得到证明,确立了这种方法作为IBD治疗的可转化策略。本研究将益生菌增强的FMT确立为精准微生物组干预的范例。

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