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小肠细菌过度生长在肝硬化中的驱动作用及相关靶向治疗策略

李仙萍 唐映梅

引用本文:
Citation:

小肠细菌过度生长在肝硬化中的驱动作用及相关靶向治疗策略

DOI: 10.12449/JCH260629
基金项目: 

国家自然科学基金 (82360108);

云南省医学领军人才 (L-2019013)

利益冲突声明:本文不存在任何利益冲突。
作者贡献声明:李仙萍负责设计论文框架,起草论文,修改论文;唐映梅负责拟定写作思路,指导撰写文章并最后定稿。
详细信息
    通信作者:

    唐映梅, tangyingmei_med@kmmu.edu.cn (ORCID: 0000-0002-0731-4198)

Driving role and related targeted therapeutic strategies of small intestinal bacterial overgrowth in liver cirrhosis

Research funding: 

National Natural Science Foundation of China (82360108);

Medicine Leading Talents of Yunnan Province (L-2019013)

More Information
  • 摘要: 小肠细菌过度生长(SIBO)在肝硬化患者中的发生率显著升高。近年研究表明,SIBO不仅是一种伴随现象,更是通过“肠-肝轴”机制主动驱动肝硬化进展的关键因素。本文创新性提出“菌群-免疫-纤维化”病理正反馈循环模型,系统阐述了SIBO通过破坏肠道屏障功能、促进细菌及内毒素易位、诱发系统性炎症反应及加速肝纤维化等多重机制,推动疾病进展的连续性病理过程。同时,评估了目前针对SIBO的抗生素治疗、微生态调节、中草药治疗及饮食疗法等策略的临床应用价值与局限,为开发多靶点、个体化的综合治疗策略提供了理论依据与未来研究方向。

     

  • 注: SIBO,小肠细菌过度生长;LPS,脂多糖;TLR4,Toll样受体4;NF-κB,核因子κB;TNF-α,肿瘤坏死因子α;IL,白细胞介素;MyD88,髓样分化因子88;Bambi,骨形态发生蛋白和激活素膜结合抑制剂;TGF-β,转化生长因子β。

    图  1  SIBO促进肝硬化进展的核心机制

    Figure  1.  Core mechanism of SIBO promoting cirrhosis progression

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