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共生微生物群在炎症性肠病治疗和预防中的相关性。

Relevance of commensal microbiota in the treatment and prevention of inflammatory bowel disease.

机构信息

Division of Immunology, Department of Microbiology and Immunobiology, Harvard Medical School, Boston, Massachusetts.

出版信息

Inflamm Bowel Dis. 2013 Oct;19(11):2478-89. doi: 10.1097/MIB.0b013e318297d884.

Abstract

Commensal microbiota that reside primarily in the gut of mammals influence the hosts' health to a great extent. Shaping of host immunity locally, a vital component of this influence, can have pro-inflammatory, anti-inflammatory, or neutral outcomes, presumably depending on the composition of the microbiota in an individual and type of molecules expressed in the individual members of the microbiota. Thus, these microbial species can be thought of as a reservoir of molecules that can be used to improve or worsen the condition of patients suffering from immunity or inflammation-driven pathologies like inflammatory bowel disease. In the current review, we elaborate, based on the literature available from murine models of disease and clinical case studies, the need to identify individual members of commensal microbiota that can precipitate or resolve inflammatory bowel disease. Therapeutic approaches could entail enrichment of members of microbiota (or molecules from these microbes), which induces expansion or enhancement of function of regulatory T cells or tolerogenic dendritic cells and reduce members that cause inflammation either directly or indirectly by influencing metabolic and other host molecules. Efficiency of bacteria-driven therapy would potentially be enhanced as we refine our approaches from the use of complete feces as done in fecal transplantation to utilization of microbiota-derived molecules as exemplified by the capsular polysaccharide A from the human gut commensal Bacteroides fragilis. We also highlight the advantages and disadvantages of each approach, defining a natural alternative to the current chemical-based immunosuppressive regimen for patients with inflammatory bowel disease.

摘要

主要存在于哺乳动物肠道内的共生微生物群在很大程度上影响宿主的健康。这种影响的一个重要组成部分是局部塑造宿主免疫,其结果可能具有促炎、抗炎或中性,这可能取决于个体微生物群的组成和个体微生物群成员中表达的分子类型。因此,可以认为这些微生物物种是可以用来改善或恶化患有免疫或炎症驱动的疾病(如炎症性肠病)的患者病情的分子的储存库。在当前的综述中,我们根据来自疾病的小鼠模型和临床病例研究的文献,详细阐述了需要确定能够引发或解决炎症性肠病的共生微生物群的个体成员。治疗方法可能需要富集微生物群的成员(或这些微生物的分子),这会诱导调节性 T 细胞或耐受性树突状细胞的扩张或增强功能,并减少通过直接或间接影响代谢和其他宿主分子而引起炎症的成员。随着我们从使用完整粪便(如粪便移植中所做的那样)到利用微生物群衍生的分子(如人类肠道共生拟杆菌的荚膜多糖 A 所举例说明的那样)来改进我们的方法,细菌驱动的治疗效率将得到提高。我们还强调了每种方法的优缺点,为炎症性肠病患者定义了一种替代当前基于化学的免疫抑制方案的自然选择。

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