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二十年来,从病因到治疗,肠道菌群与炎症性肠病一览无余。

Highlights on two decades with microbiota and inflammatory bowel disease from etiology to therapy.

机构信息

Oakland University William Beaumont School of Medicine, Rochester, MI, USA.

Department of Anatomy, Biology and Physiological Sciences, Faculty of Medicine, American University of Beirut, Beirut, Lebanon; Department of Biomedicine, Neuroscience and Advanced Diagnostics, Institute of Human Anatomy and Histology, University of Palermo, Palermo, Italy.

出版信息

Transpl Immunol. 2023 Jun;78:101835. doi: 10.1016/j.trim.2023.101835. Epub 2023 Apr 7.

Abstract

Inflammatory Bowel diseases (IBDs) constitute a complex panel of disorders characterized with chronic inflammation affecting the alimentary canal along with extra intestinal manifestations. Its exact etiology is still unknown; however, it seems to be the result of uncharacterized environmental insults in the intestine and their immunological consequences along with dysbiosis, in genetically predisposed individuals. It was the main target of our team since 2002 to explore the etiology of IBD and the related role of bacteria. For almost two decades, our laboratory, among others, has been involved in the reciprocal interaction between the host gastrointestinal lining and the homing microbiota. In the first decade, the attention of scientists focused on the possible role of enteropathogenic E. coli and its relationship to the mechanistic pathways involved in IBD induced in both rats and mice by chemicals like Iodoacetamide, Dextran Sodium Sulfate, Trinitrobenzene, thus linking microbial alteration to IBD pathology. A thorough characterization of the various models was the focus of research in addition to exploring how to establish an active homeostatic composition of the commensal microbiota, including its wide diversity by restoration of gut microbiota by probiotics and moving from dysbiosis to eubiosis. In the last six years and in order to effectively translate such findings into clinical practice, it was critical to explore their relationship to colorectal cancer CRC both in solid tumors and chemically induced CRC. It was also critical to explore the degree of intestinal dysbiosis and linking to IBD, CRC and diabetes. Remarkably, the active mechanistic pathways were proposed as well as the role of microbiota or bacterial metabolites involved. This review covers two decades of investigations in our laboratory and sheds light on the different aspects of the relationship between microbiota and IBD with an emphasis on dysbiosis, probiotics and the multiple mechanistic pathways involved.

摘要

炎症性肠病(IBD)是一组复杂的疾病,其特征为慢性炎症影响消化道,并伴有肠道外表现。其确切病因尚不清楚;然而,它似乎是肠道内未明环境刺激及其免疫后果以及微生物失调的结果,在遗传易感性个体中。自 2002 年以来,我们团队一直致力于探索 IBD 的病因及其相关细菌的作用。近二十年来,我们的实验室与其他实验室一起,一直在研究宿主胃肠道与归巢微生物群之间的相互作用。在第一个十年中,科学家们的注意力集中在肠致病性大肠杆菌及其与化学物质如碘乙酰胺、葡聚糖硫酸钠、三硝基苯诱导的大鼠和小鼠中 IBD 相关的机制途径的可能作用上,从而将微生物改变与 IBD 病理学联系起来。除了探索如何通过益生菌恢复共生微生物群的积极稳态组成及其广泛多样性外,还对各种模型进行了深入的特征描述,包括从微生物失调到微生物正常化。在过去的六年中,为了将这些发现有效地转化为临床实践,探索它们与结直肠癌(CRC)的关系至关重要,包括在实体瘤和化学诱导的 CRC 中。探索肠道微生物失调的程度及其与 IBD、CRC 和糖尿病的关系也至关重要。值得注意的是,还提出了积极的机制途径以及微生物群或细菌代谢物的作用。这篇综述涵盖了我们实验室近二十年来的研究,阐明了微生物群与 IBD 之间的不同关系,重点关注微生物失调、益生菌和涉及的多种机制途径。

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