炎症性肠病中微生物群的致病机制:细菌蛋白水解活性的作用

Alba Santiago Badenas, Elena F. Verdu
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摘要

炎症性肠病是一种免疫介导的疾病,包括克罗恩病和溃疡性结肠炎,引起胃肠道的慢性炎症。虽然炎症性肠病的确切病因尚不清楚,但普遍认为遗传、环境和免疫因素共同参与了其发病机制。迄今为止,所有的研究都集中在炎症性肠病发生后发生的改变上,然而,引发疾病发病的原因仍不清楚。NOD2、ATG16L1、XBP1等多个参与肠道内稳态的基因受到影响有明显的遗传基础。然而,这些遗传因素不足以导致疾病的发生,还需要其他环境因素,如肠道微生物群和免疫系统失调。炎症性肠病患者的微生物多样性较低,厚壁菌门相对丰度降低,变形菌门增加,但并非在所有研究中都有发现。除了微生物组成的变化外,在横断面研究中也观察到功能变化。最近对有炎症性肠病风险的患者进行了纵向队列研究,使我们能够询问特定的微生物群落和功能是否可能影响疾病的发病。事实上,在炎症性肠病高危人群队列(GEM队列)中进行的一项转化研究显示,在溃疡性结肠炎发病前,粪便蛋白水解活性增加,与微生物组成变化相关。这些发现可能有助于开发新的非侵入性诊断技术,以及炎症性肠病的新治疗方法。
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Mecanismos patogénicos del microbioma en la enfermedad inflamatoria intestinal: rol de la actividad proteolítica bacteriana
nflammatory bowel disease is an immune mediated condition that includes Crohn’s disease and ulcerative colitis and causes chronic inflammation of the gastrointestinal tract. Although the exact cause for inflammatory bowel disease is unknown, there is consensus that a combination of genetic, environmental, and immune factors participate in its pathogenesis. To date, all the studies have been focused on alterations that occur once IBD has developed, however, the causes triggering the onset of the disease are still unclear. There is an evident genetic basis in which multiple genes involved in intestinal homeostasis are affected, such as NOD2, ATG16L1 and XBP1. However, these genetic factors are not sufficient for disease onset and additional environmental factors such as those related to dysregulation of gut microbiota and the immune system are required. A lower microbial diversity and a decrease in the relative abundance of Firmicutes, as well as an increase in Proteobacteria, have been described in patients with inflammatory bowel disease, but are not found in all studies. In addition to variations in microbial composition, functional changes have also been observed in cross-sectional studies. Longitudinal cohorts in patients at risk for inflammatory bowel disease have recently been conducted allowing us to interrogate whether specific microbial communities and functions could be influencing the onset of the disease. Indeed, a translational study performed in a cohort of at-risk individuals for inflammatory bowel disease (GEM cohort) showed an increased fecal proteolytic activity, associated with microbial composition changes, before the onset of ulcerative colitis. These findings may help develop new non-invasive diagnostic techniques, as well as new therapeutical approaches for inflammatory bowel disease.
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