胚胎衍生和单核细胞衍生肠巨噬细胞参与炎症性肠病的发病机制及其作为治疗靶点的前景

Shujun Zuo, Liping Jiang, Luying Chen, Weikang Wang, Jintao Gu, Jiajie Kuai, Xuezhi Yang, Yang Ma, Chen-chen Han, Wei Wei
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摘要

炎症性肠病(IBD)是一组以慢性、复发性、缓解性或进行性炎症为特征的肠道炎症性疾病,它导致巨噬细胞等免疫细胞、上皮细胞和微生物之间的平衡紊乱。肠巨噬细胞(IMs)是人体内最大的巨噬细胞群,IMs 功能异常是导致 IBD 的重要原因。大部分肠巨噬细胞来自血液单核细胞的补充,小部分来自胚胎,可以自我更新。在肠道炎症微环境的刺激下,单核细胞衍生的 IMs 可与肠道上皮细胞、肠道成纤维细胞和肠道菌群相互作用,导致促炎表型分化增加,抗炎表型分化减少,释放大量促炎因子,加重肠道炎症。基于这一机制,抑制 IMs 促炎因子的分泌,增强抗炎表型的分化,有助于缓解肠道炎症,促进组织修复。目前,IBD的临床治疗药物主要包括5-氨基水杨酸(5-ASA)、糖皮质激素、免疫抑制剂和TNF-α抑制剂等。治疗的总体原则是控制急性发作、缓解病情、减少复发和预防并发症。大多数影响 IMs 的经典 IBD 疗法通过多种方式发挥作用,如抑制炎症信号通路和诱导 IM2 型巨噬细胞分化。本综述探讨了目前对IMs参与IBD发病机制的认识及其作为治疗靶点的前景。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Involvement of Embryo-Derived and Monocyte-Derived Intestinal Macrophages in the Pathogenesis of Inflammatory Bowel Disease and Their Prospects as Therapeutic Targets
Inflammatory bowel disease (IBD) is a group of intestinal inflammatory diseases characterized by chronic, recurrent, remitting, or progressive inflammation, which causes the disturbance of the homeostasis between immune cells, such as macrophages, epithelial cells, and microorganisms. Intestinal macrophages (IMs) are the largest population of macrophages in the body, and the abnormal function of IMs is an important cause of IBD. Most IMs come from the replenishment of blood monocytes, while a small part come from embryos and can self-renew. Stimulated by the intestinal inflammatory microenvironment, monocyte-derived IMs can interact with intestinal epithelial cells, intestinal fibroblasts, and intestinal flora, resulting in the increased differentiation of proinflammatory phenotypes and the decreased differentiation of anti-inflammatory phenotypes, releasing a large number of proinflammatory factors and aggravating intestinal inflammation. Based on this mechanism, inhibiting the secretion of IMs’ proinflammatory factors and enhancing the differentiation of anti-inflammatory phenotypes can help alleviate intestinal inflammation and promote tissue repair. At present, the clinical medication of IBD mainly includes 5-aminosalicylic acids (5-ASAs), glucocorticoid, immunosuppressants, and TNF-α inhibitors. The general principle of treatment is to control acute attacks, alleviate the condition, reduce recurrence, and prevent complications. Most classical IBD therapies affecting IMs function in a variety of ways, such as inhibiting the inflammatory signaling pathways and inducing IM2-type macrophage differentiation. This review explores the current understanding of the involvement of IMs in the pathogenesis of IBD and their prospects as therapeutic targets.
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