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Macrophages in intestinal inflammation and resolution: a potential therapeutic target in IBD.肠道炎症和消退中的巨噬细胞:IBD 的潜在治疗靶点。
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Concise Review: Towards the Clinical Translation of Induced Pluripotent Stem Cell-Derived Blood Cells-Ready for Take-Off.简明综述:诱导多能干细胞衍生血细胞的临床转化——蓄势待发。
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IL-10 受体缺陷型极早发炎症性肠病小鼠模型中,巨噬细胞功能恢复可改善疾病病理生理。

Restored Macrophage Function Ameliorates Disease Pathophysiology in a Mouse Model for IL10 Receptor-deficient Very Early Onset Inflammatory Bowel Disease.

机构信息

Pediatric Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.

Translational Hematology of Congenital Diseases, Institute of Experimental Hematology, REBIRTH Research Center for Translational and Regenerative Medicine, Hannover Medical School, Hannover, Germany.

出版信息

J Crohns Colitis. 2021 Sep 25;15(9):1588-1595. doi: 10.1093/ecco-jcc/jjab031.

DOI:10.1093/ecco-jcc/jjab031
PMID:33596307
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8464221/
Abstract

BACKGROUND AND AIMS

Mutations in IL10 or the IL10 receptor lead to very early onset [VEO] inflammatory bowel disease [IBD], a life-threatening disease which is often unresponsive to conventional medication. Recent studies have demonstrated that defective IL-10 receptor signalling in innate immune cells is a key driver of severe intestinal inflammation in VEO-IBD. Specifically, IL10 unresponsiveness of macrophages, which govern the tight balance between pro- and anti-inflammatory responses in the intestinal system, plays a central role in the events leading to excessive inflammatory responses and the development of IBD.

METHODS AND RESULTS

We here evaluated haematopoietic stem cell gene therapy in a VEO-IBD mouse model and demonstrated that the therapeutic response closely correlates with gene correction of the IL10 signalling pathway in intestinal macrophages. This finding prompted us to evaluate the therapeutic efficacy of macrophage transplantation in the Il10rb-/- VEO-IBD mouse model. A 6-week regimen employing a combination of depletion of endogenous hyperinflammatory macrophages followed by intraperitoneal administration of wild-type [WT] macrophages significantly reduced colitis symptoms.

CONCLUSIONS

In summary, we show that the correction of the IL10 receptor defect in macrophages, either by genetic therapy or transfer of WT macrophages to the peritoneum, can ameliorate disease-related symptoms and potentially represent novel treatment approaches for VEO-IBD patients.

摘要

背景和目的

IL10 或 IL10 受体的突变导致极早发炎症性肠病(VEO-IBD),这是一种危及生命的疾病,通常对常规药物治疗无反应。最近的研究表明,先天免疫细胞中 IL-10 受体信号的缺陷是 VEO-IBD 中严重肠道炎症的关键驱动因素。具体来说,巨噬细胞对 IL10 无反应,而巨噬细胞在肠道系统中控制着促炎和抗炎反应之间的紧密平衡,在导致过度炎症反应和 IBD 发展的事件中起着核心作用。

方法和结果

我们在此评估了 VEO-IBD 小鼠模型中的造血干细胞基因治疗,并证明治疗反应与肠道巨噬细胞中 IL10 信号通路的基因校正密切相关。这一发现促使我们评估巨噬细胞移植在 Il10rb-/-VEO-IBD 小鼠模型中的治疗效果。采用内源性高炎症性巨噬细胞耗竭联合腹腔内给予野生型(WT)巨噬细胞的 6 周方案,显著减轻了结肠炎症状。

结论

总之,我们表明,通过基因治疗或向腹腔内转移 WT 巨噬细胞来纠正巨噬细胞中的 IL10 受体缺陷,可以改善与疾病相关的症状,并可能为 VEO-IBD 患者提供新的治疗方法。