原发性硬化性胆管炎患者的炎症性肠病:一种不同形式的结肠炎

Amber Bangma, Paola Pibiri, Sofie de Jong, Emilia V. Bigaeva, Gwenny M.P.J. Verstappen, Gursah Kats-Urgulu, Marcela A. Hermoso, Monique G.P. van der Wijst, Johannes R. Bjork, Shiqiang Sun, Naomi Karmi, Frans G.M. Kroese, Arnau Vich Vila, Klaas Nico Faber, Rinse K. Weersma, Werna T.C. Uniken Venema, Eleonora A.M. Festen
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摘要

背景和目的原发性硬化性胆管炎(PSC)是一种胆管炎症性疾病,通常伴有炎症性肠病(PSC-IBD)。据观察,PSC-IBD 和溃疡性结肠炎(UC)在临床表现上存在很大差异。本研究旨在利用单细胞 mRNA 测序找出 PSC-IBD 的不同病理机制。方法收集并分离 47 例 PSC-IBD(n=24)、UC(n=18)(尽可能匹配炎症(I)非炎症(NI))和非 IBD 受试者(n=5)的结肠粘膜活检组织。文库制备和测序处理后进行差异丰度、差异表达和细胞-细胞相互作用分析。对组织切片进行了 DUOX2 和 HLA-DR 染色。结果总共发现了 71798 个细胞,包括 54 种不同的细胞类型,其中包括一种新的细胞类型:DUOX2+ 肠细胞,主要存在于发炎的结肠中,是抗原呈递细胞(HLA-DR+)。干细胞在 PSC-NI 中的丰度有所增加,而在 UC-NI 中则没有。此外,我们还发现了 PSC 和 UC 中与炎症有关的不同基因表达谱:PSC 炎症主要激活炎性单核细胞,而 UC 炎症则激活炎性成纤维细胞。结论我们的研究发现了一种新的细胞类型--DUOX2+肠细胞,这种细胞主要存在于炎症环境中,根据其表达谱,可能具有抗原呈递功能。此外,我们还强调,PSC-IBD(而非 UC)的特征是炎性 HLA-DRB1+ 单核细胞的活化,而这些单核细胞很可能参与了 CD4+ T 细胞的活化。值得注意的是,我们观察到非炎症性PSC-IBD中干细胞数量增加,这可能与PSC-IBD结直肠癌风险升高有关。
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Inflammatory Bowel Disease in patients with Primary Sclerosing Cholangitis: a distinct form of colitis
Background and aims Primary sclerosing cholangitis (PSC) is an inflammatory disorder of the bile ducts, often accompanied by inflammatory bowel disease (PSC-IBD). Substantial differences in clinical presentation are observed between PSC-IBD and ulcerative colitis (UC). In this study we aim to find distinct pathomechanisms for PSC-IBD using single-cell mRNA sequencing. Methods Forty-seven colonic mucosal biopsies of PSC-IBD (n=24), UC (n=18) (where possible matched inflamed (I) non-inflamed (NI)), and non-IBD subjects (n=5) were collected and dissociated. Library preparation and processing for sequencing was followed by differential abundance, differential expression, and cell-cell-interaction analyses. Stainings for DUOX2 and HLA-DR were applied on tissue sections. Results In total, 71,798 cells comprised 54 distinct cell types, including a new cell type: the DUOX2+ enterocyte, mainly present in inflamed colon and acting as antigen presenting cells (HLA-DR+). Stem cells exhibited increased abundances in PSC-NI but not in UC-NI. Additionally, we found distinct gene expression profiles in PSC and UC which were related to inflammation: while mainly inflammatory monocytes were activated in PSC inflammation, and inflammatory fibroblasts were activated in UC inflammation. Conclusion Our study found a new cell type, the DUOX2+ enterocyte that is primarily present in inflamed conditions, and based on their expression profile, potentially perform antigen presentation. Moreover, we highlight that PSC-IBD, but not UC, is characterized by the activation of inflammatory HLA-DRB1+ monocytes, which are likely involved in the activation of CD4+ T cells. Notably, we observed an increased abundance of stem cells in non-inflamed PSC-IBD, possibly linked to the elevated risk of colorectal cancer in PSC-IBD.
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