Ileal Paneth Cell Phenotype is a Cellular Biomarker for Pouch Complications in Ulcerative Colitis.

Changqing Ma, Talin Haritunians, Anas K Gremida, Gaurav Syal, Janaki Shah, Shaohong Yang, Claudia Ramos Del Aguila de Rivers, Chad E Storer, Ling Chen, Emebet Mengesha, Angela Mujukian, Mary Hanna, Phillip Fleshner, David G Binion, Kelli L VanDussen, Thaddeus S Stappenbeck, Richard D Head, Matthew A Ciorba, Dermot P B McGovern, Ta-Chiang Liu
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Abstract

Background & aims: Biomarkers that integrate genetic and environmental factors and predict outcome in complex immune diseases such as inflammatory bowel disease (IBD; including Crohn's disease [CD] and ulcerative colitis [UC]) are needed. We showed that morphologic patterns of ileal Paneth cells (Paneth cell phenotype [PCP]; a surrogate for PC function) is one such cellular biomarker for CD. Given the shared features between CD and UC, we hypothesized that PCP is also associated with molecular/genetic features and outcome in UC. Because PC density is highest in the ileum, we further hypothesized that PCP predicts outcome in UC subjects who underwent total colectomy and ileal pouch-anal anastomosis (IPAA).

Methods: Uninflamed ileal resection margins from UC subjects with colectomy and IPAA were used for PCP and transcriptomic analyses. PCP was defined using defensin 5 immunofluorescence. Genotyping was performed using Immunochip. UC transcriptomic and genotype associations of PCP were incorporated with data from CD subjects to identify common IBD-related pathways and genes that regulate PCP.

Results: The prevalence of abnormal ileal PCP was 27%, comparable to that seen in CD. Combined analysis of UC and CD subjects showed that abnormal PCP was associated with transcriptomic pathways of secretory granule maturation and polymorphisms in innate immunity genes. Abnormal ileal PCP at the time of colectomy was also associated with pouch complications including de novo CD in the pouch and time to first episode of pouchitis.

Conclusions: Ileal PCP is biologically and clinically relevant in UC and can be used as a biomarker in IBD.

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回肠Paneth细胞表型是溃疡性结肠炎肠袋并发症的细胞生物标记物
背景和目的:炎症性肠病(IBD,包括克罗恩病[CD]和溃疡性结肠炎[UC])等复杂的免疫性疾病需要能整合遗传和环境因素并预测其预后的生物标志物。我们的研究表明,回肠帕奈斯细胞的形态模式(帕奈斯细胞表型 [PCP];帕奈斯细胞功能的代用指标)是 CD 的细胞生物标志物之一。鉴于 CD 和 UC 的共同特征,我们假设 PCP 也与 UC 的分子/遗传特征和预后相关。由于 PC 密度在回肠中最高,我们进一步假设 PCP 可预测接受全结肠切除术和回肠袋-肛门吻合术(IPAA)的 UC 受试者的预后:方法:对接受结肠切除术和IPAA的UC受试者未发炎的回肠切除边缘进行PCP和转录组分析。使用防御素 5 免疫荧光法定义 PCP。基因分型使用 Immunochip 进行。PCP的UC转录组和基因型与CD受试者的数据相结合,以确定调控PCP的常见IBD相关通路和基因:结果:回肠PCP的异常发生率为27%,与CD的发生率相当。对UC和CD受试者的综合分析表明,PCP异常与分泌颗粒成熟的转录组通路和先天性免疫基因的多态性有关。结肠切除术时的回肠PCP异常还与肠袋并发症有关,包括肠袋内的新发CD和肠袋炎首次发作的时间:结论:回肠PCP与UC的生物和临床相关,可用作IBD的生物标记物。
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