Intraintestinal Heterogeneity of Drug Target Expression in Inflammatory Bowel Disease.

IF 1.1 4区 医学 Q4 MEDICAL LABORATORY TECHNOLOGY
Katelyn Swanson, Mamoun Younes
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引用次数: 0

Abstract

Objective: There has been no significant improvement in remission rate in inflammatory bowel disease (IBD) despite several new drugs being introduced in the past two decades. Post-treatment biopsies sometimes show histologic healing in some areas of the intestine while other areas within the same intestine continue to show active inflammation. The aim of this short descriptive study was to determine whether heterogeneous treatment response in IBD may be caused by heterogeneous expression of treatment targets within the same intestine.

Methods: Six cases of Crohn's disease and five cases of ulcerative colitis in which moderate to severe active inflammation was present in at least two biopsies from the same intestine obtained during the same endoscopy procedure were entered in the study. Sections were stained for TNFα and phospho-JAK1 (p-JAK1) using immunohistochemistry. Expression of TNFα and p-JAK1 was recorded as high when the staining intensity was moderate or high, or low when there was no or week staining. The number of eosinophils per high power field was counted in the area of peak density.

Results: Different sites within the same intestine from IBD patients with moderate to severe active inflammation may express different levels of TNFα and p-JAK1. For example, in one patient with Crohn's disease with histologically moderate to severe activity in biopsies from the ileum (site 1) and cecum (site 2), there was high expression of p-JAK1 and low TNFα in the ileum biopsy with the exact opposite in the cecum biopsy (low p-JAK1 and high TNFα expression). In this example neither small molecule drug targeting JAK1 nor anti-TNFα biologic given as single agent therapy would be expected to induce histologic remission in both actively inflamed sites in this patient.

Conclusions: The heterogeneous expression of treatment targets within the same intestine may explain why some patients with IBD may not have complete remission on single drug. Studies are needed to determine whether assay for target expression in mucosal biopsies from IBD patients can help to optimize treatment selection.

炎症性肠病中药物靶点表达的肠内异质性
目的:尽管在过去二十年中推出了多种新药,但炎症性肠病(IBD)的缓解率一直没有明显改善。治疗后的活组织切片有时会显示肠道某些区域的组织学愈合,而同一肠道内的其他区域则继续显示活跃的炎症。这项简短的描述性研究旨在确定 IBD 的异质性治疗反应是否可能由同一肠道内治疗靶点的异质性表达引起:方法:6 例克罗恩病和 5 例溃疡性结肠炎患者在同一次内镜检查过程中从同一条肠道获取的至少两份活检组织中发现中度至重度活动性炎症。用免疫组化方法对切片进行 TNFα 和磷酸-JAK1(p-JAK1)染色。当染色强度为中度或高度时,TNFα和p-JAK1的表达被记录为高;当无染色或染色一周时,则被记录为低。每个高倍视野中嗜酸性粒细胞的数量按密度峰值区域计算:结果:患有中度至重度活动性炎症的 IBD 患者的同一肠道的不同部位可能会表达不同水平的 TNFα 和 p-JAK1。例如,一名克罗恩病患者的回肠(1号部位)和盲肠(2号部位)活检组织学表现为中度至重度活动,回肠活检组织学表现为p-JAK1高表达、TNFα低表达,而盲肠活检组织学表现正好相反(p-JAK1低表达、TNFα高表达)。在这个例子中,无论是靶向JAK1的小分子药物还是抗TNFα的生物制剂作为单药治疗,都无法在该患者的两个炎症活跃部位诱导组织学缓解:结论:同一肠道内治疗靶点的异质性表达可能解释了为什么一些 IBD 患者在接受单一药物治疗后可能无法完全缓解。还需要进行研究,以确定在 IBD 患者的粘膜活检组织中检测靶点表达是否有助于优化治疗选择。
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来源期刊
Annals of clinical and laboratory science
Annals of clinical and laboratory science 医学-医学实验技术
CiteScore
1.60
自引率
0.00%
发文量
112
审稿时长
6-12 weeks
期刊介绍: The Annals of Clinical & Laboratory Science welcomes manuscripts that report research in clinical science, including pathology, clinical chemistry, biotechnology, molecular biology, cytogenetics, microbiology, immunology, hematology, transfusion medicine, organ and tissue transplantation, therapeutics, toxicology, and clinical informatics.
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