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增强人空肠类器官对宿主和微生物刺激的反应性。

Enhancing responsiveness of human jejunal enteroids to host and microbial stimuli.

机构信息

Department of Pediatrics, Baylor College of Medicine, Houston, Texas, USA.

Section of Gastroenterology, Hepatology, and Nutrition, Texas Children's Hospital, Houston, Texas, USA.

出版信息

J Physiol. 2020 Aug;598(15):3085-3105. doi: 10.1113/JP279423. Epub 2020 Jun 13.

Abstract

KEY POINTS

Enteroids are a physiologically relevant model to examine the human intestine and its functions. Previously, the measurable cytokine response of human intestinal enteroids has been limited following exposure to host or microbial pro-inflammatory stimuli. Modifications to enteroid culture conditions facilitated robust human cytokine responses to pro-inflammatory stimuli. This new human enteroid culture methodology refines the ability to study microbiome:human intestinal epithelium interactions in the laboratory.

ABSTRACT

The intestinal epithelium is the primary interface between the host, the gut microbiome and its external environment. Since the intestinal epithelium contributes to innate immunity as a first line of defence, understanding how the epithelium responds to microbial and host stimuli is an important consideration in promoting homeostasis. Human intestinal enteroids (HIEs) are primary epithelial cell cultures that can provide insights into the biology of the intestinal epithelium and innate immune responses. One potential limitation of using HIEs for innate immune studies is the relative lack of responsiveness to factors that stimulate epithelial cytokine production. We report technical refinements, including removal of extracellular antioxidants, to facilitate enhanced cytokine responses in HIEs. Using this new method, we demonstrate that HIEs have distinct cytokine profiles in response to pro-inflammatory stimuli derived from host and microbial sources. Overall, we found that host-derived cytokines tumour necrosis factor and interleukin-1α stimulated reactive oxygen species and a large repertoire of cytokines. In contrast, microbial lipopolysaccharide, lipoteichoic acid and flagellin stimulated a limited number of cytokines and histamine did not stimulate the release of any cytokines. Importantly, HIE-secreted cytokines were functionally active, as denoted by the ability of human blood-derived neutrophil to migrate towards HIE supernatant containing interleukin-8. These findings establish that the immune responsiveness of HIEs depends on medium composition and stimuli. By refining the experimental culture medium and creating an environment conducive to epithelial cytokine responses by human enteroids, HIEs can facilitate exploration of many experimental questions pertaining to the role of the intestinal epithelium in innate immunity.

摘要

要点

类器官是研究人类肠道及其功能的一种与生理相关的模型。以前,人类肠道类器官在暴露于宿主或微生物促炎刺激物后,其可测量的细胞因子反应受到限制。对类器官培养条件的修改促进了对促炎刺激物的强烈人类细胞因子反应。这种新的人类类器官培养方法改进了在实验室中研究微生物组与人类肠道上皮相互作用的能力。

摘要

肠道上皮是宿主、肠道微生物群及其外部环境之间的主要界面。由于肠道上皮作为第一道防线有助于先天免疫,因此了解上皮对微生物和宿主刺激物的反应对于促进内稳态是一个重要的考虑因素。人类肠道类器官(HIEs)是主要的上皮细胞培养物,可以深入了解肠道上皮和先天免疫反应的生物学。使用 HIEs 进行先天免疫研究的一个潜在限制是相对缺乏对刺激上皮细胞因子产生的因素的反应。我们报告了技术改进,包括去除细胞外抗氧化剂,以促进 HIE 中细胞因子反应的增强。使用这种新方法,我们证明 HIEs 对来自宿主和微生物源的促炎刺激物有独特的细胞因子谱。总的来说,我们发现宿主来源的细胞因子肿瘤坏死因子和白细胞介素-1α刺激活性氧和大量细胞因子的产生。相比之下,微生物脂多糖、脂磷壁酸和鞭毛蛋白刺激有限数量的细胞因子,组胺则不能刺激任何细胞因子的释放。重要的是,HIE 分泌的细胞因子具有功能活性,这表现为人类血液衍生的中性粒细胞向含有白细胞介素-8 的 HIE 上清液迁移的能力。这些发现表明 HIE 的免疫反应性取决于培养基组成和刺激物。通过改进实验培养基并创造有利于人类类器官上皮细胞因子反应的环境,HIE 可以促进探索许多与肠道上皮在先天免疫中的作用有关的实验问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8ec6/7674265/3ee2a6be8df7/nihms-1603855-f0001.jpg

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