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人体结肠功能的离体研究:对氧的依赖性和对抗生素的敏感性。

Human colon function ex vivo: Dependence on oxygen and sensitivity to antibiotic.

机构信息

Department of Biomedical Sciences, Colorado State University, Fort Collins, Colorado, United States of America.

Department of Environmental & Radiological Health Sciences, Colorado State University, Fort Collins, Colorado, United States of America.

出版信息

PLoS One. 2019 May 16;14(5):e0217170. doi: 10.1371/journal.pone.0217170. eCollection 2019.

Abstract

BACKGROUND

Human intestines contain a heterogeneous collection of cells that include immune, neural and epithelial elements interacting in a highly complex physiology that is challenging to maintain ex vivo. There is an extreme oxygen gradient across the intestinal wall due in part to microbiota in the lumen and close to the gut wall, which complicates the design of tissue culture systems. The current study established the use of an organotypic slice model of human intestinal tissue derived from colonoscopy biopsies to study host-microbial interactions after antibiotic treatment, and the influence of oxygen concentration on gut wall function.

METHODS

Organotypic slices from human colon biopsies collected during routine colonoscopy provided three-dimensional environments that maintained cellular morphology ex vivo. Biopsy slices were used to study impacts of oxygen concentrations and antibiotic treatments on epithelial proliferation rates, and metabolites from tissue culture supernatants.

RESULTS

Immune function was validated via demonstration of a T lymphocyte response to Salmonella enterica serovar Typhimurium. Following 24 h of Salmonella exposure there was a significant increase in CD3+ T-lymphocytes in biopsy slices. Metabolite profiling of tissue culture supernatants validated the influence of antibiotic treatment under varied oxygen culture conditions on both host and microbiome-mediated metabolism. Epithelial health was influenced by oxygen and antibiotic. Increased epithelial proliferation was measured in lowered oxygen conditions (1% = 5.9 mmHg) compared to atmospheric conditions standard at 5000 feet above sea level in Colorado (~17% = 100 mmHg). Antibiotic treatment reduced epithelial proliferation only in 5.9 mmHg oxygen cultured slices.

CONCLUSIONS

A human colon organotypic slice model was established for applications ranging from gut epithelial proliferation to enteric pathogen influence on mucosal immune functions ex vivo. The results further support the need to account for oxygen concentration in primary tissue cultures, and that antibiotic use impacts gut-microbe-immune interactions.

摘要

背景

人类肠道中包含多种细胞,包括免疫、神经和上皮细胞,它们在高度复杂的生理学环境中相互作用,这种环境很难在体外维持。由于腔隙和靠近肠道壁的微生物群,肠道壁存在极端的氧气梯度,这使得组织培养系统的设计变得复杂。本研究建立了使用源自结肠镜活检的人肠道组织器官型切片模型来研究抗生素治疗后宿主-微生物相互作用以及氧浓度对肠道壁功能的影响。

方法

从常规结肠镜检查活检中获取的人结肠切片提供了三维环境,使细胞形态在体外得以维持。使用活检切片来研究氧浓度和抗生素处理对上皮细胞增殖率以及组织培养上清代谢物的影响。

结果

通过证明对肠炎沙门氏菌血清型 Typhimurium 的 T 淋巴细胞反应,验证了免疫功能。在沙门氏菌暴露 24 小时后,活检切片中的 CD3+T 淋巴细胞明显增加。在不同氧培养条件下,抗生素处理对宿主和微生物群介导的代谢物的代谢产物谱分析验证了其影响。上皮健康受到氧和抗生素的影响。与科罗拉多州海拔 5000 英尺(约 17%=100mmHg)的标准大气条件相比,在低氧条件(1%=5.9mmHg)下测量到的上皮增殖增加。仅在 5.9mmHg 氧培养切片中,抗生素处理会降低上皮细胞增殖。

结论

建立了人结肠器官型切片模型,可用于从肠道上皮细胞增殖到肠病原体对粘膜免疫功能的影响等各种应用。结果进一步支持了在原代组织培养中需要考虑氧浓度的需求,并且抗生素的使用会影响肠道-微生物-免疫相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7d06/6522050/a66551443d90/pone.0217170.g001.jpg

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