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适应胃肠道类器官用于生物安全三级(BSL-3)条件下的病原体感染和单细胞测序。

Adapting Gastrointestinal Organoids for Pathogen Infection and Single Cell Sequencing under Biosafety Level 3 (BSL-3) Conditions.

机构信息

Department of Infectious Diseases, Molecular Virology, Heidelberg University Hospital; Department of Molecular Genetics and Microbiology, College of Medicine, University of Florida, Gainesville;

Department of Molecular Genetics and Microbiology, College of Medicine, University of Florida, Gainesville; Department of Infectious Diseases, Virology, Heidelberg University Hospital; Research Group "Cellular Polarity and Viral Infection", German Cancer Research Center (DKFZ);

出版信息

J Vis Exp. 2021 Sep 10(175). doi: 10.3791/62857.

Abstract

Human intestinal organoids constitute the best cellular model to study pathogen infections of the gastrointestinal tract. These organoids can be derived from all sections of the GI tract (gastric, jejunum, duodenum, ileum, colon, rectum) and, upon differentiation, contain most of the cell types that are naturally found in each individual section. For example, intestinal organoids contain nutrient-absorbing enterocytes, secretory cells (Goblet, Paneth, and enteroendocrine), stem cells, as well as all lineage-specific differentiation intermediates (e.g., early or immature cell types). The greatest advantage in using gastrointestinal tract-derived organoids to study infectious diseases is the possibility of precisely identifying which cell type is targeted by the enteric pathogen and to address whether the different sections of the gastrointestinal tract and their specific cell types similarly respond to pathogen challenges. Over the past years, gastrointestinal models, as well as organoids from other tissues, have been employed to study viral tropism and the mechanisms of pathogenesis. However, utilizing all the advantages of using organoids when employing highly pathogenic viruses represents a technical challenge and requires strict biosafety considerations. Additionally, as organoids are often grown in three dimensions, the basolateral side of the cells is facing the outside of the organoid while their apical side is facing the inside (lumen) of the organoids. This organization poses a challenge for enteric pathogens as many enteric infections initiate from the apical/luminal side of the cells following ingestion. The following manuscript will provide a comprehensive protocol to prepare human intestinal organoids for infection with enteric pathogens by considering the infection side (apical vs. basolateral) to perform single-cell RNA sequencing to characterize cell-type-specific host/pathogen interactions. This method details the preparation of the organoids as well as the considerations needed to perform this work under biosafety level 3 (BSL-3) containment conditions.

摘要

人类肠道类器官是研究胃肠道病原体感染的最佳细胞模型。这些类器官可以从胃肠道的所有部位(胃、空肠、十二指肠、回肠、结肠、直肠)获得,并且在分化后,包含了每个部位自然存在的大多数细胞类型。例如,肠道类器官包含吸收营养的肠上皮细胞、分泌细胞(杯状细胞、潘氏细胞和肠内分泌细胞)、干细胞以及所有谱系特异性分化中间产物(例如早期或不成熟的细胞类型)。使用胃肠道来源的类器官研究传染病的最大优势在于可以精确确定肠道病原体靶向的细胞类型,并研究胃肠道的不同部位及其特定细胞类型是否同样对病原体的挑战产生反应。在过去的几年中,胃肠道模型以及其他组织的类器官已被用于研究病毒嗜性和发病机制。然而,在使用高度致病性病毒时充分利用类器官的所有优势代表了一个技术挑战,并且需要严格的生物安全考虑。此外,由于类器官通常在三维中生长,细胞的基底外侧面朝向类器官的外部,而其顶端面朝向类器官的内部(腔)。这种组织方式对肠道病原体构成了挑战,因为许多肠道感染是在摄入后从细胞的顶端/腔侧开始的。本手稿将提供一个全面的方案,以考虑感染部位(顶端与基底外侧)来准备人类肠道类器官用于肠道病原体感染,并通过单细胞 RNA 测序来描述细胞类型特异性的宿主/病原体相互作用,从而对肠道病原体感染人类肠道类器官进行研究。该方法详细介绍了类器官的制备以及在生物安全 3 级(BSL-3)条件下进行这项工作所需的注意事项。

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