SCENITH检测低温保存对免疫细胞代谢的影响。

Oxford open immunology Pub Date : 2024-12-20 eCollection Date: 2025-01-01 DOI:10.1093/oxfimm/iqae015
Curtis Luscombe, Eben Jones, Michaela Gregorova, Nicholas Jones, Laura Rivino
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引用次数: 0

摘要

免疫细胞的动态功能是由细胞代谢过程调节的,对功能失调免疫反应的免疫代谢相关因素的研究日益引起人们的兴趣。SCENITH是一种新颖的基于流式细胞术的技术,可以在异质样品中对免疫细胞进行体外代谢分析。临床样品的低温保存通常是为了促进免疫反应的高通量处理和纵向分析,但被认为会导致细胞代谢功能障碍。我们的目的是研究低温保存对免疫细胞代谢的影响,利用SCENITH的独特能力来描述不同免疫细胞亚群的不同生物能量特征。我们证明激活后,T细胞不能充分/容易地进行代谢重编程。此外,我们发现低温保存引入了一个时间依赖性的代谢伪影,有利于糖酵解并损害氧化磷酸化,这表明低温保存导致线粒体功能障碍。尽管存在这种人工制品,SCENITH仍然能够揭示冷冻保存后对比免疫细胞群体的独特生物能量谱。虽然SCENITH可以提供有关免疫细胞代谢的宝贵信息,即使在冷冻保存的样本中,我们的发现对未来研究的设计具有重要意义。研究者应该仔细考虑如何处理和储存临床样本,以确保低温保存不会混淆分析,特别是在需要纵向取样的情况下。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Impact of cryopreservation on immune cell metabolism as measured by SCENITH.

The dynamic functioning of immune cells is regulated by cellular metabolic processes, and there is growing interest in the study of immunometabolic correlates of dysfunctional immune responses. SCENITH is a novel flow cytometry-based technique that allows for ex vivo metabolic profiling of immune cells within heterogeneous samples. Cryopreservation of clinical samples is frequently undertaken to facilitate high throughput processing and longitudinal analyses of immune responses, but is thought to lead to cellular metabolic dysfunction. We aimed to investigate the impact of cryopreservation on immune cell metabolism, harnessing SCENITH's unique ability to describe the divergent bioenergetic characteristics of distinct immune cell subsets. We demonstrate that upon activation, T cells are unable to sufficiently/readily undergo metabolic reprogramming. Additionally, we find that cryopreservation introduces a time-dependent metabolic artefact that favours glycolysis and impairs oxidative phosphorylation, suggesting that cryopreservation results in mitochondrial dysfunction. Despite this artefact, SCENITH was still able to reveal the distinct bioenergetic profiles of contrasting immune cells populations following cryopreservation. Whilst SCENITH can provide valuable information about immune cell metabolism even in cryopreserved samples, our findings have important implications for the design of future studies. Investigators should carefully consider how to process and store clinical samples to ensure that cryopreservation does not confound analyses, particularly where longitudinal sampling is required.

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