Single-cell analysis identifies conserved features of immune dysfunction in simulated microgravity and spaceflight

单细胞分析揭示了模拟微重力和太空飞行中免疫功能障碍的保守特征

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作者:Fei Wu # ,Huixun Du # ,Eliah Overbey ,JangKeun Kim ,Priya Makhijani ,Nicolas Martin ,Chad A Lerner ,Khiem Nguyen ,Jordan Baechle ,Taylor R Valentino ,Matias Fuentealba ,Juliet M Bartleson ,Heather Halaweh ,Shawn Winer ,Cem Meydan ,Francine Garrett-Bakelman ,Nazish Sayed ,Simon Melov ,Masafumi Muratani ,Akos A Gerencser ,Herbert G Kasler ,Afshin Beheshti ,Christopher E Mason ,David Furman ,Daniel A Winer

Abstract

Microgravity is associated with immunological dysfunction, though the mechanisms are poorly understood. Here, using single-cell analysis of human peripheral blood mononuclear cells (PBMCs) exposed to short term (25 hours) simulated microgravity, we characterize altered genes and pathways at basal and stimulated states with a Toll-like Receptor-7/8 agonist. We validate single-cell analysis by RNA sequencing and super-resolution microscopy, and against data from the Inspiration-4 (I4) mission, JAXA (Cell-Free Epigenome) mission, Twins study, and spleens from mice on the International Space Station. Overall, microgravity alters specific pathways for optimal immunity, including the cytoskeleton, interferon signaling, pyroptosis, temperature-shock, innate inflammation (e.g., Coronavirus pathogenesis pathway and IL-6 signaling), nuclear receptors, and sirtuin signaling. Microgravity directs monocyte inflammatory parameters, and impairs T cell and NK cell functionality. Using machine learning, we identify numerous compounds linking microgravity to immune cell transcription, and demonstrate that the flavonol, quercetin, can reverse most abnormal pathways. These results define immune cell alterations in microgravity, and provide opportunities for countermeasures to maintain normal immunity in space.

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