Nucleic acid biomarkers of immune response and cell and tissue damage in children with COVID-19 and MIS-C

COVID-19 和 MIS-C 儿童免疫反应及细胞和组织损伤的核酸生物标志物

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作者:Conor J Loy ,Alicia Sotomayor-Gonzalez ,Venice Servellita ,Jenny Nguyen ,Joan Lenz ,Sanchita Bhattacharya ,Meagan E Williams ,Alexandre P Cheng ,Andrew Bliss ,Prachi Saldhi ,Noah Brazer ,Jessica Streithorst ,William Suslovic ,Charlotte J Hsieh ,Burak Bahar ,Nathan Wood ,Abiodun Foresythe ,Amelia Gliwa ,Kushmita Bhakta ,Maria A Perez ,Laila Hussaini ,Evan J Anderson ,Ann Chahroudi ,Meghan Delaney ,Atul J Butte ,Roberta L DeBiasi ,Christina A Rostad ,Iwijn De Vlaminck ,Charles Y Chiu

Abstract

Differential host responses in coronavirus disease 2019 (COVID-19) and multisystem inflammatory syndrome in children (MIS-C) remain poorly characterized. Here, we use next-generation sequencing to longitudinally analyze blood samples from pediatric patients with COVID-19 or MIS-C across three hospitals. Profiling of plasma cell-free nucleic acids uncovers distinct signatures of cell injury and death between COVID-19 and MIS-C, with increased multiorgan involvement in MIS-C encompassing diverse cell types, including endothelial and neuronal cells, and an enrichment of pyroptosis-related genes. Whole-blood RNA profiling reveals upregulation of similar pro-inflammatory pathways in COVID-19 and MIS-C but also MIS-C-specific downregulation of T cell-associated pathways. Profiling of plasma cell-free RNA and whole-blood RNA in paired samples yields different but complementary signatures for each disease state. Our work provides a systems-level view of immune responses and tissue damage in COVID-19 and MIS-C and informs future development of new disease biomarkers. Keywords: DNA damage; RNA sequencing; RNA-seq; SARS-CoV-2; bisulfite sequencing; cell damage; cell-free DNA; cell-free RNA; clinical severity; coronavirus disease 2019; disease biomarkers; host response; immune response; multisystem inflammatory syndrome in children; nucleic acid sequencing; pediatric; signaling pathways; systems biology; tissue damage; whole-blood RNA.

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