Single-cell transcriptomic analysis reveals a systemic immune dysregulation in COVID-19-associated pediatric encephalopathy.

Wang, Y; Luu, LDW; Liu, S; Zhu, X; Huang, S; Li, F; Huang, X; Guo, L; Zhang, J; Ge, H; Sun, Y; Hui, Y; Qu, Y; Wang, H; Wang, X; Na, W; Zhou, J; Qu, D; Tai, J

Single-cell transcriptomic analysis reveals a systemic immune dysregulation in COVID-19-associated pediatric encephalopathy.

Wang, Y Luu, LDW Liu, S Zhu, X Huang, S Li, F Huang, X Guo, L Zhang, J Ge, H Sun, Y Hui, Y Qu, Y Wang, H Wang, X Na, W Zhou, J Qu, D Tai, J

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Publisher:: SPRINGERNATURE
Publication Type:: Journal Article
Citation:: Signal Transduct Target Ther, 2023, 8, (1), pp. 398
Issue Date:: 2023-10-18

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Field	Value	Language
dc.contributor.author	Wang, Y
dc.contributor.author	Luu, LDW
dc.contributor.author	Liu, S
dc.contributor.author	Zhu, X
dc.contributor.author	Huang, S
dc.contributor.author	Li, F
dc.contributor.author	Huang, X
dc.contributor.author	Guo, L
dc.contributor.author	Zhang, J
dc.contributor.author	Ge, H
dc.contributor.author	Sun, Y
dc.contributor.author	Hui, Y
dc.contributor.author	Qu, Y
dc.contributor.author	Wang, H
dc.contributor.author	Wang, X
dc.contributor.author	Na, W
dc.contributor.author	Zhou, J
dc.contributor.author	Qu, D
dc.contributor.author	Tai, J
dc.date.accessioned	2024-01-08T06:22:05Z
dc.date.available	2023-09-01
dc.date.available	2024-01-08T06:22:05Z
dc.date.issued	2023-10-18
dc.identifier.citation	Signal Transduct Target Ther, 2023, 8, (1), pp. 398
dc.identifier.issn	2095-9907
dc.identifier.issn	2059-3635
dc.identifier.uri	http://hdl.handle.net/10453/174101
dc.description.abstract	Unraveling the molecular mechanisms for COVID-19-associated encephalopathy and its immunopathology is crucial for developing effective treatments. Here, we utilized single-cell transcriptomic analysis and integrated clinical observations and laboratory examination to dissect the host immune responses and reveal pathological mechanisms in COVID-19-associated pediatric encephalopathy. We found that lymphopenia was a prominent characteristic of immune perturbation in COVID-19 patients with encephalopathy, especially those with acute necrotizing encephalopathy (AE). This was characterized a marked reduction of various lymphocytes (e.g., CD8+ T and CD4+ T cells) and significant increases in other inflammatory cells (e.g., monocytes). Further analysis revealed activation of multiple cell apoptosis pathways (e.g., granzyme/perforin-, FAS- and TNF-induced apoptosis) may be responsible for lymphopenia. A systemic S100A12 upregulation, primarily from classical monocytes, may have contributed to cytokine storms in patients with AE. A dysregulated type I interferon (IFN) response was observed which may have further exacerbated the S100A12-driven inflammation in patients with AE. In COVID-19 patients with AE, myeloid cells (e.g., monocytic myeloid-derived suppressor cells) were the likely contributors to immune paralysis. Finally, the immune landscape in COVID-19 patients with encephalopathy, especially for AE, were also characterized by NK and T cells with widespread exhaustion, higher cytotoxic scores and inflammatory response as well as a dysregulated B cell-mediated humoral immune response. Taken together, this comprehensive data provides a detailed resource for elucidating immunopathogenesis and will aid development of effective COVID-19-associated pediatric encephalopathy treatments, especially for those with AE.
dc.format	Electronic
dc.language	eng
dc.publisher	SPRINGERNATURE
dc.relation.ispartof	Signal Transduct Target Ther
dc.relation.isbasedon	10.1038/s41392-023-01641-y
dc.rights	info:eu-repo/semantics/openAccess
dc.subject.classification	3101 Biochemistry and cell biology
dc.subject.mesh	Humans
dc.subject.mesh	Child
dc.subject.mesh	CD8-Positive T-Lymphocytes
dc.subject.mesh	COVID-19
dc.subject.mesh	S100A12 Protein
dc.subject.mesh	Transcriptome
dc.subject.mesh	CD4-Positive T-Lymphocytes
dc.subject.mesh	Lymphopenia
dc.subject.mesh	CD4-Positive T-Lymphocytes
dc.subject.mesh	CD8-Positive T-Lymphocytes
dc.subject.mesh	Humans
dc.subject.mesh	Lymphopenia
dc.subject.mesh	Child
dc.subject.mesh	Transcriptome
dc.subject.mesh	S100A12 Protein
dc.subject.mesh	COVID-19
dc.title	Single-cell transcriptomic analysis reveals a systemic immune dysregulation in COVID-19-associated pediatric encephalopathy.
dc.type	Journal Article
utslib.citation.volume	8
utslib.location.activity	England
pubs.organisational-group	/University of Technology Sydney
pubs.organisational-group	/University of Technology Sydney/Faculty of Science
pubs.organisational-group	/University of Technology Sydney/Faculty of Science/School of Life Sciences
utslib.copyright.status	open_access	*
dc.date.updated	2024-01-08T06:21:49Z
pubs.issue	1
pubs.publication-status	Published online
pubs.volume	8
utslib.citation.issue	1

Abstract:

Unraveling the molecular mechanisms for COVID-19-associated encephalopathy and its immunopathology is crucial for developing effective treatments. Here, we utilized single-cell transcriptomic analysis and integrated clinical observations and laboratory examination to dissect the host immune responses and reveal pathological mechanisms in COVID-19-associated pediatric encephalopathy. We found that lymphopenia was a prominent characteristic of immune perturbation in COVID-19 patients with encephalopathy, especially those with acute necrotizing encephalopathy (AE). This was characterized a marked reduction of various lymphocytes (e.g., CD8+ T and CD4+ T cells) and significant increases in other inflammatory cells (e.g., monocytes). Further analysis revealed activation of multiple cell apoptosis pathways (e.g., granzyme/perforin-, FAS- and TNF-induced apoptosis) may be responsible for lymphopenia. A systemic S100A12 upregulation, primarily from classical monocytes, may have contributed to cytokine storms in patients with AE. A dysregulated type I interferon (IFN) response was observed which may have further exacerbated the S100A12-driven inflammation in patients with AE. In COVID-19 patients with AE, myeloid cells (e.g., monocytic myeloid-derived suppressor cells) were the likely contributors to immune paralysis. Finally, the immune landscape in COVID-19 patients with encephalopathy, especially for AE, were also characterized by NK and T cells with widespread exhaustion, higher cytotoxic scores and inflammatory response as well as a dysregulated B cell-mediated humoral immune response. Taken together, this comprehensive data provides a detailed resource for elucidating immunopathogenesis and will aid development of effective COVID-19-associated pediatric encephalopathy treatments, especially for those with AE.

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http://hdl.handle.net/10453/174101