Elevated IFNA1 and suppressed IL12p40 associated with persistent hyperinflammation in COVID-19 pneumonia

Kyeongseok Jeon; Yuri Kim; Shin Kwang Kang; Uni Park; Jayoun Kim; Nanhee Park; Jaemoon Koh; Man Shik Shim; Minsoo Kim; Youn Ju Rhee; Hyeongseok Jeong; Siyoung Lee; Donghyun Park; Jinyoung Lim; Hyunsu Kim; Na Young Ha; Hye Yeong Jo; Sang Cheol Kim; Ju Hee Lee; Jiwon Shon; Hoon Kim; Yoon Kyung Jeon; Youn Soo Choi; Hye Young Kim; Won Woo Lee; Murim Choi; Hyun Young Park; Woong Yang Park; Yeon Sook Kim; Nam Hyuk Cho

doi:10.3389/fimmu.2023.1101808

Elevated IFNA1 and suppressed IL12p40 associated with persistent hyperinflammation in COVID-19 pneumonia

Kyeongseok Jeon
, Yuri Kim
, Shin Kwang Kang
, Uni Park
, Jayoun Kim
, Nanhee Park
, Jaemoon Koh
, Man Shik Shim
, Minsoo Kim
, Youn Ju Rhee
, Hyeongseok Jeong
, Siyoung Lee
, Donghyun Park
, Jinyoung Lim
, Hyunsu Kim
, Na Young Ha
, Hye Yeong Jo
, Sang Cheol Kim
, Ju Hee Lee
, Jiwon Shon

Hoon Kim, Yoon Kyung Jeon, Youn Soo Choi, Hye Young Kim, Won Woo Lee, Murim Choi, Hyun Young Park, Woong Yang Park, Yeon Sook Kim, Nam Hyuk Cho

Research output: Contribution to journal › Article › peer-review

4 Scopus citations

Abstract

Introduction: Despite of massive endeavors to characterize inflammation in COVID-19 patients, the core network of inflammatory mediators responsible for severe pneumonia stillremain remains elusive. Methods: Here, we performed quantitative and kinetic analysis of 191 inflammatory factors in 955 plasma samples from 80 normal controls (sample n = 80) and 347 confirmed COVID-19 pneumonia patients (sample n = 875), including 8 deceased patients. Results: Differential expression analysis showed that 76% of plasmaproteins (145 factors) were upregulated in severe COVID-19 patients comparedwith moderate patients, confirming overt inflammatory responses in severe COVID-19 pneumonia patients. Global correlation analysis of the plasma factorsrevealed two core inflammatory modules, core I and II, comprising mainly myeloid cell and lymphoid cell compartments, respectively, with enhanced impact in a severity-dependent manner. We observed elevated IFNA1 and suppressed IL12p40, presenting a robust inverse correlation in severe patients, which was strongly associated with persistent hyperinflammation in 8.3% of moderate pneumonia patients and 59.4% of severe patients. Discussion: Aberrant persistence of pulmonary and systemic inflammation might be associated with long COVID-19 sequelae. Our comprehensive analysis of inflammatory mediators in plasmarevealed the complexity of pneumonic inflammation in COVID-19 patients anddefined critical modules responsible for severe pneumonic progression.

Original language	English
Article number	1101808
Journal	Frontiers in Immunology
Volume	14
DOIs	https://doi.org/10.3389/fimmu.2023.1101808
State	Published - 27 Jan 2023

Keywords

COVID-19
IFNa
IL-12p40
inflammation
pneumonia
SARS-CoV-2

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3389/fimmu.2023.1101808

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Jeon, K., Kim, Y., Kang, S. K., Park, U., Kim, J., Park, N., Koh, J., Shim, M. S., Kim, M., Rhee, Y. J., Jeong, H., Lee, S., Park, D., Lim, J., Kim, H., Ha, N. Y., Jo, H. Y., Kim, S. C., Lee, J. H., ... Cho, N. H. (2023). Elevated IFNA1 and suppressed IL12p40 associated with persistent hyperinflammation in COVID-19 pneumonia. Frontiers in Immunology, 14, Article 1101808. https://doi.org/10.3389/fimmu.2023.1101808

@article{a76e9a5a4eed47de9411720cdcf94002,

title = "Elevated IFNA1 and suppressed IL12p40 associated with persistent hyperinflammation in COVID-19 pneumonia",

abstract = "Introduction: Despite of massive endeavors to characterize inflammation in COVID-19 patients, the core network of inflammatory mediators responsible for severe pneumonia stillremain remains elusive. Methods: Here, we performed quantitative and kinetic analysis of 191 inflammatory factors in 955 plasma samples from 80 normal controls (sample n = 80) and 347 confirmed COVID-19 pneumonia patients (sample n = 875), including 8 deceased patients. Results: Differential expression analysis showed that 76\% of plasmaproteins (145 factors) were upregulated in severe COVID-19 patients comparedwith moderate patients, confirming overt inflammatory responses in severe COVID-19 pneumonia patients. Global correlation analysis of the plasma factorsrevealed two core inflammatory modules, core I and II, comprising mainly myeloid cell and lymphoid cell compartments, respectively, with enhanced impact in a severity-dependent manner. We observed elevated IFNA1 and suppressed IL12p40, presenting a robust inverse correlation in severe patients, which was strongly associated with persistent hyperinflammation in 8.3\% of moderate pneumonia patients and 59.4\% of severe patients. Discussion: Aberrant persistence of pulmonary and systemic inflammation might be associated with long COVID-19 sequelae. Our comprehensive analysis of inflammatory mediators in plasmarevealed the complexity of pneumonic inflammation in COVID-19 patients anddefined critical modules responsible for severe pneumonic progression.",

keywords = "COVID-19, IFNa, IL-12p40, inflammation, pneumonia, SARS-CoV-2",

author = "Kyeongseok Jeon and Yuri Kim and Kang, \{Shin Kwang\} and Uni Park and Jayoun Kim and Nanhee Park and Jaemoon Koh and Shim, \{Man Shik\} and Minsoo Kim and Rhee, \{Youn Ju\} and Hyeongseok Jeong and Siyoung Lee and Donghyun Park and Jinyoung Lim and Hyunsu Kim and Ha, \{Na Young\} and Jo, \{Hye Yeong\} and Kim, \{Sang Cheol\} and Lee, \{Ju Hee\} and Jiwon Shon and Hoon Kim and Jeon, \{Yoon Kyung\} and Choi, \{Youn Soo\} and Kim, \{Hye Young\} and Lee, \{Won Woo\} and Murim Choi and Park, \{Hyun Young\} and Park, \{Woong Yang\} and Kim, \{Yeon Sook\} and Cho, \{Nam Hyuk\}",

note = "Publisher Copyright: Copyright {\textcopyright} 2023 Jeon, Kim, Kang, Park, Kim, Park, Koh, Shim, Kim, Rhee, Jeong, Lee, Park, Lim, Kim, Ha, Jo, Kim, Lee, Shon, Kim, Jeon, Choi, Kim, Lee, Choi, Park, Park, Kim and Cho.",

year = "2023",

month = jan,

day = "27",

doi = "10.3389/fimmu.2023.1101808",

language = "English",

volume = "14",

journal = "Frontiers in Immunology",

issn = "1664-3224",

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Jeon, K, Kim, Y, Kang, SK, Park, U, Kim, J, Park, N, Koh, J, Shim, MS, Kim, M, Rhee, YJ, Jeong, H, Lee, S, Park, D, Lim, J, Kim, H, Ha, NY, Jo, HY, Kim, SC, Lee, JH, Shon, J, Kim, H, Jeon, YK, Choi, YS, Kim, HY, Lee, WW, Choi, M, Park, HY, Park, WY, Kim, YS & Cho, NH 2023, 'Elevated IFNA1 and suppressed IL12p40 associated with persistent hyperinflammation in COVID-19 pneumonia', Frontiers in Immunology, vol. 14, 1101808. https://doi.org/10.3389/fimmu.2023.1101808

TY - JOUR

T1 - Elevated IFNA1 and suppressed IL12p40 associated with persistent hyperinflammation in COVID-19 pneumonia

AU - Jeon, Kyeongseok

AU - Kim, Yuri

AU - Kang, Shin Kwang

AU - Park, Uni

AU - Kim, Jayoun

AU - Park, Nanhee

AU - Koh, Jaemoon

AU - Shim, Man Shik

AU - Kim, Minsoo

AU - Rhee, Youn Ju

AU - Jeong, Hyeongseok

AU - Lee, Siyoung

AU - Park, Donghyun

AU - Lim, Jinyoung

AU - Kim, Hyunsu

AU - Ha, Na Young

AU - Jo, Hye Yeong

AU - Kim, Sang Cheol

AU - Lee, Ju Hee

AU - Shon, Jiwon

AU - Kim, Hoon

AU - Jeon, Yoon Kyung

AU - Choi, Youn Soo

AU - Kim, Hye Young

AU - Lee, Won Woo

AU - Choi, Murim

AU - Park, Hyun Young

AU - Park, Woong Yang

AU - Kim, Yeon Sook

AU - Cho, Nam Hyuk

N1 - Publisher Copyright: Copyright © 2023 Jeon, Kim, Kang, Park, Kim, Park, Koh, Shim, Kim, Rhee, Jeong, Lee, Park, Lim, Kim, Ha, Jo, Kim, Lee, Shon, Kim, Jeon, Choi, Kim, Lee, Choi, Park, Park, Kim and Cho.

PY - 2023/1/27

Y1 - 2023/1/27

N2 - Introduction: Despite of massive endeavors to characterize inflammation in COVID-19 patients, the core network of inflammatory mediators responsible for severe pneumonia stillremain remains elusive. Methods: Here, we performed quantitative and kinetic analysis of 191 inflammatory factors in 955 plasma samples from 80 normal controls (sample n = 80) and 347 confirmed COVID-19 pneumonia patients (sample n = 875), including 8 deceased patients. Results: Differential expression analysis showed that 76% of plasmaproteins (145 factors) were upregulated in severe COVID-19 patients comparedwith moderate patients, confirming overt inflammatory responses in severe COVID-19 pneumonia patients. Global correlation analysis of the plasma factorsrevealed two core inflammatory modules, core I and II, comprising mainly myeloid cell and lymphoid cell compartments, respectively, with enhanced impact in a severity-dependent manner. We observed elevated IFNA1 and suppressed IL12p40, presenting a robust inverse correlation in severe patients, which was strongly associated with persistent hyperinflammation in 8.3% of moderate pneumonia patients and 59.4% of severe patients. Discussion: Aberrant persistence of pulmonary and systemic inflammation might be associated with long COVID-19 sequelae. Our comprehensive analysis of inflammatory mediators in plasmarevealed the complexity of pneumonic inflammation in COVID-19 patients anddefined critical modules responsible for severe pneumonic progression.

AB - Introduction: Despite of massive endeavors to characterize inflammation in COVID-19 patients, the core network of inflammatory mediators responsible for severe pneumonia stillremain remains elusive. Methods: Here, we performed quantitative and kinetic analysis of 191 inflammatory factors in 955 plasma samples from 80 normal controls (sample n = 80) and 347 confirmed COVID-19 pneumonia patients (sample n = 875), including 8 deceased patients. Results: Differential expression analysis showed that 76% of plasmaproteins (145 factors) were upregulated in severe COVID-19 patients comparedwith moderate patients, confirming overt inflammatory responses in severe COVID-19 pneumonia patients. Global correlation analysis of the plasma factorsrevealed two core inflammatory modules, core I and II, comprising mainly myeloid cell and lymphoid cell compartments, respectively, with enhanced impact in a severity-dependent manner. We observed elevated IFNA1 and suppressed IL12p40, presenting a robust inverse correlation in severe patients, which was strongly associated with persistent hyperinflammation in 8.3% of moderate pneumonia patients and 59.4% of severe patients. Discussion: Aberrant persistence of pulmonary and systemic inflammation might be associated with long COVID-19 sequelae. Our comprehensive analysis of inflammatory mediators in plasmarevealed the complexity of pneumonic inflammation in COVID-19 patients anddefined critical modules responsible for severe pneumonic progression.

KW - COVID-19

KW - IFNa

KW - IL-12p40

KW - inflammation

KW - pneumonia

KW - SARS-CoV-2

UR - https://www.scopus.com/pages/publications/85147808038

U2 - 10.3389/fimmu.2023.1101808

DO - 10.3389/fimmu.2023.1101808

M3 - Article

C2 - 36776879

AN - SCOPUS:85147808038

SN - 1664-3224

VL - 14

JO - Frontiers in Immunology

JF - Frontiers in Immunology

M1 - 1101808

ER -

Elevated IFNA1 and suppressed IL12p40 associated with persistent hyperinflammation in COVID-19 pneumonia

Abstract

Keywords

UN SDGs

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