Immune Cells Are Differentially Affected by SARS-CoV-2 Viral Loads iK18-hACE2 Mice

Jung Ah Kim; Sung Hee Kim; Jeong Jin Kim; Hyuna Noh; Su Bin Lee; Haengdueng Jeong; Jiseon Kim; Donghun Jeon; Jung Seon Seo; Dain On; Suhyeon Yoon; Sang Gyu Lee; Youn Woo Lee; Hui Jeong Jang; In Ho Park; Jooyeon Oh; Sang Hyuk Seok; Yu Jin Lee; Seung Min Hong; Se Hee An; Joon Yong Bae; Jung Ah Choi; Seo Yeon Kim; Young Been Kim; Ji Yeon Hwang; Hyo Jung Lee; Hong Bin Kim; Dae Gwin Jeong; Daesub Song; Manki Song; Man Seong Park; Kang Seuk Choi; Jun Won Park; Jun Won Yun; Jeon Soo Shin; Ho Young Lee; Ho Keun Kwon; Jun Young Seo; Ki Taek Nam; Heon Yung Gee; Je Kyung Seong

doi:10.4110/in.2024.24.e7

Immune Cells Are Differentially Affected by SARS-CoV-2 Viral Loads iK18-hACE2 Mice

Jung Ah Kim
, Sung Hee Kim
, Jeong Jin Kim
, Hyuna Noh
, Su Bin Lee
, Haengdueng Jeong
, Jiseon Kim
, Donghun Jeon
, Jung Seon Seo
, Dain On
, Suhyeon Yoon
, Sang Gyu Lee
, Youn Woo Lee
, Hui Jeong Jang
, In Ho Park
, Jooyeon Oh
, Sang Hyuk Seok
, Yu Jin Lee
, Seung Min Hong
, Se Hee An

Joon Yong Bae, Jung Ah Choi, Seo Yeon Kim, Young Been Kim, Ji Yeon Hwang, Hyo Jung Lee, Hong Bin Kim, Dae Gwin Jeong, Daesub Song, Manki Song, Man Seong Park, Kang Seuk Choi, Jun Won Park, Jun Won Yun, Jeon Soo Shin, Ho Young Lee, Ho Keun Kwon, Jun Young Seo^*, Ki Taek Nam^*, Heon Yung Gee^*, Je Kyung Seong^*

^*Corresponding author for this work

Department of Biomedical Sciences

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

1 Citation (Scopus)

Abstract

Viral load and the duration of viral shedding of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) are important determinants of the transmission of coronavirus disease 2019. In this study, we examined the effects of viral doses on the lung and spleen of K18-hACE2 transgenic mice by temporal histological and transcriptional analyses. Approximately, 1×10⁵ plaque-forming units (PFU) of SARS-CoV-2 induced strong host responses in the lungs from 2 days post inoculation (dpi) which did not recover until the mice died, whereas responses to the virus were obvious at 5 days, recovering to the basal state by 14 dpi at 1×10² PFU. Further, flow cytometry showed that number of CD8+ T cells continuously increased in 1×10² PFU-virus-infected lungs from 2 dpi, but not in 1×10⁵ PFU-virus-infected lungs. In spleens, responses to the virus were prominent from 2 dpi, and number of B cells was significantly decreased at 1×10⁵ PFU; however, 1×10² PFU of virus induced very weak responses from 2 dpi which recovered by 10 dpi. Although the defense responses returned to normal and the mice survived, lung histology showed evidence of fibrosis, suggesting sequelae of SARS-CoV-2 infection. Our findings indicate that specific effectors of the immune response in the lung and spleen were either increased or depleted in response to doses of SARS-CoV-2. This study demonstrated that the response of local and systemic immune effectors to a viral infection varies with viral dose, which either exacerbates the severity of the infection or accelerates its elimination.

Original language	English
Article number	e7
Journal	Immune Network
Volume	24
Issue number	2
DOIs	https://doi.org/10.4110/in.2024.24.e7
Publication status	Published - 2024 Apr

Bibliographical note

Publisher Copyright:
© 2024. The Korean Association of Immunologists.

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

Dose-response relationship, immunologic
Immune response
K18-hACE2 mice
SARS-CoV-2
Transcriptome profiling

ASJC Scopus subject areas

Immunology and Allergy
Immunology
Infectious Diseases

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10.4110/in.2024.24.e7

Cite this

Kim, J. A., Kim, S. H., Kim, J. J., Noh, H., Lee, S. B., Jeong, H., Kim, J., Jeon, D., Seo, J. S., On, D., Yoon, S., Lee, S. G., Lee, Y. W., Jang, H. J., Park, I. H., Oh, J., Seok, S. H., Lee, Y. J., Hong, S. M., ... Seong, J. K. (2024). Immune Cells Are Differentially Affected by SARS-CoV-2 Viral Loads iK18-hACE2 Mice. Immune Network, 24(2), Article e7. https://doi.org/10.4110/in.2024.24.e7

Kim, JA, Kim, SH, Kim, JJ, Noh, H, Lee, SB, Jeong, H, Kim, J, Jeon, D, Seo, JS, On, D, Yoon, S, Lee, SG, Lee, YW, Jang, HJ, Park, IH, Oh, J, Seok, SH, Lee, YJ, Hong, SM, An, SH, Bae, JY, Choi, JA, Kim, SY, Kim, YB, Hwang, JY, Lee, HJ, Kim, HB, Jeong, DG, Song, D, Song, M, Park, MS, Choi, KS, Park, JW, Yun, JW, Shin, JS, Lee, HY, Kwon, HK, Seo, JY, Nam, KT, Gee, HY & Seong, JK 2024, 'Immune Cells Are Differentially Affected by SARS-CoV-2 Viral Loads iK18-hACE2 Mice', Immune Network, vol. 24, no. 2, e7. https://doi.org/10.4110/in.2024.24.e7

@article{01b09436b9cc4e3cb57b34d9442fb18f,

title = "Immune Cells Are Differentially Affected by SARS-CoV-2 Viral Loads iK18-hACE2 Mice",

abstract = "Viral load and the duration of viral shedding of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) are important determinants of the transmission of coronavirus disease 2019. In this study, we examined the effects of viral doses on the lung and spleen of K18-hACE2 transgenic mice by temporal histological and transcriptional analyses. Approximately, 1×105 plaque-forming units (PFU) of SARS-CoV-2 induced strong host responses in the lungs from 2 days post inoculation (dpi) which did not recover until the mice died, whereas responses to the virus were obvious at 5 days, recovering to the basal state by 14 dpi at 1×102 PFU. Further, flow cytometry showed that number of CD8+ T cells continuously increased in 1×102 PFU-virus-infected lungs from 2 dpi, but not in 1×105 PFU-virus-infected lungs. In spleens, responses to the virus were prominent from 2 dpi, and number of B cells was significantly decreased at 1×105 PFU; however, 1×102 PFU of virus induced very weak responses from 2 dpi which recovered by 10 dpi. Although the defense responses returned to normal and the mice survived, lung histology showed evidence of fibrosis, suggesting sequelae of SARS-CoV-2 infection. Our findings indicate that specific effectors of the immune response in the lung and spleen were either increased or depleted in response to doses of SARS-CoV-2. This study demonstrated that the response of local and systemic immune effectors to a viral infection varies with viral dose, which either exacerbates the severity of the infection or accelerates its elimination.",

keywords = "Dose-response relationship, immunologic, Immune response, K18-hACE2 mice, SARS-CoV-2, Transcriptome profiling",

author = "Kim, \{Jung Ah\} and Kim, \{Sung Hee\} and Kim, \{Jeong Jin\} and Hyuna Noh and Lee, \{Su Bin\} and Haengdueng Jeong and Jiseon Kim and Donghun Jeon and Seo, \{Jung Seon\} and Dain On and Suhyeon Yoon and Lee, \{Sang Gyu\} and Lee, \{Youn Woo\} and Jang, \{Hui Jeong\} and Park, \{In Ho\} and Jooyeon Oh and Seok, \{Sang Hyuk\} and Lee, \{Yu Jin\} and Hong, \{Seung Min\} and An, \{Se Hee\} and Bae, \{Joon Yong\} and Choi, \{Jung Ah\} and Kim, \{Seo Yeon\} and Kim, \{Young Been\} and Hwang, \{Ji Yeon\} and Lee, \{Hyo Jung\} and Kim, \{Hong Bin\} and Jeong, \{Dae Gwin\} and Daesub Song and Manki Song and Park, \{Man Seong\} and Choi, \{Kang Seuk\} and Park, \{Jun Won\} and Yun, \{Jun Won\} and Shin, \{Jeon Soo\} and Lee, \{Ho Young\} and Kwon, \{Ho Keun\} and Seo, \{Jun Young\} and Nam, \{Ki Taek\} and Gee, \{Heon Yung\} and Seong, \{Je Kyung\}",

note = "Publisher Copyright: {\textcopyright} 2024. The Korean Association of Immunologists.",

year = "2024",

month = apr,

doi = "10.4110/in.2024.24.e7",

language = "English",

volume = "24",

journal = "Immune Network",

issn = "1598-2629",

publisher = "Korean Association of Immunologists",

number = "2",

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T1 - Immune Cells Are Differentially Affected by SARS-CoV-2 Viral Loads iK18-hACE2 Mice

AU - Kim, Jung Ah

AU - Kim, Sung Hee

AU - Kim, Jeong Jin

AU - Noh, Hyuna

AU - Lee, Su Bin

AU - Jeong, Haengdueng

AU - Kim, Jiseon

AU - Jeon, Donghun

AU - Seo, Jung Seon

AU - On, Dain

AU - Yoon, Suhyeon

AU - Lee, Sang Gyu

AU - Lee, Youn Woo

AU - Jang, Hui Jeong

AU - Park, In Ho

AU - Oh, Jooyeon

AU - Seok, Sang Hyuk

AU - Lee, Yu Jin

AU - Hong, Seung Min

AU - An, Se Hee

AU - Bae, Joon Yong

AU - Choi, Jung Ah

AU - Kim, Seo Yeon

AU - Kim, Young Been

AU - Hwang, Ji Yeon

AU - Lee, Hyo Jung

AU - Kim, Hong Bin

AU - Jeong, Dae Gwin

AU - Song, Daesub

AU - Song, Manki

AU - Park, Man Seong

AU - Choi, Kang Seuk

AU - Park, Jun Won

AU - Yun, Jun Won

AU - Shin, Jeon Soo

AU - Lee, Ho Young

AU - Kwon, Ho Keun

AU - Seo, Jun Young

AU - Nam, Ki Taek

AU - Gee, Heon Yung

AU - Seong, Je Kyung

PY - 2024/4

Y1 - 2024/4

N2 - Viral load and the duration of viral shedding of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) are important determinants of the transmission of coronavirus disease 2019. In this study, we examined the effects of viral doses on the lung and spleen of K18-hACE2 transgenic mice by temporal histological and transcriptional analyses. Approximately, 1×105 plaque-forming units (PFU) of SARS-CoV-2 induced strong host responses in the lungs from 2 days post inoculation (dpi) which did not recover until the mice died, whereas responses to the virus were obvious at 5 days, recovering to the basal state by 14 dpi at 1×102 PFU. Further, flow cytometry showed that number of CD8+ T cells continuously increased in 1×102 PFU-virus-infected lungs from 2 dpi, but not in 1×105 PFU-virus-infected lungs. In spleens, responses to the virus were prominent from 2 dpi, and number of B cells was significantly decreased at 1×105 PFU; however, 1×102 PFU of virus induced very weak responses from 2 dpi which recovered by 10 dpi. Although the defense responses returned to normal and the mice survived, lung histology showed evidence of fibrosis, suggesting sequelae of SARS-CoV-2 infection. Our findings indicate that specific effectors of the immune response in the lung and spleen were either increased or depleted in response to doses of SARS-CoV-2. This study demonstrated that the response of local and systemic immune effectors to a viral infection varies with viral dose, which either exacerbates the severity of the infection or accelerates its elimination.

AB - Viral load and the duration of viral shedding of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) are important determinants of the transmission of coronavirus disease 2019. In this study, we examined the effects of viral doses on the lung and spleen of K18-hACE2 transgenic mice by temporal histological and transcriptional analyses. Approximately, 1×105 plaque-forming units (PFU) of SARS-CoV-2 induced strong host responses in the lungs from 2 days post inoculation (dpi) which did not recover until the mice died, whereas responses to the virus were obvious at 5 days, recovering to the basal state by 14 dpi at 1×102 PFU. Further, flow cytometry showed that number of CD8+ T cells continuously increased in 1×102 PFU-virus-infected lungs from 2 dpi, but not in 1×105 PFU-virus-infected lungs. In spleens, responses to the virus were prominent from 2 dpi, and number of B cells was significantly decreased at 1×105 PFU; however, 1×102 PFU of virus induced very weak responses from 2 dpi which recovered by 10 dpi. Although the defense responses returned to normal and the mice survived, lung histology showed evidence of fibrosis, suggesting sequelae of SARS-CoV-2 infection. Our findings indicate that specific effectors of the immune response in the lung and spleen were either increased or depleted in response to doses of SARS-CoV-2. This study demonstrated that the response of local and systemic immune effectors to a viral infection varies with viral dose, which either exacerbates the severity of the infection or accelerates its elimination.

KW - Dose-response relationship, immunologic

KW - Immune response

KW - K18-hACE2 mice

KW - SARS-CoV-2

KW - Transcriptome profiling

UR - https://www.scopus.com/pages/publications/85200028215

U2 - 10.4110/in.2024.24.e7

DO - 10.4110/in.2024.24.e7

M3 - Article

AN - SCOPUS:85200028215

SN - 1598-2629

VL - 24

JO - Immune Network

JF - Immune Network

IS - 2

M1 - e7

ER -

Immune Cells Are Differentially Affected by SARS-CoV-2 Viral Loads iK18-hACE2 Mice

Abstract

Bibliographical note

UN SDGs

Keywords

ASJC Scopus subject areas

Access to Document

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