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Clinical analysis and pluripotent stem cells-based model reveal possible impacts of ACE2 and lung progenitor cells on infants vulnerable to COVID-19

Introduction: An increasing number of children with severe coronavirus disease 2019 (COVID-19) is being reported, yet the spectrum of disease severity and expression patterns of angiotensin-converting enzyme 2 (ACE2) in children at different developmental stages are largely unknow. Methods: We analy...

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Autores principales: Zhang, Zhao, Guo, Liyan, Lu, Xiaoxia, Zhang, Che, Huang, Li, Wang, Xianfeng, Duan, Fuyu, Liang, Huiying, Chen, Peikai, Zeng, Liang, Shao, Jianbo, Li, Hui, Li, Le, Liu, Li, Li, Cheng, Zhang, Jinqiu, Ma, Chui Yan, Kwan, Ka Yi, Liu, Wei, Xu, Yi, Gu, Xiaoqiong, Jiang, Hua, Du, Hui, Zhang, Ting, Wu, Yanheng, Yu, Guangyin, Chen, Junhui, Luo, Ruibang, Liao, Can, Tse, Hung-fat, Chen, Zhiwei, Chen, Huanhuan Joyce, Xia, Huimin, Lian, Qizhou
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7797681/
https://www.ncbi.nlm.nih.gov/pubmed/33500718
http://dx.doi.org/10.7150/thno.53136
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author Zhang, Zhao
Guo, Liyan
Lu, Xiaoxia
Zhang, Che
Huang, Li
Wang, Xianfeng
Duan, Fuyu
Liang, Huiying
Chen, Peikai
Zeng, Liang
Shao, Jianbo
Li, Hui
Li, Le
Liu, Li
Li, Cheng
Zhang, Jinqiu
Ma, Chui Yan
Kwan, Ka Yi
Liu, Wei
Xu, Yi
Gu, Xiaoqiong
Jiang, Hua
Du, Hui
Zhang, Ting
Wu, Yanheng
Yu, Guangyin
Chen, Junhui
Luo, Ruibang
Liao, Can
Tse, Hung-fat
Chen, Zhiwei
Chen, Huanhuan Joyce
Xia, Huimin
Lian, Qizhou
author_facet Zhang, Zhao
Guo, Liyan
Lu, Xiaoxia
Zhang, Che
Huang, Li
Wang, Xianfeng
Duan, Fuyu
Liang, Huiying
Chen, Peikai
Zeng, Liang
Shao, Jianbo
Li, Hui
Li, Le
Liu, Li
Li, Cheng
Zhang, Jinqiu
Ma, Chui Yan
Kwan, Ka Yi
Liu, Wei
Xu, Yi
Gu, Xiaoqiong
Jiang, Hua
Du, Hui
Zhang, Ting
Wu, Yanheng
Yu, Guangyin
Chen, Junhui
Luo, Ruibang
Liao, Can
Tse, Hung-fat
Chen, Zhiwei
Chen, Huanhuan Joyce
Xia, Huimin
Lian, Qizhou
author_sort Zhang, Zhao
collection PubMed
description Introduction: An increasing number of children with severe coronavirus disease 2019 (COVID-19) is being reported, yet the spectrum of disease severity and expression patterns of angiotensin-converting enzyme 2 (ACE2) in children at different developmental stages are largely unknow. Methods: We analysed clinical features in a cohort of 173 children with COVID-19 (0-15 yrs.-old) between January 22, 2020 and March 15, 2020. We systematically examined the expression and distribution of ACE2 in different developmental stages of children by using a combination of children's lung biopsies, pluripotent stem cell-derived lung cells, RNA-sequencing profiles, and ex vivo SARS-CoV-2 pseudoviral infections. Results: It revealed that infants (< 1yrs.-old), with a weaker potency of immune response, are more vulnerable to develop pneumonia whereas older children (> 1 yrs.-old) are more resistant to lung injury. The expression levels of ACE2 however do not vary by age in children's lung. ACE2 is notably expressed not only in Alveolar Type II (AT II) cells, but also in SOX9 positive lung progenitor cells detected in both pluripotent stem cell derivatives and infants' lungs. The ACE2(+)SOX9(+) cells are readily infected by SARS-CoV-2 pseudovirus and the numbers of the double positive cells are significantly decreased in older children. Conclusions: Infants (< 1 yrs.-old) with SARS-CoV-2 infection are more vulnerable to lung injuries. ACE2 expression in multiple types of lung cells including SOX9 positive progenitor cells, in cooperation with an unestablished immune system, could be risk factors contributing to vulnerability of infants with COVID-19. There is a need to continue monitoring lung development in young children who have recovered from SARS-CoV-2 infection.
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spelling pubmed-77976812021-01-25 Clinical analysis and pluripotent stem cells-based model reveal possible impacts of ACE2 and lung progenitor cells on infants vulnerable to COVID-19 Zhang, Zhao Guo, Liyan Lu, Xiaoxia Zhang, Che Huang, Li Wang, Xianfeng Duan, Fuyu Liang, Huiying Chen, Peikai Zeng, Liang Shao, Jianbo Li, Hui Li, Le Liu, Li Li, Cheng Zhang, Jinqiu Ma, Chui Yan Kwan, Ka Yi Liu, Wei Xu, Yi Gu, Xiaoqiong Jiang, Hua Du, Hui Zhang, Ting Wu, Yanheng Yu, Guangyin Chen, Junhui Luo, Ruibang Liao, Can Tse, Hung-fat Chen, Zhiwei Chen, Huanhuan Joyce Xia, Huimin Lian, Qizhou Theranostics Research Paper Introduction: An increasing number of children with severe coronavirus disease 2019 (COVID-19) is being reported, yet the spectrum of disease severity and expression patterns of angiotensin-converting enzyme 2 (ACE2) in children at different developmental stages are largely unknow. Methods: We analysed clinical features in a cohort of 173 children with COVID-19 (0-15 yrs.-old) between January 22, 2020 and March 15, 2020. We systematically examined the expression and distribution of ACE2 in different developmental stages of children by using a combination of children's lung biopsies, pluripotent stem cell-derived lung cells, RNA-sequencing profiles, and ex vivo SARS-CoV-2 pseudoviral infections. Results: It revealed that infants (< 1yrs.-old), with a weaker potency of immune response, are more vulnerable to develop pneumonia whereas older children (> 1 yrs.-old) are more resistant to lung injury. The expression levels of ACE2 however do not vary by age in children's lung. ACE2 is notably expressed not only in Alveolar Type II (AT II) cells, but also in SOX9 positive lung progenitor cells detected in both pluripotent stem cell derivatives and infants' lungs. The ACE2(+)SOX9(+) cells are readily infected by SARS-CoV-2 pseudovirus and the numbers of the double positive cells are significantly decreased in older children. Conclusions: Infants (< 1 yrs.-old) with SARS-CoV-2 infection are more vulnerable to lung injuries. ACE2 expression in multiple types of lung cells including SOX9 positive progenitor cells, in cooperation with an unestablished immune system, could be risk factors contributing to vulnerability of infants with COVID-19. There is a need to continue monitoring lung development in young children who have recovered from SARS-CoV-2 infection. Ivyspring International Publisher 2021-01-01 /pmc/articles/PMC7797681/ /pubmed/33500718 http://dx.doi.org/10.7150/thno.53136 Text en © The author(s) This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Zhang, Zhao
Guo, Liyan
Lu, Xiaoxia
Zhang, Che
Huang, Li
Wang, Xianfeng
Duan, Fuyu
Liang, Huiying
Chen, Peikai
Zeng, Liang
Shao, Jianbo
Li, Hui
Li, Le
Liu, Li
Li, Cheng
Zhang, Jinqiu
Ma, Chui Yan
Kwan, Ka Yi
Liu, Wei
Xu, Yi
Gu, Xiaoqiong
Jiang, Hua
Du, Hui
Zhang, Ting
Wu, Yanheng
Yu, Guangyin
Chen, Junhui
Luo, Ruibang
Liao, Can
Tse, Hung-fat
Chen, Zhiwei
Chen, Huanhuan Joyce
Xia, Huimin
Lian, Qizhou
Clinical analysis and pluripotent stem cells-based model reveal possible impacts of ACE2 and lung progenitor cells on infants vulnerable to COVID-19
title Clinical analysis and pluripotent stem cells-based model reveal possible impacts of ACE2 and lung progenitor cells on infants vulnerable to COVID-19
title_full Clinical analysis and pluripotent stem cells-based model reveal possible impacts of ACE2 and lung progenitor cells on infants vulnerable to COVID-19
title_fullStr Clinical analysis and pluripotent stem cells-based model reveal possible impacts of ACE2 and lung progenitor cells on infants vulnerable to COVID-19
title_full_unstemmed Clinical analysis and pluripotent stem cells-based model reveal possible impacts of ACE2 and lung progenitor cells on infants vulnerable to COVID-19
title_short Clinical analysis and pluripotent stem cells-based model reveal possible impacts of ACE2 and lung progenitor cells on infants vulnerable to COVID-19
title_sort clinical analysis and pluripotent stem cells-based model reveal possible impacts of ace2 and lung progenitor cells on infants vulnerable to covid-19
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7797681/
https://www.ncbi.nlm.nih.gov/pubmed/33500718
http://dx.doi.org/10.7150/thno.53136
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