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Genomic monitoring of SARS-CoV-2 uncovers an Nsp1 deletion variant that modulates type I interferon response

The SARS-CoV-2 virus, the causative agent of COVID-19, is undergoing constant mutation. Here, we utilized an integrative approach combining epidemiology, virus genome sequencing, clinical phenotyping, and experimental validation to locate mutations of clinical importance. We identified 35 recurrent...

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Autores principales: Lin, Jing-wen, Tang, Chao, Wei, Han-cheng, Du, Baowen, Chen, Chuan, Wang, Minjin, Zhou, Yongzhao, Yu, Ming-xia, Cheng, Lu, Kuivanen, Suvi, Ogando, Natacha S., Levanov, Lev, Zhao, Yuancun, Li, Chang-ling, Zhou, Ran, Li, Zhidan, Zhang, Yiming, Sun, Ke, Wang, Chengdi, Chen, Li, Xiao, Xia, Zheng, Xiuran, Chen, Sha-sha, Zhou, Zhen, Yang, Ruirui, Zhang, Dan, Xu, Mengying, Song, Junwei, Wang, Danrui, Li, Yupeng, Lei, ShiKun, Zeng, Wanqin, Yang, Qingxin, He, Ping, Zhang, Yaoyao, Zhou, Lifang, Cao, Ling, Luo, Feng, Liu, Huayi, Wang, Liping, Ye, Fei, Zhang, Ming, Li, Mengjiao, Fan, Wei, Li, Xinqiong, Li, Kaiju, Ke, Bowen, Xu, Jiannan, Yang, Huiping, He, Shusen, Pan, Ming, Yan, Yichen, Zha, Yi, Jiang, Lingyu, Yu, Changxiu, Liu, Yingfen, Xu, Zhiyong, Li, Qingfeng, Jiang, Yongmei, Sun, Jiufeng, Hong, Wei, Wei, Hongping, Lu, Guangwen, Vapalahti, Olli, Luo, Yunzi, Wei, Yuquan, Connor, Thomas, Tan, Wenjie, Snijder, Eric J., Smura, Teemu, Li, Weimin, Geng, Jia, Ying, Binwu, Chen, Lu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Inc. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7846228/
https://www.ncbi.nlm.nih.gov/pubmed/33548198
http://dx.doi.org/10.1016/j.chom.2021.01.015
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author Lin, Jing-wen
Tang, Chao
Wei, Han-cheng
Du, Baowen
Chen, Chuan
Wang, Minjin
Zhou, Yongzhao
Yu, Ming-xia
Cheng, Lu
Kuivanen, Suvi
Ogando, Natacha S.
Levanov, Lev
Zhao, Yuancun
Li, Chang-ling
Zhou, Ran
Li, Zhidan
Zhang, Yiming
Sun, Ke
Wang, Chengdi
Chen, Li
Xiao, Xia
Zheng, Xiuran
Chen, Sha-sha
Zhou, Zhen
Yang, Ruirui
Zhang, Dan
Xu, Mengying
Song, Junwei
Wang, Danrui
Li, Yupeng
Lei, ShiKun
Zeng, Wanqin
Yang, Qingxin
He, Ping
Zhang, Yaoyao
Zhou, Lifang
Cao, Ling
Luo, Feng
Liu, Huayi
Wang, Liping
Ye, Fei
Zhang, Ming
Li, Mengjiao
Fan, Wei
Li, Xinqiong
Li, Kaiju
Ke, Bowen
Xu, Jiannan
Yang, Huiping
He, Shusen
Pan, Ming
Yan, Yichen
Zha, Yi
Jiang, Lingyu
Yu, Changxiu
Liu, Yingfen
Xu, Zhiyong
Li, Qingfeng
Jiang, Yongmei
Sun, Jiufeng
Hong, Wei
Wei, Hongping
Lu, Guangwen
Vapalahti, Olli
Luo, Yunzi
Wei, Yuquan
Connor, Thomas
Tan, Wenjie
Snijder, Eric J.
Smura, Teemu
Li, Weimin
Geng, Jia
Ying, Binwu
Chen, Lu
author_facet Lin, Jing-wen
Tang, Chao
Wei, Han-cheng
Du, Baowen
Chen, Chuan
Wang, Minjin
Zhou, Yongzhao
Yu, Ming-xia
Cheng, Lu
Kuivanen, Suvi
Ogando, Natacha S.
Levanov, Lev
Zhao, Yuancun
Li, Chang-ling
Zhou, Ran
Li, Zhidan
Zhang, Yiming
Sun, Ke
Wang, Chengdi
Chen, Li
Xiao, Xia
Zheng, Xiuran
Chen, Sha-sha
Zhou, Zhen
Yang, Ruirui
Zhang, Dan
Xu, Mengying
Song, Junwei
Wang, Danrui
Li, Yupeng
Lei, ShiKun
Zeng, Wanqin
Yang, Qingxin
He, Ping
Zhang, Yaoyao
Zhou, Lifang
Cao, Ling
Luo, Feng
Liu, Huayi
Wang, Liping
Ye, Fei
Zhang, Ming
Li, Mengjiao
Fan, Wei
Li, Xinqiong
Li, Kaiju
Ke, Bowen
Xu, Jiannan
Yang, Huiping
He, Shusen
Pan, Ming
Yan, Yichen
Zha, Yi
Jiang, Lingyu
Yu, Changxiu
Liu, Yingfen
Xu, Zhiyong
Li, Qingfeng
Jiang, Yongmei
Sun, Jiufeng
Hong, Wei
Wei, Hongping
Lu, Guangwen
Vapalahti, Olli
Luo, Yunzi
Wei, Yuquan
Connor, Thomas
Tan, Wenjie
Snijder, Eric J.
Smura, Teemu
Li, Weimin
Geng, Jia
Ying, Binwu
Chen, Lu
author_sort Lin, Jing-wen
collection PubMed
description The SARS-CoV-2 virus, the causative agent of COVID-19, is undergoing constant mutation. Here, we utilized an integrative approach combining epidemiology, virus genome sequencing, clinical phenotyping, and experimental validation to locate mutations of clinical importance. We identified 35 recurrent variants, some of which are associated with clinical phenotypes related to severity. One variant, containing a deletion in the Nsp1-coding region (Δ500-532), was found in more than 20% of our sequenced samples and associates with higher RT-PCR cycle thresholds and lower serum IFN-β levels of infected patients. Deletion variants in this locus were found in 37 countries worldwide, and viruses isolated from clinical samples or engineered by reverse genetics with related deletions in Nsp1 also induce lower IFN-β responses in infected Calu-3 cells. Taken together, our virologic surveillance characterizes recurrent genetic diversity and identified mutations in Nsp1 of biological and clinical importance, which collectively may aid molecular diagnostics and drug design.
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spelling pubmed-78462282021-02-01 Genomic monitoring of SARS-CoV-2 uncovers an Nsp1 deletion variant that modulates type I interferon response Lin, Jing-wen Tang, Chao Wei, Han-cheng Du, Baowen Chen, Chuan Wang, Minjin Zhou, Yongzhao Yu, Ming-xia Cheng, Lu Kuivanen, Suvi Ogando, Natacha S. Levanov, Lev Zhao, Yuancun Li, Chang-ling Zhou, Ran Li, Zhidan Zhang, Yiming Sun, Ke Wang, Chengdi Chen, Li Xiao, Xia Zheng, Xiuran Chen, Sha-sha Zhou, Zhen Yang, Ruirui Zhang, Dan Xu, Mengying Song, Junwei Wang, Danrui Li, Yupeng Lei, ShiKun Zeng, Wanqin Yang, Qingxin He, Ping Zhang, Yaoyao Zhou, Lifang Cao, Ling Luo, Feng Liu, Huayi Wang, Liping Ye, Fei Zhang, Ming Li, Mengjiao Fan, Wei Li, Xinqiong Li, Kaiju Ke, Bowen Xu, Jiannan Yang, Huiping He, Shusen Pan, Ming Yan, Yichen Zha, Yi Jiang, Lingyu Yu, Changxiu Liu, Yingfen Xu, Zhiyong Li, Qingfeng Jiang, Yongmei Sun, Jiufeng Hong, Wei Wei, Hongping Lu, Guangwen Vapalahti, Olli Luo, Yunzi Wei, Yuquan Connor, Thomas Tan, Wenjie Snijder, Eric J. Smura, Teemu Li, Weimin Geng, Jia Ying, Binwu Chen, Lu Cell Host Microbe Article The SARS-CoV-2 virus, the causative agent of COVID-19, is undergoing constant mutation. Here, we utilized an integrative approach combining epidemiology, virus genome sequencing, clinical phenotyping, and experimental validation to locate mutations of clinical importance. We identified 35 recurrent variants, some of which are associated with clinical phenotypes related to severity. One variant, containing a deletion in the Nsp1-coding region (Δ500-532), was found in more than 20% of our sequenced samples and associates with higher RT-PCR cycle thresholds and lower serum IFN-β levels of infected patients. Deletion variants in this locus were found in 37 countries worldwide, and viruses isolated from clinical samples or engineered by reverse genetics with related deletions in Nsp1 also induce lower IFN-β responses in infected Calu-3 cells. Taken together, our virologic surveillance characterizes recurrent genetic diversity and identified mutations in Nsp1 of biological and clinical importance, which collectively may aid molecular diagnostics and drug design. Elsevier Inc. 2021-03-10 2021-01-29 /pmc/articles/PMC7846228/ /pubmed/33548198 http://dx.doi.org/10.1016/j.chom.2021.01.015 Text en © 2021 Elsevier Inc. Since January 2020 Elsevier has created a COVID-19 resource centre with free information in English and Mandarin on the novel coronavirus COVID-19. The COVID-19 resource centre is hosted on Elsevier Connect, the company's public news and information website. Elsevier hereby grants permission to make all its COVID-19-related research that is available on the COVID-19 resource centre - including this research content - immediately available in PubMed Central and other publicly funded repositories, such as the WHO COVID database with rights for unrestricted research re-use and analyses in any form or by any means with acknowledgement of the original source. These permissions are granted for free by Elsevier for as long as the COVID-19 resource centre remains active.
spellingShingle Article
Lin, Jing-wen
Tang, Chao
Wei, Han-cheng
Du, Baowen
Chen, Chuan
Wang, Minjin
Zhou, Yongzhao
Yu, Ming-xia
Cheng, Lu
Kuivanen, Suvi
Ogando, Natacha S.
Levanov, Lev
Zhao, Yuancun
Li, Chang-ling
Zhou, Ran
Li, Zhidan
Zhang, Yiming
Sun, Ke
Wang, Chengdi
Chen, Li
Xiao, Xia
Zheng, Xiuran
Chen, Sha-sha
Zhou, Zhen
Yang, Ruirui
Zhang, Dan
Xu, Mengying
Song, Junwei
Wang, Danrui
Li, Yupeng
Lei, ShiKun
Zeng, Wanqin
Yang, Qingxin
He, Ping
Zhang, Yaoyao
Zhou, Lifang
Cao, Ling
Luo, Feng
Liu, Huayi
Wang, Liping
Ye, Fei
Zhang, Ming
Li, Mengjiao
Fan, Wei
Li, Xinqiong
Li, Kaiju
Ke, Bowen
Xu, Jiannan
Yang, Huiping
He, Shusen
Pan, Ming
Yan, Yichen
Zha, Yi
Jiang, Lingyu
Yu, Changxiu
Liu, Yingfen
Xu, Zhiyong
Li, Qingfeng
Jiang, Yongmei
Sun, Jiufeng
Hong, Wei
Wei, Hongping
Lu, Guangwen
Vapalahti, Olli
Luo, Yunzi
Wei, Yuquan
Connor, Thomas
Tan, Wenjie
Snijder, Eric J.
Smura, Teemu
Li, Weimin
Geng, Jia
Ying, Binwu
Chen, Lu
Genomic monitoring of SARS-CoV-2 uncovers an Nsp1 deletion variant that modulates type I interferon response
title Genomic monitoring of SARS-CoV-2 uncovers an Nsp1 deletion variant that modulates type I interferon response
title_full Genomic monitoring of SARS-CoV-2 uncovers an Nsp1 deletion variant that modulates type I interferon response
title_fullStr Genomic monitoring of SARS-CoV-2 uncovers an Nsp1 deletion variant that modulates type I interferon response
title_full_unstemmed Genomic monitoring of SARS-CoV-2 uncovers an Nsp1 deletion variant that modulates type I interferon response
title_short Genomic monitoring of SARS-CoV-2 uncovers an Nsp1 deletion variant that modulates type I interferon response
title_sort genomic monitoring of sars-cov-2 uncovers an nsp1 deletion variant that modulates type i interferon response
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7846228/
https://www.ncbi.nlm.nih.gov/pubmed/33548198
http://dx.doi.org/10.1016/j.chom.2021.01.015
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