Crystal structure of the NS3-like helicase from Alongshan virus

Crystal structure of the NS3-like helicase from Alongshan virus

Alongshan virus (ALSV) is an emerging human pathogen that was identified in China and rapidly spread to the European continent in 2019, raising concerns about public health. ALSV belongs to the distinct Jingmenvirus group within the Flaviviridae family with segmented RNA genomes. While segments 2 an...

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Main Authors: Xiaopan Gao, Kaixiang Zhu, Justyna Aleksandra Wojdyla, Pu Chen, Bo Qin, Ziheng Li, Meitian Wang, Sheng Cui
Format: Article
Language:English
Published: International Union of Crystallography 2020-05-01
Series:IUCrJ
Subjects:
alongshan virus
ns3-like helicase
flavivirus
segmented viruses
Online Access:http://scripts.iucr.org/cgi-bin/paper?S2052252520003632
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spelling doaj-d06080b8dea34cea8e833e1e1375b5c42020-11-25T02:04:53ZengInternational Union of CrystallographyIUCrJ2052-25252020-05-017337538210.1107/S2052252520003632jt5043Crystal structure of the NS3-like helicase from Alongshan virusXiaopan Gao0Kaixiang Zhu1Justyna Aleksandra Wojdyla2Pu Chen3Bo Qin4Ziheng Li5Meitian Wang6Sheng Cui7NHC Key Laboratory of Systems Biology of Pathogens, Institute of Pathogen Biology and Center for Tuberculosis Research, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100730, People's Republic of ChinaNHC Key Laboratory of Systems Biology of Pathogens, Institute of Pathogen Biology and Center for Tuberculosis Research, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100730, People's Republic of ChinaSwiss Light Source at the Paul Scherrer Institute, CH-5232 Villigen, SwitzerlandNHC Key Laboratory of Systems Biology of Pathogens, Institute of Pathogen Biology and Center for Tuberculosis Research, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100730, People's Republic of ChinaNHC Key Laboratory of Systems Biology of Pathogens, Institute of Pathogen Biology and Center for Tuberculosis Research, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100730, People's Republic of ChinaNHC Key Laboratory of Systems Biology of Pathogens, Institute of Pathogen Biology and Center for Tuberculosis Research, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100730, People's Republic of ChinaSwiss Light Source at the Paul Scherrer Institute, CH-5232 Villigen, SwitzerlandNHC Key Laboratory of Systems Biology of Pathogens, Institute of Pathogen Biology and Center for Tuberculosis Research, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100730, People's Republic of ChinaAlongshan virus (ALSV) is an emerging human pathogen that was identified in China and rapidly spread to the European continent in 2019, raising concerns about public health. ALSV belongs to the distinct Jingmenvirus group within the Flaviviridae family with segmented RNA genomes. While segments 2 and 4 of the ALSV genome encode the VP1–VP3 proteins of unknown origin, segments 1 and 3 encode the NS2b–NS3 and NS5 proteins, which are related to Flavivirus nonstructural proteins, suggesting an evolutionary link between segmented and unsegmented viruses within the Flaviviridae family. Here, the enzymatic activity of the ALSV NS3-like helicase (NS3-Hel) was characterized and its crystal structure was determined to 2.9 Å resolution. ALSV NS3-Hel exhibits an ATPase activity that is comparable to those measured for Flavivirus NS3 helicases. The structure of ALSV NS3-Hel exhibits an overall fold similar to those of Flavivirus NS3 helicases. Despite the limited amino-acid sequence identity between ALSV NS3-Hel and Flavivirus NS3 helicases, structural features at the ATPase active site and the RNA-binding groove remain conserved in ALSV NS3-Hel. These findings provide a structural framework for drug design and suggest the possibility of developing a broad-spectrum antiviral drug against both Flavivirus and Jingmenvirus.http://scripts.iucr.org/cgi-bin/paper?S2052252520003632alongshan virusns3-like helicaseflavivirussegmented viruses
collection DOAJ
language English
format Article
sources DOAJ
author Xiaopan Gao
Kaixiang Zhu
Justyna Aleksandra Wojdyla
Pu Chen
Bo Qin
Ziheng Li
Meitian Wang
Sheng Cui
spellingShingle Xiaopan Gao
Kaixiang Zhu
Justyna Aleksandra Wojdyla
Pu Chen
Bo Qin
Ziheng Li
Meitian Wang
Sheng Cui
Crystal structure of the NS3-like helicase from Alongshan virus
IUCrJ
alongshan virus
ns3-like helicase
flavivirus
segmented viruses
author_facet Xiaopan Gao
Kaixiang Zhu
Justyna Aleksandra Wojdyla
Pu Chen
Bo Qin
Ziheng Li
Meitian Wang
Sheng Cui
author_sort Xiaopan Gao
title Crystal structure of the NS3-like helicase from Alongshan virus
title_short Crystal structure of the NS3-like helicase from Alongshan virus
title_full Crystal structure of the NS3-like helicase from Alongshan virus
title_fullStr Crystal structure of the NS3-like helicase from Alongshan virus
title_full_unstemmed Crystal structure of the NS3-like helicase from Alongshan virus
title_sort crystal structure of the ns3-like helicase from alongshan virus
publisher International Union of Crystallography
series IUCrJ
issn 2052-2525
publishDate 2020-05-01
description Alongshan virus (ALSV) is an emerging human pathogen that was identified in China and rapidly spread to the European continent in 2019, raising concerns about public health. ALSV belongs to the distinct Jingmenvirus group within the Flaviviridae family with segmented RNA genomes. While segments 2 and 4 of the ALSV genome encode the VP1–VP3 proteins of unknown origin, segments 1 and 3 encode the NS2b–NS3 and NS5 proteins, which are related to Flavivirus nonstructural proteins, suggesting an evolutionary link between segmented and unsegmented viruses within the Flaviviridae family. Here, the enzymatic activity of the ALSV NS3-like helicase (NS3-Hel) was characterized and its crystal structure was determined to 2.9 Å resolution. ALSV NS3-Hel exhibits an ATPase activity that is comparable to those measured for Flavivirus NS3 helicases. The structure of ALSV NS3-Hel exhibits an overall fold similar to those of Flavivirus NS3 helicases. Despite the limited amino-acid sequence identity between ALSV NS3-Hel and Flavivirus NS3 helicases, structural features at the ATPase active site and the RNA-binding groove remain conserved in ALSV NS3-Hel. These findings provide a structural framework for drug design and suggest the possibility of developing a broad-spectrum antiviral drug against both Flavivirus and Jingmenvirus.
topic alongshan virus
ns3-like helicase
flavivirus
segmented viruses
url http://scripts.iucr.org/cgi-bin/paper?S2052252520003632
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