Your search keyword '"Zhenzhi Han"' showing total 39 results

1. The Cumulative Variations of Respiratory Syncytial Virus Fusion Protein (F) in Ten Consecutive Years in China

Author

Fengjie Wang, Mingli Jiang, Zhenzhi Han, Yanpeng Xu, Yu Sun, Runan Zhu, Dongmei Chen, Qi Guo, Yutong Zhou, Yao Yao, Ling Cao, Dong Qu, Muya Li, and Linqing Zhao

Subjects

respiratory syncytial virus, fusion protein, antigenic sites, variations, Other systems of medicine, RZ201-999

Abstract

Background: Variations in the fusion (F) protein of respiratory syncytial virus (RSV) with main antigenic sites I–V and Ø may affect the development of RSV vaccines and therapies. Methods: In the study, 30 respiratory specimens positive for RSV were randomly selected from children with acute lower respiratory infections (ALRI) in Beijing every year from 2012 to 2021 for F gene sequencing. Then, 300 F gene sequences and 508 uploaded to GenBank from China were subjected to phylogenetic analysis. Results: The results indicated the nucleotide identities were 95.4–100% among 446 sequences of RSV A, and 96.3–100% among 362 of RSV B. The most common variant loci were N80K (100.00%) and R213S (97.76%) for site Ø, and V384I/T (98.43%) for site I among sequences of RSV A, and M152I (100.00%), I185V (100.00%), and L172Q/H (94.48%) for site V, and R202Q (99.45%) for site Ø among sequences of RSV B. N276S appears in 95.29% sequences of RSV A, while S276N and N262 I/S appear in 1.38% and 0.55% sequences of RSV B, respectively. No variation was found in all sequences at the binding sites of 14N4 and motavizumab. Conclusions: There were cumulative variations of the RSV F gene, especially at some binding sites of antigenic sites.

Published

2024

2. Diverse Head-to-Tail Sequences in the Circular Genome of Human Bocavirus Genotype 1 among Children with Acute Respiratory Infections Implied the Switch of Template Chain in the Rolling-Circle Replication Model

Author

Kexiang Zhang, Ri De, Yanpeng Xu, Zhenzhi Han, Runan Zhu, Yu Sun, Liping Jia, Dongmei Chen, Yutong Zhou, Qi Guo, Yao Yao, Shuang Liu, Dong Qu, Yuan Qian, and Linqing Zhao

Subjects

children, human bocavirus genotype 1, head-to-tail sequence, diverse, rolling-circle replication model, Medicine

Abstract

Head-to-tail sequences have been reported in human bocavirus (HBoV) 1-4. To reveal their features and functions, HBoV DNA was screened among respiratory specimens from pediatric patients with an acute respiratory infection (ARI) between April 2020 and December 2022, followed by HBoV genotyping. Head-to-tail sequences were detected using nested PCR, TA cloning, and Sanger sequencing, and these findings were confirmed by mNGS and amplicon sequencing. The secondary structure was predicted using the Mfold web server. The results indicated that head-to-tail sequences were detected in 42 specimens through TA cloning from 351 specimens positive for HBoV1 DNA, yielding 92 sequences into 32 types and 2 categories. Additionally, head-to-tail sequences were detected in 16 specimens by amplicon sequencing, yielding 60 sequences categorized into 23 types. The 374nt type, detected in 13 specimens, contains variants 374a and 374b, which differ in the unpaired loop regions of the palindrome or complementary reverse sequences, implying a switch of template chains during the replication process. The mNGS results in three specimens confirmed the presence of circular genome in copies below 1%. In conclusion, head-to-tail sequences of HBoV1 were common in children with ARI and were highly diverse in length and sequences. The variants may be generated by the switch of the template chain in the rolling-circle replication model.

Published

2024

3. High-Frequency Recombination of Human Adenovirus in Children with Acute Respiratory Tract Infections in Beijing, China

Author

Fangming Wang, Ri De, Zhenzhi Han, Yanpeng Xu, Runan Zhu, Yu Sun, Dongmei Chen, Yutong Zhou, Qi Guo, Dong Qu, Ling Cao, Liying Liu, and Linqing Zhao

Subjects

children, human adenovirus, co-infections, recombination, HAdV-D115, Microbiology, QR1-502

Abstract

Recombination events in human adenovirus (HAdV) have led to some new highly pathogenic or infectious types. It is vital to monitor recombinant HAdVs, especially in children with acute respiratory tract infections (ARIs). In the retrospective study, HAdV positive specimens were collected from pediatric patients with ARIs during 2015 to 2021, then typed by sequence analysis of the penton base, hexon and fiber gene sequence. For those with inconsistent typing results, a modified method with species-specific primer sets of a fiber gene sequence was developed to distinguish co-infections of different types from recombinant HAdV infections. Then, plaque assays combined with meta-genomic next-generation sequencing (mNGS) were used to reveal the HAdV genomic characteristics. There were 466 cases positive for HAdV DNA (2.89%, 466/16,097) and 350 (75.11%, 350/466) successfully typed with the most prevalent types HAdV-B3 (56.57%, 198/350) and HAdV-B7 (32.00%, 112/350), followed by HAdV-C1 (6.00%, 21/350). Among 35 cases (7.51%, 35/466) with inconsistent typing results, nine cases were confirmed as co-infections by different types of HAdVs, and 26 cases as recombinant HAdVs in six genetic patterns primarily clustered to species C (25 cases) in pattern 1–5, or species D (1 case) in pattern 6. The novel recombinant HAdV of species D was identified with multiple recombinant events among HAdV-D53, HAdV-D64, and HAdV-D8, and officially named as HAdV-D115. High-frequency recombination of HAdVs in six genetic recombination patterns were identified among children with ARIs in Beijing. Specifically, there is a novel Adenovirus D human/CHN/S8130/2023/115[P22H8F8] designed as HAdV D115.

Published

2024

4. Whole-genome analysis of coxsackievirus B3 reflects its genetic diversity in China and worldwide

Author

Qian Yang, Dongmei Yan, Yang Song, Shuangli Zhu, Yun He, Zhenzhi Han, Dongyan Wang, Tianjiao Ji, Yong Zhang, and Wenbo Xu

Subjects

Coxsackievirus B3 (CVB3), Genome, Recombination lineages, Genetic diversity, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Coxsackievirus B3 (CVB3) has emerged as an active pathogen in myocarditis, aseptic meningitis, hand, foot, and mouth disease (HFMD), and pancreatitis, and is a heavy burden on public health. However, CVB3 has not been systematically analyzed with regard to whole-genome diversity and recombination. Therefore, this study was undertaken to systematically examine the genetic characteristics of CVB3 based on its whole genome. Methods We combined CVB3 isolates from our national HFMD surveillance and global sequences retrieved from GenBank. Phylogenetic analysis was performed to examine the whole genome variety and recombination forms of CVB3 in China and worldwide. Results Phylogenetic analysis showed that CVB3 strains isolated worldwide could be classified into clusters A–E based on the sequence of the entire VP1 region. The predominant CVB3 strains in China belonged to cluster D, whereas cluster E CVB3 might be circulated globally compared to other clusters. The average nucleotide substitution rate in the P1 region of CVB3 was 4.82 × 10–3 substitutions/site/year. Myocarditis was more common with cluster A. Clusters C and D presented more cases of acute flaccid paralysis, and cluster D may be more likely to cause HFMD. Multiple recombination events were detected among CVB3 variants, and there were twenty-three recombinant lineages of CVB3 circulating worldwide. Conclusions Overall, this study provides full-length genomic sequences of CVB3 isolates with a wide geographic distribution over a long-term time scale in China, which will be helpful for understanding the evolution of this pathogen. Simultaneously, continuous surveillance of CVB3 is indispensable to determine its genetic diversity in China as well as worldwide.

Published

2022

5. Genetic characterization and molecular epidemiology of Coxsackievirus A12 from mainland China during 2010–2019

Author

Qin Guo, Hehe Zhao, Yong Zhang, Xianjun Wang, Qiuli Yu, Zhaolin Tan, Huanhuan Lu, Jinbo Xiao, Tianjiao Ji, Shuangli Zhu, Dongyan Wang, Qian Yang, Zhenzhi Han, Wenbo Xu, and Dongmei Yan

Subjects

Coxsackievirus A12, phylogenetic analysis, evolutionary dynamics, recombination, hand, foot and mouth disease, Microbiology, QR1-502

Abstract

Coxsackievirus A12 (CVA12) is an enterovirus that has been isolated in many countries in recent years. However, studies on CVA12 are limited, and its effective population size, evolutionary dynamics and recombination patterns have not been clarified now. In this study, we described the phylogenetic characteristics of 16 CVA12 strains isolated from pediatric HFMD patients in mainland China from 2010 to 2019. Comparison of the nucleotide sequences and amino acid sequences with the CVA12 prototype strain revealed that the 16 CVA12 strains are identical in 78.8–79% and 94–94.2%, respectively. A phylodynamic analysis based on the 16 full-length VP1 sequences from this study and 21 sequences obtained from GenBank revealed a mean substitution rate of 6.61 × 10−3 substitutions/site/year (95% HPD: 5.16–8.20 × 10−3), dating the time to most recent common ancestor (tMRCA) of CVA12 back to 1946 (95% HPD: 1942–1947). The Bayesian skyline plot showed that the effective population size has experienced twice dynamic fluctuations since 2007. Phylogeographic analysis identified two significant migration pathways, indicating the existence of cross-provincial transmission of CVA12 in mainland China. Recombination analysis revealed two recombination patterns between 16 CVA12 strains and other EV-A, suggesting that there may be extensive genetic exchange between CVA12 and other enteroviruses. In summary, a total of 16 full-length CVA12 strains were reported in this study, providing valuable references for further studies of CVA12 worldwide.

Published

2022

6. Development of a real-time RT-PCR assay for the detection of pan-human parechoviruses

Author

Huanhuan Lu, Jinbo Xiao, Keyi Zhang, Zhenzhi Han, Yang Song, Dongyan Wang, Tianjiao Ji, Dongmei Yan, Shuangli Zhu, Wenbo Xu, and Yong Zhang

Subjects

Human parechoviruses, VP1 region, Real-time RT-PCR, Typing, Phylogenetics, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Parechoviruses (PeV-As), which constitute a new genus within the family Picornaviridae, have been associated with numerous localized outbreaks of serious diseases, such as coryza, pneumonia, maculopapular exanthem, and conjunctivitis. However, to the best of our knowledge, only a few laboratories worldwide conduct tests for the identification of this group of viruses. Therefore, in this study, we aimed to develop and validate a real-time RT-PCR assay for the identification of PeV-As. Methods To design and validate a real-time PCR primer–probe targeting the 5′-UTR region of PeV-As, the 5′-UTR sequences of PeV-As available in GenBank were aligned using the MUSCLE algorithm in MEGA v7.0. Thereafter, the highly conserved 5′-UTR region was selected, and its primer–probe sequence was designed using Primer Premier v5.0. This primer–probe sequence was then evaluated for specificity, sensitivity, and repeatability, and for its validation, it was tested using fecal samples from 728 healthy children living in Beijing (China). Results The PeV-A real-time RT-PCR assay detected only the RNA-positive standards of PeV-A genotypes (1–8, 14, 17, and 18), whereas 72 serotypes of non-PeV-A EV viruses were undetected. In addition, the VP1 region of these 11 PeV-A genotypes that tested positive were amplified using the primers designed in this study. Typing results indicated that eight, one, and two strains of the 11 were PeV-A1, PeV-A4, and PeV-A6, respectively. We also determined and presented the genetic characterization and phylogenetic analyses results corresponding to these 11 VP1 region sequences. Furthermore, real-time RT-PCR assay showed good sensitivity with LOD of 102 copies/μL. Positive results in eight parallel experiments at each concentration gradient from 107 copies/μL to 102 copies/μL, indicating good repeatability. Conclusion Our findings suggested that the real-time RT-PCR assay developed in this study can be applied for routine PeV-A identification. We detected PeV-A1, 4 and 6 genotypes in the 728 faecal samples using this method. Additionally, we believe that our results will serve as a foundation for further studies on PeV-As and facilitate the expansion of the gene sequence information available in GenBank.

Published

2021

7. Epidemiology of hand, foot, and mouth disease and the genetic characteristics of Coxsackievirus A16 in Taiyuan, Shanxi, China from 2010 to 2021

Author

Jiane Guo, Zijun Cao, Hongyan Liu, Jihong Xu, Lifeng Zhao, Li Gao, Zhihong Zuo, Yang Song, Zhenzhi Han, Yong Zhang, and Jitao Wang

Subjects

hand, foot, and mouth disease, epidemiology, Coxsackievirus A16, genetic characteristics, Microbiology, QR1-502

Abstract

Hand, foot, and mouth disease (HFMD) is a common childhood infectious disease caused by human enteroviruses (EV). This study aimed to describe the epidemiological features of HFMD and the genetic characteristics of Coxsackievirus A16 (CVA16) in Taiyuan, Shanxi, China, from 2010 to 2021. Descriptive epidemiological methods were used to analyze the time and population distribution of HFMD and the genetic characteristics of CVA16. Except being affected by the COVID-19 epidemic in 2020, HFMD epidemics were sporadic from January to March each year, and began to increase in April, with a major epidemic peak from May to August, which declined in September, followed by a secondary peak from October to December. The prevalence of EV infection was the highest in children aged one to five years (84.42%), whereas its incidence was very low in children under one year of age (5.48%). Enterovirus nucleic acid was detected by real-time reverse transcription polymerase chain reaction in 6641 clinical specimens collected from patients with HFMD from 2010 to 2021, and 4236 EV-positive specimens were detected, including 988 enterovirus A71 (EV-A71), 1488 CVA16, and 1760 other enteroviruses. CVA16 remains prevalent and has co-circulated with other EVs in Taiyuan from 2010 to 2021. A phylogenetic tree constructed based on the VP1 region showed that all CVA16 strains belonged to two different clades of the B1 genotype, B1a and B1b. They showed a nucleotide similarity of 86.5–100%, and an amino acid similarity of 96.9–100%. Overall, these findings add to the global genetic resources of CVA16, demonstrate the epidemiological characteristics of HFMD as well as the genetic features of CVA16 in Taiyuan City during 2010–2021, and provide supporting evidence for the prevention and control of HFMD.

Published

2022

8. Genomic Epidemiology and Phylodynamic Analysis of Enterovirus A71 Reveal Its Transmission Dynamics in Asia

Author

Jinbo Xiao, Keqiang Huang, Huanhuan Lu, Yang Song, Zhenzhi Han, Man Zhang, Jichen Li, Xiaofang Zhou, Jianhua Chen, Qiuli Yu, Ming Yang, Dongmei Yan, Tianjiao Ji, Qian Yang, Shuangli Zhu, Wenbo Xu, and Yong Zhang

Subjects

Bayesian phylodynamics, EV-A71, hand foot and mouth disease, phylogenetics, recombination, Microbiology, QR1-502

Abstract

ABSTRACT Enterovirus A71 (EV-A71) is one of the main pathogens causing hand, foot, and mouth disease (HFMD) outbreaks in Asian children under 5 years of age. In severe cases, it can cause neurological complications and be life-threatening. In this study, 200 newly sequenced EV-A71 whole-genome sequences were combined with 772 EV-A71 sequences from GenBank for large-scale analysis to investigate global EV-A71 epidemiology, phylogeny, and Bayesian phylodynamic characteristics. Based on the phylogenetic analysis of the EV-A71 3Dpol region, six new evolutionary lineages (lineages B, J, K, O, P, and Q) were found in this study, and the number of evolutionary lineages was expanded from 11 to 17. Temporal dynamics and recombination breakpoint analyses based on genotype C revealed that recombination of nonstructural protein-coding regions, including 3Dpol, is an important reason for the emergence of new lineages. The EV-A71 epidemic in the Asia-Pacific region is complex, and phylogeographic analysis found that Vietnam played a key role in the spread of subgenotypes B5 and C4. The origin of EV-A71 subgenotype C4 in China is East China, which is closely related to the prevalence of subgenotype C4 in the south and throughout China. Selection pressure analysis revealed that, in addition to VP1 amino acid residues VP1-98 and VP1-145, which are associated with EV-A71 pathogenicity, amino acid residues VP1-184 and VP1-249 were also positively selected, and their functions still need to be determined by biology and immunology. This study aimed to provide a solid theoretical basis for EV-A71-related disease surveillance and prevention, antiviral research, and vaccine development through a comprehensive analysis. IMPORTANCE EV-A71 is one of the most important pathogens causing HFMD outbreaks; however, large-scale studies of EV-A71 genomic epidemiology are currently lacking. In this study, 200 new EV-A71 whole-genome sequences were determined. Combining these with 772 EV-A71 whole-genome sequences in the GenBank database, the evolutionary and transmission characteristics of global and Asian EV-A71 were analyzed. Six new evolutionary lineages were identified in this study. We also found that recombination in nonstructural protein-coding regions, including 3Dpol, is an important cause for the emergence of new lineages. The results provided a solid theoretical basis for EV-A71-related disease surveillance and prevention, antiviral research, and vaccine development.

Published

2022

9. Highly diverse ribonucleic acid viruses in the viromes of eukaryotic host species in Yunnan province, China

Author

Zhenzhi Han, Jinbo Xiao, Yang Song, Xiaonan Zhao, Qiang Sun, Huanhuan Lu, Keyi Zhang, Jichen Li, Junhan Li, Fenfen Si, Guoyan Zhang, Hehe Zhao, Senquan Jia, Jienan Zhou, Dongyan Wang, Shuangli Zhu, Dongmei Yan, Wenbo Xu, Xiaoqing Fu, and Yong Zhang

Subjects

metagenomic next-generation sequencing (mNGS), virome, RNA viruses, picornavirus, coronavirus, viral evolution, Microbiology, QR1-502

Abstract

BackgroundThe diversity in currently documented viruses and their morphological characteristics indicates the need for understanding the evolutionary characteristics of viruses. Notably, further studies are needed to obtain a comprehensive landscape of virome, the virome of host species in Yunnan province, China.Materials and methodsWe implemented the metagenomic next-generation sequencing strategy to investigate the viral diversity, which involved in 465 specimens collected from bats, pangolins, monkeys, and other species. The diverse RNA viruses were analyzed, especially focusing on the genome organization, genetic divergence and phylogenetic relationships.ResultsIn this study, we investigated the viral composition of eight libraries from bats, pangolins, monkeys, and other species, and found several diverse RNA viruses, including the Alphacoronavirus from bat specimens. By characterizing the genome organization, genetic divergence, and phylogenetic relationships, we identified five Alphacoronavirus strains, which shared phylogenetic association with Bat-CoV-HKU8-related strains. The pestivirus-like virus related to recently identified Dongyang pangolin virus (DYPV) strains from dead pangolin specimens, suggesting that these viruses are evolving. Some genomes showed higher divergence from known species (e.g., calicivirus CS9-Cali-YN-CHN-2020), and many showed evidence of recombination events with unknown or known strains (e.g., mamastroviruses BF2-astro-YN-CHN-2020 and EV-A122 AKM5-YN-CHN-2020). The newly identified viruses showed extensive changes and could be assigned as new species, or even genus (e.g., calicivirus CS9-Cali-YN-CHN-2020 and iflavirus Ifla-YN-CHN-2020). Moreover, we identified several highly divergent RNA viruses and estimated their evolutionary characteristics among different hosts, providing data for further examination of their evolutionary dynamics.ConclusionOverall, our study emphasizes the close association between emerging viruses and infectious diseases, and the need for more comprehensive surveys.

Published

2022

10. Temporal phylogeny and molecular characterization of echovirus 30 associated with aseptic meningitis outbreaks in China

Author

Xiaoling Tian, Zhenzhi Han, Yulong He, Qiang Sun, Wenrui Wang, Wenbo Xu, Hongying Li, and Yong Zhang

Subjects

Echovirus 30 (E30), Molecular epidemiology, Phylodynamics, Aseptic meningitis, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background An outbreak of aseptic meningitis occurred from June to August 2016, in Inner Mongolia Autonomous Region, China. Methods To determine its epidemiological characteristics, etiologic agent, and possible origin, specimens were collected for virus isolation and identification, followed by molecular epidemiological analysis. Results A total of 363 patients were clinically diagnosed from June 1st to August 31st 2016, and most cases (63.1%, n = 229) were identified between June 22nd and July 17th, with children aged 6 to 12 years constituting the highest percentage (68.9%, n = 250). All viral isolates from this study belonged to genotype C of echovirus 30 (E30), which dominated transmission in China. To date, two E30 transmission lineages have been identified in China, of which Lineage 2 was predominant. We observed fluctuant progress of E30 genetic diversity, with Lineage 2 contributing to increased genetic diversity after 2002, whereas Lineage 1 was significant for the genetic diversity of E30 before 2002. Conclusions We identified the epidemiological and etiological causes of an aseptic meningitis outbreak in Inner Mongolia in 2016, and found that Lineage 2 played an important role in recent outbreaks. Moreover, we found that Gansu province could play an important role in E30 spread and might be a possible origin site. Furthermore, Fujian, Shandong, Taiwan, and Zhejiang provinces also demonstrated significant involvement in E30 evolution and persistence over time in China.

Published

2021

11. Genetic Evolution and Variation of Human Adenovirus Serotype 31 Epidemic Strains in Beijing, China, during 2010–2022

Author

Liying Liu, Yuan Qian, Zhenzhi Han, Liping Jia, Huijin Dong, Linqing Zhao, and Runan Zhu

Subjects

human adenovirus 31, diarrhea, molecular revolution, genetic diversity, children, Microbiology, QR1-502

Abstract

Human adenovirus serotype 31 (HAdV-31) is closely associated with gastroenteritis in children and can cause fatal systemic disseminated diseases in immunocompromised patients. The lack of genomic data for HAdV-31, especially in China, will greatly limit research on its prevention and control. Sequencing and bioinformatics analyses were performed for HAdV-31 strains from diarrheal children in Beijing, China, during 2010–2022. Three capsid protein genes (hexon, penton, and fiber) were obtained in 37 cases, including one in which the whole genome was sequenced. HAdV-31 strains clustered into three distinct clades (I–III) in a phylogenetic tree constructed based on concatenated genes and the whole genome; the endemic strains only gathered into clade II, and most of the reference strains clustered into clade I. Compared with penton and hexon, fiber had a faster evolutionary rate (1.32 × 10−4 substitutions/site/year), an earlier divergence time (1697), lower homology (98.32–100% at the amino acid level), and greater genetic variation (0.0032). Four out of the six predicted positive selection pressure codons were also in the knob of fiber. These results reveal the molecular evolution characteristics and variations of HAdV-31 in Beijing, and fiber may be one of the main evolution driving forces.

Published

2023

12. A novel interspecies recombinant enterovirus (Enterovirus A120) isolated from a case of acute flaccid paralysis in China

Author

Huanhuan Lu, Mei Hong, Yong Zhang, Jinbo Xiao, Man Zhang, Keyi Zhang, Yang Song, Zhenzhi Han, Qian Yang, Dongyan Wang, Dongmei Yan, Shuangli Zhu, and Wenbo Xu

Subjects

EV-A120, genomic characterization, phylogenetic analysis, recombinant analysis, seroepidemiology, temperature sensitivity, Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502

Abstract

ABSTRACTEV-A120 is a recently identified serotype of the enterovirus A species. Only one full-length genomic sequence is currently available in GenBank, and very few studies have been conducted on EV-A120 globally. Thus, additional information and research on EV-A120 are needed to explore its genetic characteristics, phylogeny, and relationship with enteroviral disease. In this study, we report the phylogenetic characteristics of a EV-A120 strain (Q0082/XZ/CHN/2000) from Tibet, China. The amino acid sequence similarity and nucleotide sequence similarity of the full-length genomic sequence of this EV-A120 strain and the EV-A120 prototype strain were 96.3% and 79.9%, respectively, showing an evolutionary trend. Recombination analysis found intraspecies recombination in the 5′ -UTR, 2B, 2C, and 3D regions. Serum neutralization testing of the EV-A120 (Q0082) strain was also carried out. Low serum-positive rates and geometric mean titres (GMTs) indicated that the extent of EV-A120 transmission and exposure in the population was very limited compared with that in the outbreaks of EV-A71 and CV-A16 in China since 2008. The EV-A120 strain (Q0082) is non-temperature sensitive, indicating its potential to spread in the population. In summary, this study reports the full-length genomic sequence of EV-A120 and provides important information for its global molecular epidemiology.

Published

2020

13. Genomic Epidemiology and Transmission Dynamics of Global Coxsackievirus B4

Author

Jinbo Xiao, Jianxing Wang, Huanhuan Lu, Yang Song, Dapeng Sun, Zhenzhi Han, Jichen Li, Qian Yang, Dongmei Yan, Shuangli Zhu, Yaowen Pei, Xianjun Wang, Wenbo Xu, and Yong Zhang

Subjects

Coxsackievirus B4, hand, foot, and mouth disease, phylogenetics, recombination, transmission dynamics, Microbiology, QR1-502

Abstract

The aim of this study was to determine the global genetic diversity and transmission dynamics of coxsackievirus B4 (CVB4) and to propose future directions for disease surveillance. Next-generation sequencing was performed to obtain the complete genome sequence of CVB4, and the genetic diversity and transmission dynamics of CVB4 worldwide were analyzed using bioinformatics methods such as phylogenetic analysis, evolutionary dynamics, and phylogeographic analysis. Forty complete genomes of CVB4 were identified from asymptomatic infected individuals and hand, foot, and mouth disease (HFMD) patients. Frequent recombination between CVB4 and EV-B multiple serotypes in the 3Dpol region was found and formed 12 recombinant patterns (A-L). Among these, the CVB4 isolated from asymptomatic infected persons and HFMD patients belonged to lineages H and I, respectively. Transmission dynamics analysis based on the VP1 region revealed that CVB4 epidemics in countries outside China were dominated by the D genotype, whereas the E genotype was dominant in China, and both genotypes evolved at a rate of > 6.50 × 10−3 substitutions/site/year. CVB4 spreads through the population unseen, with the risk of disease outbreaks persisting as susceptible individuals accumulate. Our findings add to publicly available CVB4 genomic sequence data and deepen our understanding of CVB4 molecular epidemiology.

Published

2023

14. Molecular Characteristics and Genetic Evolution of Echovirus 33 in Mainland of China

Author

Wenhui Wang, Huan Fan, Shuaifeng Zhou, Shikang Li, Alitengsaier NIGEDELI, Yong Zhang, Qiang Sun, Yun He, Qin Guo, Xiaoyi Wang, Huanhuan Lu, Jinbo Xiao, Hehe Zhao, Zhenzhi Han, Tianjiao Ji, Le Zhang, and Dongmei Yan

Subjects

echovirus 33, recombinant analysis, genomic characterization, phyletic evolution, spatial transmission, Medicine

Abstract

Echovirus, a member of the Enterovirus B (EV-B) family, has led to numerous outbreaks and pandemics, causing a broad spectrum of diseases. Based on the national hand, foot, and mouth disease (HFMD) surveillance system, seven strains of echovirus 33 (E33) were isolated from Mainland of China between 2010 and 2018. The whole genomes of these strains were isolated and sequenced, and phylogenetic trees were constructed based on the gene sequences in different regions of the EV-B prototype strains. It was found that E33 may be recombined in the P2 and P3 regions. Five genotypes (A–E) were defined based on the entire VP1 region of E33, of which the C gene subtype was the dominant gene subtype at present. Recombinant analysis showed that genotype C strains likely recombined with EV-B80, EV-B85, E13, and CVA9 in the P2 and P3 regions, while genotype E had the possibility of recombination with CVB3, E3, E6, and E4. Results of Bayesian analysis indicated that E33 may have appeared around 1955 (95% confidence interval: 1945–1959), with a high evolutionary rate of 1.11 × 10−2 substitution/site/year (95% highest posterior density (HPD): 8.17 × 10−3 to 1.4 × 10−2 substitution/site/year). According to spatial transmission route analysis, two significant transmission routes were identified: from Australia to India and from Oman to Thailand, which the E33 strain in Mainland of China likely introduced from Mexico and India. In conclusion, our study fills the gaps in the evolutionary analysis of E33 and can provide important data for enterovirus surveillance.

Published

2022

15. Two Coxsackievirus B3 outbreaks associated with hand, foot, and mouth disease in China and the evolutionary history worldwide

Author

Zhenzhi Han, Yong Zhang, Keqiang Huang, Jianxing Wang, Huifang Tian, Yang Song, Qian Yang, Dongmei Yan, Shuangli Zhu, Mingxiao Yao, Xianjun Wang, and Wenbo Xu

Subjects

Enterovirus, CV-B3, Molecular epidemiology, HFMD, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Coxsackievirus B3 (CV-B3) is usually associated with aseptic meningitis and myocarditis; however, the association between CV-B3 and hand, foot, and mouth disease (HFMD) has not been clearly demonstrated, and the phylogenetic dynamics and transmission history of CV-B3 have not been well summarized. Method Two HFMD outbreaks caused by CV-B3 were described in Hebei Province in 2012 and in Shandong Province in 2016 in China. To analyze the epidemiological features of two CV-B3 outbreaks, a retrospective analysis was conducted. All clinical specimens from CV-B3 outbreaks were collected and disposed according to the standard procedures supported by the WHO Global Poliovirus Specialized Laboratory. EV genotyping and phylogenetic analysis were performed to illustrate the genetic characteristics of CV-B3 in China and worldwide. Results Two transmissible lineages (lineage 2 and 3) were observed in Northern China, which acted as an important “reservoir” for the transmission of CV-B3. Sporadic exporting and importing of cases were observed in almost all regions. In addition, the global sequences of CV-B3 showed a tendency of geographic-specific clustering, indicating that geographic-driven adaptation plays a major role in the diversification and evolution of CV-B3. Conclusions Overall, our study indicated that CV-B3 is a causative agent of HFMD outbreak and revealed the phylogenetic dynamics of CV-B3 worldwide, as well as provided an insight on CV-B3 outbreaks for effective intervention and countermeasures.

Published

2019

16. Molecular Epidemiological, Serological, and Pathogenic Analysis of EV-B75 Associated With Acute Flaccid Paralysis Cases in Tibet, China

Author

Keyi Zhang, Mei Hong, Yong Zhang, Zhenzhi Han, Jinbo Xiao, Huanhuan Lu, Yang Song, Dongmei Yan, Dongyan Wang, Shuangli Zhu, Wenbo Xu, and Guizhen Wu

Subjects

enterovirus B75, seroprevalence, temperature sensitivity, Tibet, phylogenetic analyses, Microbiology, QR1-502

Abstract

Enterovirus B75 (EV-B75) is a newly identified serotype of the enterovirus B species. To date, only 112 cases related to EV-B75 have been reported worldwide, and research on EV-B75 is still limited with only two full-length genome sequences available in GenBank. The present study reported seven EV-B75 sequences from a child with acute flaccid paralysis and six asymptomatic close contacts in Shigatse, Tibet. Phylogenetic analysis revealed that the Tibetan strain was possibly imported from neighboring India. Seroepidemiological analyses indicated that EV-B75 has not yet caused a large-scale epidemic in Tibet. Similarity plots and boot scanning analyses revealed frequent intertypic recombination in the non-structural region of all seven Tibet EV-B75 strains. All seven Tibetan strains were temperature-sensitive, suggesting their poor transmissibility in the environment. Overall, though the seven Tibetan strains did not cause large-scale infection, prevention and control of the novel enterovirus cannot be underestimated.

Published

2021

17. Molecular Epidemiology and Evolution of Coxsackievirus A9

Author

Hehe Zhao, Jianxing Wang, Jianhua Chen, Ruifang Huang, Yong Zhang, Jinbo Xiao, Yang Song, Tianjiao Ji, Qian Yang, Shuangli Zhu, Dongyan Wang, Huanhuan Lu, Zhenzhi Han, Guoyan Zhang, Jichen Li, and Dongmei Yan

Subjects

coxsackievirus A9, genotyping, recombination, evolutionary reconstruction, Microbiology, QR1-502

Abstract

Nineteen CVA9 isolates were obtained between 2010 and 2019 from six provinces of mainland China, using the HFMD surveillance network established in China. Nucleotide sequencing revealed that the full-length VP1 of 19 CVA9 isolates was 906 bases encoding 302 amino acids. The combination of the thresholds of the phylogenetic tree and nucleotide divergence of different genotypes within the same serotype led to a value of 15–25%, and enabled CVA9 worldwide to be categorized into ten genotypes: A–J. The phylogenetic tree showed that the prototype strain was included in genotype A, and that the B, C, D, E, H, and J genotypes disappeared during virus evolution, whereas the F, I, and G genotypes showed co-circulation. Lineage G was the dominant genotype of CVA9 and included most of the strains from nine countries in Asia, North America, Oceania, and Europe. Most Chinese strains belonged to the G genotype, suggesting that the molecular epidemiology of China is consistent with that observed worldwide. The 165 partial VP1 strains (723 nt) showed a mean substitution rate of 3.27 × 10−3 substitution/site/year (95% HPD range 2.93–3.6 × 10−3), dating the tMRCA of CVA9 back to approximately 1922 (1911–1932). The spatiotemporal dynamics of CVA9 showed the spread of CVA9 obviously increased in recent years. Most CVA9 isolates originated in USA, but the epidemic areas of CVA9 are now concentrated in the Asia–Pacific region, European countries, and North America. Recombination analysis within the enterovirus B specie (59 serotypes) revealed eight recombination patterns in China at present, CVB4, CVB5, E30, CVB2, E11, HEV106, HEV85, and HEV75. E14, and E6 may act as recombinant donors in multiple regions. Comparison of temperature sensitivity revealed that temperature-insensitive strains have more amino acid substitutions in the RGD motif of the VP1 region, and the sites T283S, V284M, and R288K in the VP1 region may be related to the temperature tolerance of CVA9.

Published

2022

18. Global Spread of the B5 Subgenotype EV-A71 and the Phylogeographical Analysis of Chinese Migration Events

Author

Keqiang Huang, Yong Zhang, Zhenzhi Han, Xiaofang Zhou, Yang Song, Dongyan Wang, Shuangli Zhu, Dongmei Yan, Wen Xu, and Wenbo Xu

Subjects

B5 subgenotype, enterovirus A71, molecular evolution, migration, phylogeographical analysis, Microbiology, QR1-502

Abstract

The subgenotype B5 of EV-A71 is a widely circulating subgenotype that frequently spreads across the globe. Several outbreaks have occurred in nations, such as Malaysia, Thailand, Vietnam, and Japan. Appearing first in Taiwan, China, the subgenotype has been frequently reported in mainland of China even though no outbreaks have been reported so far. The current study reconstructed the migration of the B5 subgenotype of EV-A71 in China via phylogeographical analysis. Furthermore, we investigated its population dynamics in order to draw more credible inferences. Following a dataset cleanup of B5 subgenotype of EV-A71, we detected earlier B5 subgenotypes of EV-A71 sequences that had been circulating in Malaysia and Singapore since the year 2000, which was before the 2003 outbreak that occurred in Sarawak. The Bayesian inference indicated that the most recent common ancestor of B5 subgenotype EV-A71 appeared in September, 1994 (1994.75). With respect to the overall prevalence, geographical reconstruction revealed that the B5 subgenotype EV-A71 originated singly from single-source cluster and subsequently developed several active lineages. Based on a large amount of data that was accumulated, we conclude that the appearance of the B5 subgenotype of EV-A71 in mainland of China was mainly due to multiple migrations from different origins.

Published

2020

19. A Large-Scale Outbreak of Echovirus 30 in Gansu Province of China in 2015 and Its Phylodynamic Characterization

Author

Jianhua Chen, Zhenzhi Han, Haizhuo Wu, Wenbo Xu, Deshan Yu, and Yong Zhang

Subjects

echovirus 30 (E-30), phylogenetic analysis, molecular epidemiology, phylodynamics, encephalitis, Microbiology, QR1-502

Abstract

BackgroundEchovirus 30 (E-30) has been investigated and reported worldwide and is closely associated with several infectious diseases, including encephalitis; myocarditis; and hand, foot, and mouth disease. Although many E-30 outbreaks associated with encephalitis have been reported around the world, it was not reported in northwest China until 2015.MethodsThe clinical samples, including the feces, serum, throat swabs, and cerebrospinal fluid, were collected for this study and were analyzed for diagnosis. E-30 was isolated and processed according to the standard procedures. The epidemiological and phylogenetic analysis were performed to indicate the characteristics of E-30 outbreaks and phylodynamics of E-30 in China.ResultsThe E-30 outbreaks affected nine towns of Gansu Province in 2015, starting at a school of Nancha town and spreading to other towns within 1 month. The epidemiological features showed that children aged 6–15 years were more susceptible to E-30 infection. The genotypes B and C cocirculated in the world, whereas the latter dominated the circulation of E-30 in China. The genome sequences of this outbreak present 99.3–100% similarity among these strains, indicating a genetic-linked aggregate outbreak of E-30 in this study. Two larger genetic diversity expansions and three small fluctuations of E-30 were observed from 1987 to 2016 in China, which revealed the oscillating patterns of E-30 in China. In addition, the coastal provinces of China, such as Zhejiang, Fujian, and Shandong, were initially infected, followed by other parts of the country. The E-30 strains isolated from mainland of China may have originated from Taiwan of China in the last century.ConclusionThe highly similar E-30 genomes in this outbreak showed an aggregate outbreak of E-30, with nine towns affected. Our results suggested that, although the genetic diversity of E-30 oscillates, the dominant lineages of E-30 in China has complex genetic transmission. The coastal provinces played an important role in E-30 spread, which implied further development of effective countermeasures. This study provides a further insight into the E-30 outbreak and transmission and illustrates the importance of valuable surveillance in the future.

Published

2020

20. Molecular typing and characterization of a novel genotype of EV-B93 isolated from Tibet, China.

Author

Man Zhang, Yong Zhang, Mei Hong, Jinbo Xiao, Zhenzhi Han, Yang Song, Shuangli Zhu, Dongmei Yan, Qian Yang, Wenbo Xu, and Zhijun Liu

Subjects

Medicine, Science

Abstract

EV-B93 is a novel serotype within the Enterovirus B species and is uncommon worldwide. Currently, only one full-length genomic sequence (the prototype strain) has been deposited in the GenBank database. In this study, three EV-B93 were identified, including one from an acute flaccid paralysis (AFP) patient (named 99052/XZ/CHN/1999, hereafter XZ99052) and two from healthy children (named 99096/XZ/CHN/1999 and 99167/XZ/CHN/1999, hereafter XZ99096 and XZ99167, respectively) from Tibet in 1999 during the polio eradication program. The identity between the nucleotide and amino acid sequences of the Tibet EV-B93 strain and the EV-B93 prototype strain is 83.2%-83.4% and 96.8%-96.9%, respectively. The Tibet EV-B93 strain was found to have greater nucleotide sequence identity in the P3 region to another enterovirus EV-B107 as per a phylogenetic tree analysis, which revealed that recombination occurred. Seroepidemiology data showed that EV-B93 has not produced an epidemic in Tibet and there may be susceptible individuals. The three Tibet EV-B93 strains are temperature-resistant with prognosticative virulence, suggesting the possibility of a potential large-scale outbreak of EV-B93. The analyzed EV-B93 strains enrich our knowledge about this serotype and provide valuable information on global EV-B93 molecular epidemiology. What is more, they permit the appraisal of the serotype's potential public health impact and aid in understanding the role of recombination events in the evolution of enteroviruses.

Published

2020

21. Genetic characterization and molecular epidemiological analysis of novel enterovirus EV-B80 in China

Author

Zhenzhi Han, Yong Zhang, Keqiang Huang, Hui Cui, Mei Hong, Haishu Tang, Yang Song, Qian Yang, Shuangli Zhu, Dongmei Yan, and Wenbo Xu

Subjects

Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502

Abstract

Abstract Enterovirus B80 (EV-B80) is a newly identified serotype belonging to the enterovirus B species. To date, only two full-length genomic sequences of EV-B80 are available in GenBank, and few studies on EV-B80 have been conducted in China or worldwide. More information and research on EV-B80 is needed to assess its genetic characteristics, phylogenetic relationships, and association with enteroviral diseases. In this study, we report the phylogenetic characteristics of three Xinjiang EV-B80 strains and one Tibet EV-B80 strain in China. The full-length genomic sequences of four strains show 78.8–79% nucleotide identity and 94–94.2% amino acid identity with the prototype of EV-B80, indicating a tendency for evolution. Based on a maximum likelihood phylogenetic tree based on the entire VP1 region, three genotypes (A–C) were defined, revealing the possible origin of EV-B80 strains in the mainland of China. Recombination analysis revealed intraspecies recombinations in all four EV-B80 strains in nonstructural regions along with two recombination patterns. Due to the geographic factor, the coevolution of EV-B strains formed two different patterns of circulation. An antibody seroprevalence study against EV-B80 in two Xinjiang prefectures also showed that EV-B80 strains were widely prevalent in Xinjiang, China, compared to other studies on EV-B106 and EV-B89. All four EV-B80 strains are not temperature sensitive, showing a higher transmissibility in the population. In summary, this study reports the full-length genomic sequences of EV-B80 and provides valuable information on global EV-B80 molecular epidemiology.

Published

2018

22. The Husavirus Posa-Like Viruses in China, and a New Group of Picornavirales

Author

Zhenzhi Han, Jinbo Xiao, Yang Song, Mei Hong, Guolong Dai, Huanhuan Lu, Man Zhang, Yueling Liang, Dongmei Yan, Shuangli Zhu, Wenbo Xu, and Yong Zhang

Subjects

husavirus, posa-like virus, Picornavirales, phylogeny, evolution, Microbiology, QR1-502

Abstract

Novel posa-like viral genomes were first identified in swine fecal samples using metagenomics and were designated as unclassified viruses in the order Picornavirales. In the present study, nine husavirus strains were identified in China. Their genomes share 94.1–99.9% similarity, and alignment of these nine husavirus strains identified 697 nucleotide polymorphism sites across their full-length genomes. These nine strains were directly clustered with the Husavirus 1 lineage, and their genomic arrangement showed similar characteristics. These posa-like viruses have undergone a complex evolutionary process, and have a wide geographic distribution, complex host spectrum, deep phylogenetic divergence, and diverse genomic organizations. The clade of posa-like viruses forms a single group, which is evolutionarily distinct from other known families and could represent a distinct family within the Picornavirales. The genomic arrangement of Picornavirales and the new posa-like viruses are different, whereas the posa-like viruses have genomic modules similar to the families Dicistroviridae and Marnaviridae. The present study provides valuable genetic evidence of husaviruses in China, and clarifies the phylogenetic dynamics and the evolutionary characteristics of Picornavirales.

Published

2020

23. Genetic Diversity Analysis of Coxsackievirus A8 Circulating in China and Worldwide Reveals a Highly Divergent Genotype

Author

Yang Song, Dongyan Wang, Yong Zhang, Zhenzhi Han, Jinbo Xiao, Huanhuan Lu, Dongmei Yan, Tianjiao Ji, Qian Yang, Shuangli Zhu, and Wenbo Xu

Subjects

coxsackievirus A8, emerging diseases, evolutionary dynamics, genetic diversity, hand, foot, Microbiology, QR1-502

Abstract

Coxsackievirus A8 (CV-A8) is one of the pathogens associated with hand, foot and mouth disease (HFMD) and herpangina (HA), occasionally leading to severe neurological disorders such as acute flaccid paralysis (AFP). Only one study aimed at CV-A8 has been published to date, and only 12 whole-genome sequences are publicly available. In this study, complete genome sequences from 11 CV-A8 strains isolated from HFMD patients in extensive regions from China between 2013 and 2018 were determined, and all sequences from GenBank were retrieved. A phylogenetic analysis based on a total of 34 complete VP1 sequences of CV-A8 revealed five genotypes: A, B, C, D and E. The newly emerging genotype E presented a highly phylogenetic divergence compared with the other genotypes and was composed of the majority of the strains sequenced in this study. Markov chain Monte Carlo (MCMC) analysis revealed that genotype E has been evolving for nearly a century and somehow arose in approximately 2010. The Bayesian skyline plot showed that the population size of CV-A8 has experienced three dynamic fluctuations since 2001. Amino acid residues of VP1100N, 103Y, 240T and 241V, which were embedded in the potential capsid loops of genotype E, might enhance genotype E adaption to the human hosts. The CV-A8 whole genomes displayed significant intra-genotypic genetic diversity in the non-capsid region, and a total of six recombinant lineages were detected. The Chinese viruses from genotype E might have emerged recently from recombining with European CV-A6 strains. CV-A8 is a less important HFMD pathogen, and the capsid gene diversity and non-capsid recombination variety observed in CV-A8 strains indicated that the constant generation of deleterious genomes and a constant selection pressure against these deleterious mutations is still ongoing within CV-A8 quasispecies. It is possible that CV-A8 could become an important pathogen in the HFMD spectrum in the future. Further surveillance of CV-A8 is greatly needed.

Published

2020

24. Importation and circulation of rubella virus lineages 1E-L2 and 2B-L2c between 2018 and 2021 in China: Virus evolution and spatial–temporal transmission characteristics

Author

Ying Liu, Zhenzhi Han, Chuyun Kang, Aili Cui, Yan Zhang, Li Liu, Ying Chen, Lili Deng, Hua Zhao, Jun Zhou, Fangcai Li, Shujie Zhou, Daxing Feng, Xiaoling Tian, Yan Feng, Xiaoxian Cui, Yue Lei, Yan Wang, Fang Yuan, Lixia Fan, Xiaomin Tang, Meng Chen, Xiaofang Peng, Yu Guo, Hui Gao, Suting Wang, Liqun Li, Ting Zhang, Xiuying Deng, Haiyun Chen, Shuang Wang, Yu Ma, Zhen Zhu, and Wenbo Xu

Subjects

Virology, Microbiology

Abstract

To better understand the importation and circulation patterns of rubella virus lineages 1E-L2 and 2B-L2c circulating in China since 2018, 3,312 viral strains collected from 27 out of 31 provinces in China between 2018 and 2021 were sequenced and analyzed with the representative international strains of lineages 1E-L2 and 2B-L2c based on genotyping region. Time-scale phylogenetic analysis revealed that the global lineages 1E-L2 and 2B-L2c presented distinct evolutionary patterns. Lineage 1E-L2 circulated in relatively limited geographical areas (mainly Asia) and showed geographical and temporal clustering, while lineage 2B-L2c strains circulated widely throughout the world and exhibited a complicated topology with several independently evolved branches. Furthermore, both lineages showed extensive international transmission activities, and phylogeographic inference provided evidence that lineage 1E-L2 strains circulating in China possibly originated from Japan, while the source of lineage 2B-L2c isolated since 2018 is still unclear. After importation into China in 2018, the spread of lineage 1E-L2 presented a three-stage transmission pattern from southern to northern China, whereas lineage 2B-L2c spread from a single point in western China to all the other four regions. These two transmission patterns allowed both imported lineages to spread rapidly across China during the 2018–9 rubella epidemic and eventually established endemic circulations. This study provides critical scientific data for rubella control and elimination in China and worldwide.

Published

2022

25. Pathological Characteristics of Echovirus 30 Infection in a Mouse Model

Author

Jichen Li, Guoyan Zhang, Qiang Sun, Keyi Zhang, Huanhuan Lu, Jinbo Xiao, Zhenzhi Han, Hehe Zhao, Wenbo Xu, Yong Zhang, and Zhijun Liu

Subjects

Mice, Knockout, Immunology, Echovirus Infections, Glioma, Sequence Analysis, DNA, Microbiology, Enterovirus B, Human, Disease Models, Animal, Mice, Cell Line, Tumor, Virology, Insect Science, Pathogenesis and Immunity, Animals, Humans, RNA, Viral, Meningitis, Aseptic, Phylogeny

Abstract

Echovirus 30 (E30), a member of species B enterovirus, is associated with outbreaks of aseptic meningitis and has become a global health emergency. However, the pathogenesis of E30 remains poorly understood due to the lack of appropriate animal models. In this study, we established a mouse infection model to explore the pathogenicity of E30. The 2-day-old IFNAR(−/−) mice infected with E30 strain WZ16 showed lethargy and paralysis, and some died. Obvious pathological changes were observed in the skeletal muscle, brain tissue, and other tissues, with the highest viral load in the skeletal muscles. Transcriptome analysis of brain and skeletal muscle tissues from infected mice showed that significant differentially expressed genes were enriched in complement response and neuropathy-related pathways. Using immunofluorescence assay, we found that the viral double-stranded RNA (dsRNA) was detected in the mouse brain region and could infect human glioma (U251) cells. These results indicated that E30 affects the nervous system, and they provide a theoretical basis for understanding its pathogenesis. IMPORTANCE Echovirus 30 (E30) infection causes a wide spectrum of diseases with mild symptoms, such as hand, foot, and mouth disease (HFMD), acute flaccid paralysis, and aseptic meningitis and other diseases, especially one of the most common pathogens causing aseptic meningitis outbreaks. We established a novel mouse model of E30 infection by inoculating neonatal mice with clinical isolates of E30 and observed the pathological changes induced by E30. Using the E30 infection model, we found complement responses and neuropathy-related genes in the mice tissues at the transcriptome level. Moreover, we found that the viral dsRNA localized in the mouse brain and could replicate in human glioma cell line U251 rather than in the neuroblastoma cell line, SK-N-SH.

Published

2022

26. A novel interspecies recombinant enterovirus (Enterovirus A120) isolated from a case of acute flaccid paralysis in China

Author

Yong Zhang, Wenbo Xu, Qian Yang, Jinbo Xiao, Zhenzhi Han, Yang Song, Dongyan Wang, Shuangli Zhu, Man Zhang, Mei Hong, Keyi Zhang, Dongmei Yan, and Huanhuan Lu

Subjects

Male, temperature sensitivity, 0301 basic medicine, Epidemiology, Antibodies, Viral, Tibet, medicine.disease_cause, Drug Discovery, Peptide sequence, Genetics, education.field_of_study, Phylogenetic tree, Strain (biology), recombinant analysis, Nucleic acid sequence, Neuromuscular Diseases, Articles, genomic characterization, General Medicine, Myelitis, Infectious Diseases, Child, Preschool, GenBank, RNA, Viral, EV-A120, seroepidemiology, Research Article, 030106 microbiology, Immunology, Population, Genome, Viral, Biology, Microbiology, 03 medical and health sciences, Cell Line, Tumor, Virology, Enterovirus Infections, medicine, Humans, Amino Acid Sequence, education, Molecular epidemiology, Sequence Analysis, RNA, phylogenetic analysis, Antibodies, Neutralizing, Enterovirus A, Human, Molecular Typing, 030104 developmental biology, Central Nervous System Viral Diseases, Enterovirus, Parasitology

Abstract

EV-A120 is a recently identified serotype of the enterovirus A species. Only one full-length genomic sequence is currently available in GenBank, and very few studies have been conducted on EV-A120 globally. Thus, additional information and research on EV-A120 are needed to explore its genetic characteristics, phylogeny, and relationship with enteroviral disease. In this study, we report the phylogenetic characteristics of a EV-A120 strain (Q0082/XZ/CHN/2000) from Tibet, China. The amino acid sequence similarity and nucleotide sequence similarity of the full-length genomic sequence of this EV-A120 strain and the EV-A120 prototype strain were 96.3% and 79.9%, respectively, showing an evolutionary trend. Recombination analysis found intraspecies recombination in the 5′ -UTR, 2B, 2C, and 3D regions. Serum neutralization testing of the EV-A120 (Q0082) strain was also carried out. Low serum-positive rates and geometric mean titres (GMTs) indicated that the extent of EV-A120 transmission and exposure in the population was very limited compared with that in the outbreaks of EV-A71 and CV-A16 in China since 2008. The EV-A120 strain (Q0082) is non-temperature sensitive, indicating its potential to spread in the population. In summary, this study reports the full-length genomic sequence of EV-A120 and provides important information for its global molecular epidemiology.

Published

2020

27. Temporal phylogeny and molecular characterization of echovirus 30 associated with aseptic meningitis outbreaks in China

Author

Wenbo Xu, Qiang Sun, Yong Zhang, Yulong He, Zhenzhi Han, Wenrui Wang, Xiaoling Tian, and Hongying Li

Subjects

0301 basic medicine, China, Lineage (genetic), Echovirus, Echovirus 30 (E30), 030106 microbiology, Echovirus Infections, Infectious and parasitic diseases, RC109-216, Biology, medicine.disease_cause, Disease Outbreaks, 03 medical and health sciences, Aseptic meningitis, Virology, Genotype, medicine, Humans, Meningitis, Aseptic, Child, Phylogeny, Genetic diversity, Molecular epidemiology, Research, Outbreak, medicine.disease, Phylodynamics, Enterovirus B, Human, 030104 developmental biology, Infectious Diseases, Viral phylodynamics

Abstract

Background An outbreak of aseptic meningitis occurred from June to August 2016, in Inner Mongolia Autonomous Region, China. Methods To determine its epidemiological characteristics, etiologic agent, and possible origin, specimens were collected for virus isolation and identification, followed by molecular epidemiological analysis. Results A total of 363 patients were clinically diagnosed from June 1st to August 31st 2016, and most cases (63.1%, n = 229) were identified between June 22nd and July 17th, with children aged 6 to 12 years constituting the highest percentage (68.9%, n = 250). All viral isolates from this study belonged to genotype C of echovirus 30 (E30), which dominated transmission in China. To date, two E30 transmission lineages have been identified in China, of which Lineage 2 was predominant. We observed fluctuant progress of E30 genetic diversity, with Lineage 2 contributing to increased genetic diversity after 2002, whereas Lineage 1 was significant for the genetic diversity of E30 before 2002. Conclusions We identified the epidemiological and etiological causes of an aseptic meningitis outbreak in Inner Mongolia in 2016, and found that Lineage 2 played an important role in recent outbreaks. Moreover, we found that Gansu province could play an important role in E30 spread and might be a possible origin site. Furthermore, Fujian, Shandong, Taiwan, and Zhejiang provinces also demonstrated significant involvement in E30 evolution and persistence over time in China.

Published

2021

28. Coxsackievirus B4: a Undervalued Pathogen that Associated with Hand, Foot and Mouth Disease Outbreak

Author

Yang Song, Shuangli Zhu, Xianjun Wang, Dapeng Sun, Huanhuan Lu, Zhenzhi Han, Yaowen Pei, Wenbo Xu, Yong Zhang, Jinbo Xiao, Dongmei Yan, and Jianxing Wang

Subjects

biology, business.industry, Medicine, Outbreak, Coxsackievirus, business, medicine.disease, biology.organism_classification, Pathogen, Virology, Hand-foot-and-mouth disease

Abstract

Objectives: This study was conducted to discover the causes of Coxsackievirus B4 (CVB4) -induced hand, foot, and mouth disease (HFMD) outbreaks and its evolutionary characteristics.Methods: In this study, we sequenced isolates obtained during the outbreak for comparative analyses with previously sequenced strains. Phylogenetic analysis and evolutionary dynamics were performed to illustrate the genetic characteristics of CVB4 in China and worldwide.Results: The nucleotide sequence of CVB4 isolated during the outbreak in 2011 was more similar to that of CVB4 isolated in Shandong Province, China in 2010 (95.7–99.4%) than to other CVB4 isolated in China (90.9–98.8%). A phylogenetic analysis showed that CVB4 originated from a common ancestor in Shandong. CVB4 strains isolated worldwide could be classified into genotypes A–E according to the VP1 region. All CVB4 strains in China belonged to genotype E. The global population diversity of CVB4 fluctuated substantially over time, and CVB4 isolated from China accounted for a significant increase in diversity of CVB4. The average nucleotide substitution rate in VP1 of Chinese CVB4 (5.20 × 10-3 substitutions/site/year) was slightly higher than that of global CVB4 (4.82 × 10-3 substitutions/site/year). Conclusions: These findings explain both the 2011 outbreak and a global increase in CVB4 diversity. In addition to improving our understanding of a major outbreak, these findings provide a basis for the development of surveillance strategies.

Published

2021

29. Molecular analysis of Coxsackievirus A24 variant isolates from three outbreaks of acute hemorrhagic conjunctivitis in 1988, 1994 and 2007 in Beijing, China

Author

Junhan Li, Fang Huang, Yong Zhang, Tianjiao Ji, Shuangli Zhu, Dongyan Wang, Zhenzhi Han, Jinbo Xiao, Fenfen Si, Wenbo Xu, and Dongmei Yan

Subjects

China, Nucleotides, Immunology, Coxsackievirus Infections, Bayes Theorem, Disease Outbreaks, Enterovirus C, Human, Virology, Beijing, Molecular Medicine, Humans, Conjunctivitis, Acute Hemorrhagic, Amino Acids, Phylogeny

Abstract

Coxsackievirus A24 variant (CVA24v) is a major pathogen that causes continued outbreaks and pandemics of acute hemorrhagic conjunctivitis (AHC). In China, the first confirmed outbreak of CVA24v-related AHC occurred in Beijing in 1988, followed by another two significant outbreaks respectively in 1994 and 2007, which coincides with the three-stage dynamic distribution of AHC in the world after 1970s. To illustrate the genetic characteristics of CVA24v in different periods, a total of 23 strains were isolated from those three outbreaks and the whole genome of those isolations were sequenced and analyzed. Compared with the prototype strain, the 23 strains shared four nucleotide deletions in the 5' UTR except the 0744 strain isolated in 2007. And at the 98th site, one nucleotide insertion was found in all the strains collected from 2007. From 1994 to 2007, amino acid polarity in the VP1 region at the 25th and the 32nd site were changed. Both the 3C and VP1 phylogenetic tree indicated that isolates from 1988 and 1994 belonged to Genotype III (GIII), and 2007 strains to Genotype IV (GIV). According to the Bayesian analysis based on complete genome sequence, the most recent common ancestors for the isolates in 1988, 1994 and 2007 were respectively estimated around October 1987, February 1993 and December 2004. The evolutionary rate of the CVA24v was estimated to be 7.45 ​× ​10

Published

2021

30. Genomic epidemiology of coxsackievirus A16 in mainland of China, 2000-18

Author

Xianjun Wang, Yanjun Zhang, Dongmei Yan, Qian Yang, Chonghai Li, Tianjiao Ji, Haiyan Wei, Shuangli Zhu, Yong Zhang, Qiuli Yu, Ying Xiong, Yonglin Shi, Jinbo Xiao, Deshan Yu, Wei Huang, Yang Song, Jia-meng Li, Zhifei Zhan, Wenbo Xu, Lili Jiang, Zhenzhi Han, Jie Li, and Hanri Zeng

Subjects

Mainland China, medicine.medical_specialty, phylogeny, Microbiology, law.invention, 03 medical and health sciences, law, Virology, Epidemiology, Genotype, medicine, AcademicSubjects/MED00860, China, 030304 developmental biology, coxsackievirus A16, 0303 health sciences, Genetic diversity, 030306 microbiology, enterovirus, AcademicSubjects/SCI01130, AcademicSubjects/SCI02285, phylodynamics, Viral phylodynamics, Transmission (mechanics), Geography, Mainland, epidemiology, Demography, Research Article

Abstract

Hand, foot, and mouth disease (HFMD), which is a frequently reported and concerning disease worldwide, is a severe burden on societies globally, especially in the countries of East and Southeast Asia. Coxsackievirus A16 (CV-A16) is one of the most important causes of HFMD and a severe threat to human health, especially in children under 5 years of age. To investigate the epidemiological characteristics, spread dynamics, recombinant forms (RFs), and other features of CV-A16, we leveraged the continuous surveillance data of CV-A16-related HFMD cases collected over an 18-year period. With the advent of the EV-A71 vaccine since 2016, which targeted the EV-A71-related HFMD cases, EV-A71-related HFMD cases decreased dramatically, whereas the CV-A16-related HFMD cases showed an upward trend from 2017 to October 2019. The CV-A16 strains observed in this study were genetically related and widely distributed in the mainland of China. Our results show that three clusters (B1a–B1c) existed in the mainland of China and that the cluster of B1b dominates the diffusion of CV-A16 in China. We found that eastern China played a decisive role in seeding the diffusion of CV-A16 in China, with a more complex and variant transmission trend. Although EV-A71 vaccine was launched in China in 2016, it did not affect the genetic diversity of CV-A16, and its genetic diversity did not decline, which confirmed the epidemiological surveillance trend of CV-A16. Two discontinuous clusters (2000–13 and 2014–18) were observed in the full-length genome and arranged along the time gradient, which revealed the reason why the relative genetic diversity of CV-A16 increased and experienced more complex fluctuation model after 2014. In addition, the switch from RFs B (RF-B) and RF-C co-circulation to RF-D contributes to the prevalence of B1b cluster in China after 2008. The correlation between genotype and RFs partially explained the current prevalence of B1b. This study provides unprecedented full-length genomic sequences of CV-A16 in China, with a wider geographic distribution and a long-term time scale. The study presents valuable information about CV-A16, aimed at developing effective control strategies, as well as a call for a more robust surveillance system, especially in the Asia-Pacific region.

Published

2020

31. Genetic Diversity Analysis of Coxsackievirus A8 Circulating in China and Worldwide Reveals a Highly Divergent Genotype

Author

Shuangli Zhu, Wenbo Xu, Qian Yang, Tianjiao Ji, Jinbo Xiao, Dongmei Yan, Yong Zhang, Zhenzhi Han, Yang Song, Dongyan Wang, and Huanhuan Lu

Subjects

0301 basic medicine, China, Genotype, 030106 microbiology, lcsh:QR1-502, Genome, Viral, Viral quasispecies, Coxsackievirus, emerging diseases, Genome, lcsh:Microbiology, Article, 03 medical and health sciences, Virology, Databases, Genetic, Humans, Gene, coxsackievirus A8, Genetics, Genetic diversity, Phylogenetic tree, biology, phylogenetic analysis, Genetic Variation, and mouth disease, genetic diversity, biology.organism_classification, Enterovirus A, Human, 030104 developmental biology, Infectious Diseases, GenBank, foot, evolutionary dynamics, hand, Hand, Foot and Mouth Disease

Abstract

Coxsackievirus A8 (CV-A8) is one of the pathogens associated with hand, foot and mouth disease (HFMD) and herpangina (HA), occasionally leading to severe neurological disorders such as acute flaccid paralysis (AFP). Only one study aimed at CV-A8 has been published to date, and only 12 whole-genome sequences are publicly available. In this study, complete genome sequences from 11 CV-A8 strains isolated from HFMD patients in extensive regions from China between 2013 and 2018 were determined, and all sequences from GenBank were retrieved. A phylogenetic analysis based on a total of 34 complete VP1 sequences of CV-A8 revealed five genotypes: A, B, C, D and E. The newly emerging genotype E presented a highly phylogenetic divergence compared with the other genotypes and was composed of the majority of the strains sequenced in this study. Markov chain Monte Carlo (MCMC) analysis revealed that genotype E has been evolving for nearly a century and somehow arose in approximately 2010. The Bayesian skyline plot showed that the population size of CV-A8 has experienced three dynamic fluctuations since 2001. Amino acid residues of VP1100N, 103Y, 240T and 241V, which were embedded in the potential capsid loops of genotype E, might enhance genotype E adaption to the human hosts. The CV-A8 whole genomes displayed significant intra-genotypic genetic diversity in the non-capsid region, and a total of six recombinant lineages were detected. The Chinese viruses from genotype E might have emerged recently from recombining with European CV-A6 strains. CV-A8 is a less important HFMD pathogen, and the capsid gene diversity and non-capsid recombination variety observed in CV-A8 strains indicated that the constant generation of deleterious genomes and a constant selection pressure against these deleterious mutations is still ongoing within CV-A8 quasispecies. It is possible that CV-A8 could become an important pathogen in the HFMD spectrum in the future. Further surveillance of CV-A8 is greatly needed.

Published

2020

32. The Husavirus Posa-Like Viruses in China, and a New Group of Picornavirales

Author

Huanhuan Lu, Wenbo Xu, Man Zhang, Dongmei Yan, Guolong Dai, Zhenzhi Han, Shuangli Zhu, Jinbo Xiao, Yueling Liang, Mei Hong, Yong Zhang, and Yang Song

Subjects

0301 basic medicine, Dicistroviridae, biology, Phylogenetic tree, Lineage (evolution), 030106 microbiology, lcsh:QR1-502, posa-like virus, Picornavirales, biology.organism_classification, phylogeny, Genome, lcsh:Microbiology, Marnaviridae, 03 medical and health sciences, 030104 developmental biology, Infectious Diseases, Phylogenetics, Evolutionary biology, husavirus, Virology, evolution, Clade

Abstract

Novel posa-like viral genomes were first identified in swine fecal samples using metagenomics and were designated as unclassified viruses in the order Picornavirales. In the present study, nine husavirus strains were identified in China. Their genomes share 94.1&ndash, 99.9% similarity, and alignment of these nine husavirus strains identified 697 nucleotide polymorphism sites across their full-length genomes. These nine strains were directly clustered with the Husavirus 1 lineage, and their genomic arrangement showed similar characteristics. These posa-like viruses have undergone a complex evolutionary process, and have a wide geographic distribution, complex host spectrum, deep phylogenetic divergence, and diverse genomic organizations. The clade of posa-like viruses forms a single group, which is evolutionarily distinct from other known families and could represent a distinct family within the Picornavirales. The genomic arrangement of Picornavirales and the new posa-like viruses are different, whereas the posa-like viruses have genomic modules similar to the families Dicistroviridae and Marnaviridae. The present study provides valuable genetic evidence of husaviruses in China, and clarifies the phylogenetic dynamics and the evolutionary characteristics of Picornavirales.

Published

2020

33. Molecular typing and characterization of a novel genotype of EV-B93 isolated from Tibet, China

Author

Shuangli Zhu, Wenbo Xu, Dongmei Yan, Mei Hong, Zhenzhi Han, Qian Yang, Yang Song, Man Zhang, Yong Zhang, Jinbo Xiao, and Zhijun Liu

Subjects

0301 basic medicine, Serotype, RNA viruses, Male, Viral Diseases, medicine.disease_cause, Tibet, Pathology and Laboratory Medicine, Biochemistry, Pediatrics, Enteroviruses, Disease Outbreaks, Geographical Locations, Feces, Medical Conditions, Seroepidemiologic Studies, Genotype, Medicine and Health Sciences, Public and Occupational Health, Phylogeny, Genetics, Recombination, Genetic, Multidisciplinary, Phylogenetic tree, Nucleotides, Nucleic acid sequence, Child Health, Genomics, Enterovirus B, Human, Nucleic acids, Infectious Diseases, Medical Microbiology, GenBank, Viral Pathogens, Child, Preschool, Viruses, Medicine, RNA, Viral, Female, Pathogens, Research Article, Asia, Sequence analysis, DNA recombination, Science, 030106 microbiology, Nucleotide Sequencing, Genome, Viral, Biology, Research and Analysis Methods, Microbiology, 03 medical and health sciences, medicine, Enterovirus Infections, Humans, Paralysis, Molecular Biology Techniques, Sequencing Techniques, Microbial Pathogens, Molecular Biology, Molecular epidemiology, Sequence Analysis, RNA, Organisms, Biology and Life Sciences, Infant, DNA, Molecular Typing, 030104 developmental biology, Enterovirus Infection, People and Places, Enterovirus

Abstract

EV-B93 is a novel serotype within the Enterovirus B species and is uncommon worldwide. Currently, only one full-length genomic sequence (the prototype strain) has been deposited in the GenBank database. In this study, three EV-B93 were identified, including one from an acute flaccid paralysis (AFP) patient (named 99052/XZ/CHN/1999, hereafter XZ99052) and two from healthy children (named 99096/XZ/CHN/1999 and 99167/XZ/CHN/1999, hereafter XZ99096 and XZ99167, respectively) from Tibet in 1999 during the polio eradication program. The identity between the nucleotide and amino acid sequences of the Tibet EV-B93 strain and the EV-B93 prototype strain is 83.2%-83.4% and 96.8%-96.9%, respectively. The Tibet EV-B93 strain was found to have greater nucleotide sequence identity in the P3 region to another enterovirus EV-B107 as per a phylogenetic tree analysis, which revealed that recombination occurred. Seroepidemiology data showed that EV-B93 has not produced an epidemic in Tibet and there may be susceptible individuals. The three Tibet EV-B93 strains are temperature-resistant with prognosticative virulence, suggesting the possibility of a potential large-scale outbreak of EV-B93. The analyzed EV-B93 strains enrich our knowledge about this serotype and provide valuable information on global EV-B93 molecular epidemiology. What is more, they permit the appraisal of the serotype's potential public health impact and aid in understanding the role of recombination events in the evolution of enteroviruses.

Published

2020

34. Antibody Response to COVID-19 Virus - Heilongjiang Province and Gansu Province, China, 2020

Author

Naiying, Mao, Zhen, Zhu, Shuangli, Zhu, Deshan, Yu, Jun, Xu, Aili, Cui, Lei, Cao, Jinyuan, Guo, Huiling, Wang, Dongyan, Wang, Dongmei, Yan, Yang, Song, Qian, Yang, Zhongyi, Jiang, Hui, Zhang, Chang, Shu, Ming, Yang, Yanhai, Wang, Jinbo, Xiao, Zhenzhi, Han, Yong, Zhang, Yan, Zhang, and Wenbo, Xu

Subjects

Coronavirus disease 2019 (COVID-19), biology, business.industry, Disease, Virus, Serology, Vaccination, Immune system, Preplanned Studies, Immunology, Pandemic, biology.protein, Medicine, Antibody, General Agricultural and Biological Sciences, business

Abstract

What is already known about this topic? Coronavirus disease 2019 (COVID-19) has become a global pandemic, while the profile of antibody response against the COVID-19 virus has not been well clarified. What is added by this report? In this study, 210 serum samples from 160 confirmed COVID-19 cases with different disease severities were recruited. The IgM, IgA, IgG, and neutralizing antibodies (NAb) against COVID-19 virus were determined. Our findings indicated that four antibodies could be detectable at low levels within 2 weeks of disease onset, then rapidly increasing and peaking from the 3rd to 5th Weeks. NAb decreased between 5th and 9th Weeks, and a higher IgM/IgA level was observed in the groups with mild/moderate severity within 2 weeks (p

Published

2020

35. A Large-Scale Outbreak of Echovirus 30 in Gansu Province of China in 2015 and Its Phylodynamic Characterization

Author

Deshan Yu, Wenbo Xu, Haizhuo Wu, Jianhua Chen, Yong Zhang, and Zhenzhi Han

Subjects

Microbiology (medical), Veterinary medicine, Echovirus, encephalitis, lcsh:QR1-502, medicine.disease_cause, Microbiology, molecular epidemiology, lcsh:Microbiology, 03 medical and health sciences, Genotype, echovirus 30 (E-30), medicine, China, 030304 developmental biology, Original Research, 0303 health sciences, Genetic diversity, Molecular epidemiology, 030306 microbiology, Transmission (medicine), phylogenetic analysis, Outbreak, phylodynamics, Geography, Viral phylodynamics

Abstract

Background: Echovirus 30 (E-30) has been investigated and reported worldwide and is closely associated with several infectious diseases, including encephalitis; myocarditis; and hand, foot, and mouth disease. Although many E-30 outbreaks associated with encephalitis have been reported around the world, it was not reported in northwest China until 2015. Methods: The clinical samples, including the feces, serum, throat swabs, and cerebrospinal fluid, were collected for this study and were analyzed for diagnosis. E-30 was isolated and processed according to the standard procedures. The epidemiological and phylogenetic analysis were performed to indicate the characteristics of E-30 outbreaks and phylodynamics of E-30 in China. Results: The E-30 outbreaks affected nine towns of Gansu province in 2015, starting at a school of Nancha town and spreading to other towns within one month. The epidemiological features showed that children aged 6-15 years were more susceptible to E-30 infection. The genotype B and C co-circulated in the world, whereas the latter dominated the circulation of E-30 in China. The genome sequences of this outbreak present 99.3% - 100% similarity among these strains, indicating a genetic-linked aggregate outbreak of E-30 in this study. Two larger genetic diversity expansions and three small fluctuations of E-30 were observed from 1987 to 2016 in China, which revealed the oscillating patterns of E-30 in China. In addition, the coastal provinces of China, such as Zhejiang, Fujian and Shandong, were initially infected, followed by other parts of the country. The E-30 strains isolated from mainland of China may have originated from Taiwan of China in the last century. Conclusion: The highly similarity E-30 genomes in this outbreak showed an aggregate outbreak of E-30, with 9 towns affected. Our results suggested that although the genetic diversity of E-30 oscillates, the dominant lineages of E-30 in China has complex genetic transmission. The coastal provinces played an important role in E-30 spread, which implied further development of effective countermeasures. This study provides a further insight into the E-30 outbreak and transmission, and illustrates the importance of valuable surveillance in the future.

Published

2020

36. Global Spread of the B5 Subgenotype EV-A71 and the Phylogeographical Analysis of Chinese Migration Events

Author

Yang Song, Keqiang Huang, Dongmei Yan, Wenbo Xu, Shuangli Zhu, Xiaofang Zhou, Dongyan Wang, Yong Zhang, Zhenzhi Han, and Wen Xu

Subjects

0301 basic medicine, Microbiology (medical), China, 030106 microbiology, Immunology, Population, lcsh:QR1-502, Taiwan, Disease cluster, migration, Microbiology, lcsh:Microbiology, 03 medical and health sciences, Cellular and Infection Microbiology, Japan, Enterovirus Infections, Humans, education, Phylogeny, Original Research, education.field_of_study, Singapore, molecular evolution, Outbreak, Bayes Theorem, Enterovirus a71, Thailand, Enterovirus A, Human, 030104 developmental biology, Infectious Diseases, Geography, enterovirus A71, Vietnam, Evolutionary biology, phylogeographical analysis, Mainland, Hand, Foot and Mouth Disease, B5 subgenotype

Abstract

The subgenotype B5 of EV-A71 is a widely circulating subgenotype that frequently spreads across the globe. Several outbreaks have occurred in nations, such as Malaysia, Thailand, Vietnam, and Japan. Appearing first in Taiwan, China, the subgenotype has been frequently reported in mainland of China even though no outbreaks have been reported so far. The current study reconstructed the migration of the B5 subgenotype of EV-A71 in China via phylogeographical analysis. Furthermore, we investigated its population dynamics in order to draw more credible inferences. Following a dataset cleanup of B5 subgenotype of EV-A71, we detected earlier B5 subgenotypes of EV-A71 sequences that had been circulating in Malaysia and Singapore since the year 2000, which was before the 2003 outbreak that occurred in Sarawak. The Bayesian inference indicated that the most recent common ancestor of B5 subgenotype EV-A71 appeared in September, 1994 (1994.75). With respect to the overall prevalence, geographical reconstruction revealed that the B5 subgenotype EV-A71 originated singly from single-source cluster and subsequently developed several active lineages. Based on a large amount of data that was accumulated, we conclude that the appearance of the B5 subgenotype of EV-A71 in mainland of China was mainly due to multiple migrations from different origins.

Published

2020

37. Additional file 1: of Two Coxsackievirus B3 outbreaks associated with hand, foot, and mouth disease in China and the evolutionary history worldwide

Author

Zhenzhi Han, Zhang, Yong, Keqiang Huang, Jianxing Wang, Huifang Tian, Song, Yang, Yang, Qian, Dongmei Yan, Shuangli Zhu, Mingxiao Yao, Xianjun Wang, and Wenbo Xu

Abstract

Figure S1. The result of date-randomization tests (DRTs). The temporal signal of CV-B3 datasets was tested using the Tip Dating Beast package. Based on 20 random replicates of the sampling dates produced by this package and the real datasets, the CV-B3 datasets are assured to have sufficient temporal signals for next assessment of evolutionary timescale. Table S1. The information of 236 coxsackievirus B3 (CV-B3) strains used in this analysis, including 25 isolates first reported in this study. Table S2. Evolutionary characteristics of coxsackievirus B3 (CV-B3) groups based on the entire VP1 gene. (DOCX 165 kb)

Published

2019

38. Genetic characterization and molecular epidemiological analysis of novel enterovirus EV-B80 in China

Author

Wenbo Xu, Hui Cui, Qian Yang, Haishu Tang, Keqiang Huang, Yong Zhang, Zhenzhi Han, Yang Song, Dongmei Yan, Mei Hong, and Shuangli Zhu

Subjects

0301 basic medicine, China, Epidemiology, Sequence analysis, Immunology, Population, lcsh:QR1-502, Genome, Viral, Biology, medicine.disease_cause, Antibodies, Viral, Serogroup, Microbiology, Article, lcsh:Microbiology, lcsh:Infectious and parasitic diseases, Evolution, Molecular, 03 medical and health sciences, Feces, Phylogenetics, Seroepidemiologic Studies, Virology, Drug Discovery, Genotype, medicine, Enterovirus Infections, Humans, lcsh:RC109-216, education, Phylogeny, Enterovirus, Genetics, Recombination, Genetic, education.field_of_study, Molecular epidemiology, Phylogenetic tree, Geography, Infant, Newborn, Infant, General Medicine, Sequence Analysis, DNA, 030104 developmental biology, Infectious Diseases, GenBank, Child, Preschool, RNA, Viral, Parasitology

Abstract

Enterovirus B80 (EV-B80) is a newly identified serotype belonging to the enterovirus B species. To date, only two full-length genomic sequences of EV-B80 are available in GenBank, and few studies on EV-B80 have been conducted in China or worldwide. More information and research on EV-B80 is needed to assess its genetic characteristics, phylogenetic relationships, and association with enteroviral diseases. In this study, we report the phylogenetic characteristics of three Xinjiang EV-B80 strains and one Tibet EV-B80 strain in China. The full-length genomic sequences of four strains show 78.8–79% nucleotide identity and 94–94.2% amino acid identity with the prototype of EV-B80, indicating a tendency for evolution. Based on a maximum likelihood phylogenetic tree based on the entire VP1 region, three genotypes (A–C) were defined, revealing the possible origin of EV-B80 strains in the mainland of China. Recombination analysis revealed intraspecies recombinations in all four EV-B80 strains in nonstructural regions along with two recombination patterns. Due to the geographic factor, the coevolution of EV-B strains formed two different patterns of circulation. An antibody seroprevalence study against EV-B80 in two Xinjiang prefectures also showed that EV-B80 strains were widely prevalent in Xinjiang, China, compared to other studies on EV-B106 and EV-B89. All four EV-B80 strains are not temperature sensitive, showing a higher transmissibility in the population. In summary, this study reports the full-length genomic sequences of EV-B80 and provides valuable information on global EV-B80 molecular epidemiology.

Published

2019

39. Two Coxsackievirus B3 outbreaks associated with hand, foot, and mouth disease in China and the evolutionary history worldwide

Author

Xianjun Wang, Yang Song, Jianxing Wang, Qian Yang, Keqiang Huang, Dongmei Yan, Zhenzhi Han, Huifang Tian, Wenbo Xu, Yong Zhang, Mingxiao Yao, and Shuangli Zhu

Subjects

0301 basic medicine, China, 030106 microbiology, Coxsackievirus Infections, Biology, medicine.disease_cause, lcsh:Infectious and parasitic diseases, Disease Outbreaks, 03 medical and health sciences, 0302 clinical medicine, Phylogenetics, medicine, Cluster Analysis, Humans, lcsh:RC109-216, 030212 general & internal medicine, Genotyping, Phylogeny, Retrospective Studies, Enterovirus, Phylogenetic tree, Molecular epidemiology, Transmission (medicine), CV-B3, Outbreak, Aseptic meningitis, medicine.disease, Virology, Biological Evolution, HFMD, Enterovirus B, Human, Infectious Diseases, Hand, Foot and Mouth Disease, Research Article

Abstract

Background Coxsackievirus B3 (CV-B3) is usually associated with aseptic meningitis and myocarditis; however, the association between CV-B3 and hand, foot, and mouth disease (HFMD) has not been clearly demonstrated, and the phylogenetic dynamics and transmission history of CV-B3 have not been well summarized. Method Two HFMD outbreaks caused by CV-B3 were described in Hebei Province in 2012 and in Shandong Province in 2016 in China. To analyze the epidemiological features of two CV-B3 outbreaks, a retrospective analysis was conducted. All clinical specimens from CV-B3 outbreaks were collected and disposed according to the standard procedures supported by the WHO Global Poliovirus Specialized Laboratory. EV genotyping and phylogenetic analysis were performed to illustrate the genetic characteristics of CV-B3 in China and worldwide. Results Two transmissible lineages (lineage 2 and 3) were observed in Northern China, which acted as an important “reservoir” for the transmission of CV-B3. Sporadic exporting and importing of cases were observed in almost all regions. In addition, the global sequences of CV-B3 showed a tendency of geographic-specific clustering, indicating that geographic-driven adaptation plays a major role in the diversification and evolution of CV-B3. Conclusions Overall, our study indicated that CV-B3 is a causative agent of HFMD outbreak and revealed the phylogenetic dynamics of CV-B3 worldwide, as well as provided an insight on CV-B3 outbreaks for effective intervention and countermeasures. Electronic supplementary material The online version of this article (10.1186/s12879-019-4107-z) contains supplementary material, which is available to authorized users.

Published

2018