Author:
Yadav Priya,Kumar Ankeet,Nath Sujith S,Shashidhar Geetha,Joshi Madhvi,Puvar Apurva,Sharma Sonal,Raval Janvi,Pandit Rameshchandra,Chavada Priyank,Nagaraj Sudheep,Revanaiah Yogesharadhya,Patil Deepak,Raval S K,Raval Jigar,Kanani Amit,Thakar Falguni,Kumar Naveen,Reddy Gundallhalli Bayyappa Manjunatha,Joshi Chaitanya,Gulati Baldev Raj,Tatu Utpal
Abstract
ABSTRACTLumpy skin disease virus (LSDV) belongs to the genusCapripoxvirus and familyPoxviridae. LSDV was endemic in most of Africa, Middle east and Turkey, but since 2015, several outbreaks have been reported in Asian countries. In this study we used Whole Genome Sequence (WGS) approach to investigate the origin of the outbreak and understand the genomic landscape of the virus. Our study showed that the LSDV strain of 2022 outbreak exhibited many genetic variations, compared to the Reference Neethling strain sequence and the previous field strains from India. A total of 1819 variations were found in 22 genome sequences, which includes 399 extragenic mutations, 153 insertion frameshift mutations, 234 deletion frameshift mutations, 271 Single nucleotide polymorphisms (SNPs) and 762 silent SNPs. 38 genes have more than 2 variations per gene and these genes belong to viral-core protein, viral binding proteins, replication and RNA polymerase proteins. We highlight the importance of several SNPs in various genes which may play an essential role in pathogenesis of LSDV. Phylogenetic analysis performed on all whole genome sequences of LSDV showed two types of variants in India. One group of the variant with fewer mutations was found to lie closer to the LSDV 2019 strain from Ranchi while the other group clustered with previous Russian outbreaks from 2015. Our study highlights the importance of genomic characterization of viral outbreaks to not only monitor the frequency of mutations but also address its role in pathogenesis of LSDV as the outbreak continues.
Publisher
Cold Spring Harbor Laboratory
Cited by
1 articles.
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