A bioinformatic approach of targeting SARS-CoV-2 replication by silencing a conserved alternative reserve of the orf8 gene using host miRNAs.


Journal

Computers in biology and medicine
ISSN: 1879-0534
Titre abrégé: Comput Biol Med
Pays: United States
ID NLM: 1250250

Informations de publication

Date de publication:
06 2022
Historique:
received: 05 01 2022
revised: 11 03 2022
accepted: 20 03 2022
pubmed: 3 4 2022
medline: 20 5 2022
entrez: 2 4 2022
Statut: ppublish

Résumé

The causative agent of the COVID-19 pandemic, the SARS-CoV-2 virus has yielded multiple relevant mutations, many of which have branched into major variants. The Omicron variant has a huge similarity with the original viral strain (first COVID-19 strain from Wuhan). Among different genes, the highly variable orf8 gene is responsible for crucial host interactions and has undergone multiple mutations and indels. The sequence of the orf8 gene of the Omicron variant is, however, identical with the gene sequence of the wild type. orf8 modulates the host immunity making it easier for the virus to conceal itself and remain undetected. Variants seem to be deleting this gene without affecting the viral replication. While analyzing, we came across the conserved orf7a gene in the viral genome which exhibits a partial sequence homology as well as functional similarity with the SARS-CoV-2 orf8. Hence, we have proposed here in our hypothesis that, orf7a might be an alternative reserve of orf8 present in the virus which was compensating for the lost gene. A computational approach was adopted where we screened various miRNAs targeted against the orf8 gene. These miRNAs were then docked onto the orf8 mRNA sequences. The same set of miRNAs was then used to check for their binding affinity with the orf7a reference mRNA. Results showed that miRNAs targeting the orf8 had favorable shape complementarity and successfully docked with the orf7a gene as well. These findings provide a basis for developing new therapeutic approaches where both orf8 and orf7a can be targeted simultaneously.

Identifiants

pubmed: 35366472
pii: S0010-4825(22)00228-1
doi: 10.1016/j.compbiomed.2022.105436
pmc: PMC8942883
pii:
doi:

Substances chimiques

MicroRNAs 0
RNA, Messenger 0
Viral Proteins 0

Types de publication

Journal Article

Langues

eng

Sous-ensembles de citation

IM

Pagination

105436

Informations de copyright

Copyright © 2022 Elsevier Ltd. All rights reserved.

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Auteurs

Vaggu Raghavendra Goud (VR)

School of Biotechnology, KIIT University, Bhubaneswar, India.

Rajasree Chakraborty (R)

School of Biotechnology, KIIT University, Bhubaneswar, India.

Averi Chakraborty (A)

School of Biotechnology, KIIT University, Bhubaneswar, India.

Kousalya Lavudi (K)

School of Biotechnology, KIIT University, Bhubaneswar, India.

Sriram Patnaik (S)

School of Biotechnology, KIIT University, Bhubaneswar, India.

Swati Sharma (S)

School of Biotechnology, KIIT University, Bhubaneswar, India; Dept. of Skill Buildings Shri Ramasamy Memorial University, Sikkim, Gangtok, 737102, India.

Srinivas Patnaik (S)

School of Biotechnology, KIIT University, Bhubaneswar, India. Electronic address: srinivas.patnaik@kiitbiotech.ac.in.

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