Resistance Evolution against Host-directed Antiviral Agents: Buffalopox Virus Switches to Use p38-ϒ under Long-term Selective Pressure of an Inhibitor Targeting p38-α

Author:

Chander Yogesh12,Kumar Ram1,Verma Assim12,Khandelwal Nitin1,Nagori Himanshu1,Singh Namita2,Sharma Shalini3,Pal Yash1,Puvar Apurvasinh4,Pandit Rameshchandra4,Shukla Nitin4,Chavada Priyank4,Tripathi Bhupendra N1,Barua Sanjay1,Kumar Naveen1ORCID

Affiliation:

1. National Centre for Veterinary Type Cultures, ICAR-National Research Centre on Equines , Hisar , India

2. Department of Bio and Nano Technology, Guru Jambeshwar University of Science and Technology , Hisar, Haryana , India

3. Department of Veterinary Physiology and Biochemistry, Lala Lajpat Rai University of Veterinary and Animal Sciences , Hiar, Haryana , India

4. Gujarat Biotechnology Research Centre, Department of Science & Technology, Government of Gujarat , Gandhinagar , India

Abstract

Abstract Host-dependency factors have increasingly been targeted to minimize antiviral drug resistance. In this study, we have demonstrated that inhibition of p38 mitogen-activated protein kinase (a cellular protein) suppresses buffalopox virus (BPXV) protein synthesis by targeting p38-MNK1-eIF4E signaling pathway. In order to provide insights into the evolution of drug resistance, we selected resistant mutants by long-term sequential passages (P; n = 60) in the presence of p38 inhibitor (SB239063). The P60-SB239063 virus exhibited significant resistance to SB239063 as compared to the P60-Control virus. To provide mechanistic insights on the acquisition of resistance by BPXV-P60-SB239063, we generated p38-α and p38-ϒ (isoforms of p38) knockout Vero cells by CRISPR/Cas9-mediated genome editing. It was demonstrated that unlike the wild type (WT) virus which is dependent on p38-α isoform, the resistant virus (BPXV-P60-SB239063) switches over to use p38-ϒ so as to efficiently replicate in the target cells. This is a rare evidence wherein a virus was shown to bypass the dependency on a critical cellular factor under selective pressure of a drug.

Publisher

Oxford University Press (OUP)

Subject

Genetics,Molecular Biology,Ecology, Evolution, Behavior and Systematics

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