# Molecular and evolutionary mechanisms of poxviral adaptation to new species

> **NIH NIH R21** · UNIVERSITY OF CALIFORNIA AT DAVIS · 2020 · $235,260

## Abstract

PROJECT SUMMARY
 The majority of new human diseases arise from zoonotically transmitted viruses, yet most research on
cross-species transmission is focused on a few model RNA viruses. There is a fundamental gap in understanding
how DNA viruses rapidly adapt to infect new hosts in spite of their relatively high replication fidelity. Our long-
term goal is to define molecular and evolutionary signatures that identify “high-risk” viruses poised to cross-
species barriers before an outbreak occurs. As a step towards this goal, our current objective is to define how
an experimentally evolved vaccinia virus (VACV) adapted to evade host antiviral proteins in a species-specific
manner. Our central hypothesis is that initial adaptation by gene duplication acts as a “molecular foothold”, to
broadly improve viral replication in resistant host species, and thereby enable subsequent mutations to emerge
that allow collapse of the amplified locus while maintaining the fitness benefit needed for continued replication
and spread in the new host. This hypothesis is based on our work using a cell culture-based system of experi-
mental evolution demonstrating that gene amplification of a weak viral antagonist can rapidly improve virus rep-
lication in otherwise resistant cells derived from multiple species. Subsequent adaptive mutations evolved in the
viral RNA polymerase (vRNAP) that differentially rescue virus replication in cells derived from multiple primate
species. The rationale underlying the proposed research is that once it is known how these mutations inhibit
immune proteins, we can more precisely identify poxviruses that are a higher risk to establish productive human
infections. This knowledge will also inform strategies to design safer poxvirus-vectored vaccines and oncolytic
agents that are less likely to evolve and become more pathogenic in patients. We plan to test our central hypoth-
esis for this project by completing the following two specific aims: 1) Determine how experimentally evolved
mutations in VACV vRNAP alter transcription and translation to inhibit dsRNA-mediated host restriction factors.
We will use pulse-chase RNASeq methods to define transcriptome-wide changes in the kinetics of RNA synthe-
sis and dsRNA accumulation in wt and vRNAP mutant viruses. We will also use high-dynamic range mass-
spectrometry techniques to identify changes in the viral proteome due to these mutations. 2) Define how AGM-
adapted viruses evolved to efficiently replicate in human fibroblasts. We will use our established genomics pipe-
line and newly available single molecule sequencing to define adaptive mutations that evolved during serial
passage in HF and identify structural variation in these viruses that may facilitate rapid adaptation of DNA viruses.
We believe that the research proposed in this application is innovative because it represents a novel departure
from most current viral cross-species transmission research by shifting focus to defining molecu...

## Key facts

- **NIH application ID:** 9851333
- **Project number:** 5R21AI135257-02
- **Recipient organization:** UNIVERSITY OF CALIFORNIA AT DAVIS
- **Principal Investigator:** GREGORY JASON BRENNAN
- **Activity code:** R21 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $235,260
- **Award type:** 5
- **Project period:** 2019-01-22 → 2021-12-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9851333

## Citation

> US National Institutes of Health, RePORTER application 9851333, Molecular and evolutionary mechanisms of poxviral adaptation to new species (5R21AI135257-02). Retrieved via AI Analytics 2026-06-11 from https://api.ai-analytics.org/grant/nih/9851333. Licensed CC0.

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