# Overcoming host Genetic Redundancy and Pathogen Subversion to Define new host-viral Interfaces

> **NIH NIH R35** · UT SOUTHWESTERN MEDICAL CENTER · 2024 · $405,071

## Abstract

Project Summary/Abstract
 Viruses have evolved sophisticated mechanisms to hijack host cellular machinery. For their part,
hosts have developed their own intricate defense systems. Defining how these opposing strategies
have co-evolved increases our understanding of infectious diseases and provides new opportunities to
discover unexplored areas of biology. Our understanding of host cellular defense systems has been
limited due to genetic redundancy in host genomes. A further complication is that successful pathogens
are able to inactivate host antiviral networks during infection. We have recently established a new
genetic screening platform that overcomes these roadblocks. First, we bypass genetic redundancy in
host genomes through a gain of function screen that identifies antiviral genes. Second, we use both
virulent and attenuated strains of viruses in our screening pipeline. Importantly, these attenuated
viruses have deletions or mutations in critical, yet poorly understood, immune evasion proteins that
antagonize host antiviral restriction factors. We predict that the avirulent strains of these viruses will
become sensitive to restriction factors that have otherwise defied molecular identification. Using this
strategy, one project will be to identify ancient antiviral genes that reveal unappreciated areas of host-
pathogen conflict. For example, we are unmasking how the influenza immune evasion protein, NS1
orchestrates a complex, multifaceted rewiring of host antiviral networks using comparative screens with
wild-type and NS1-deficient viruses. We are extending these studies to other virulent-attenuated virus
pairings as well. Another project takes newly identified antiviral molecules that inhibit disparate virus
families and define the molecular mechanism underlying viral inhibition. Here, we focus on the JADE
family of proteins that regulate histone acetylation. We aim to uncover functional redundancy in the
JADE family and to determine if it assembles a concerted antiviral epigenetic program. Another project
is to leverage newly identified host-pathogen conflicts to discover the physiological functions of host-
proteins that are poorly understood. In this regard, we are focusing on the CD300 family of receptor
proteins. CD300 genes are undergoing rapid positive selection, yet their physiological function remains
largely unexplored. We previously demonstrated that CD300lf is a protein receptor for murine norovirus.
We will employ the biochemical, genetic, and cellular tools we developed for studying norovirus-CD300
interactions to define the physiological ligands of CD300 receptors. Determining the ligands for these
orphan receptors will provide functional insight into these rapidly evolving proteins. Taken together, we
plot a road map for discovering new host-pathogen interfaces, defining their molecular interactions
during host defense, and how this relates to the physiological functions of these proteins and pathways.

## Key facts

- **NIH application ID:** 10877892
- **Project number:** 5R35GM142684-04
- **Recipient organization:** UT SOUTHWESTERN MEDICAL CENTER
- **Principal Investigator:** Robert C. Orchard
- **Activity code:** R35 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $405,071
- **Award type:** 5
- **Project period:** 2021-09-18 → 2026-06-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10877892

## Citation

> US National Institutes of Health, RePORTER application 10877892, Overcoming host Genetic Redundancy and Pathogen Subversion to Define new host-viral Interfaces (5R35GM142684-04). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10877892. Licensed CC0.

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