# Immunotherapy for acute lung injury secondary to influenza

> **NIH NIH R01** · STATE UNIVERSITY OF NEW YORK AT BUFFALO · 2021 · $436,772

## Abstract

PROJECT SUMMARY/ABSTRACT
The emergence of drug-resistant strains of human influenza A (IAV) and B viruses, as well as avian H5N1
virus with pandemic potential, to the only approved antiviral agents underscores the importance of developing
novel antiviral strategies. We have engineered electrostatic complexes between cationic nanoparticles (i.e.,
chitosan) and anionic RNA that target airway epithelial cells in vivo during an IAV infection. These nanoplexes
induce antiviral bioactivity directed against IAV in vivo with little or no untoward cellular or pulmonary
responses. The nanoplex constructs stimulate early type I interferon (IFN) cellular responses through 5’-
triphosphate (PPP)-RNA binding of the intracellular sensor, RIG-I. Additionally, the 5’PPP-NS1shRNA
nanoplex formulation suppresses the translation of the IAV virulence factor, NS1, which inhibits RIG-I and host
cell RNA maturation. The lung is well suited for an antiviral nanoplex strategy since it provides a portal for
inhalation administration of bioactive nanoplexes. We have demonstrated that this strategy inhibits in vivo IAV
replication therapeutically and avoids the “IFN paradox”, specifically, decreasing IAV lung injury, and IAV
impairment of bacterial clearance from the lung. The focus of the current proposal is to optimize the therapeutic
action of the 5’PPP-NS1shRNA nanoplex formulation in vitro and then in vivo. Additionally, we propose to carry
out experiments recommended by the FDA article entitled “Antiviral Product Development: Conducting and
Submitting Virological Studies to the Agency.” This includes in vitro and in vivo experiments to assess
therapeutic efficacy (antiviral activity), pharmacokinetics, drug-drug interactions, and development of viral
resistance. Additionally, because the 5’PPP-NS1shRNA nanoplex modulates the immune response, the FDA
recommends examining possible unintended adverse effects resulting from actions on the immune system.
Thus, we will also identify the specific immune system components that are altered, as well as assess the
immune-mediated complications of an IAV infection including increased severity of the respiratory tract injury,
and the risk of IAV-associated secondary bacterial pneumonia, a major cause of death in influenza cases.
Specifically, we will examine the ability of 5’PPP-NS1shRNA nanoplexes to stimulate innate antiviral immunity,
thereby changing infiltration of inflammatory cells, inflammatory cytokine milieu, adaptive immune responses,
as well as decrease respiratory injury and IAV-associated impairment of bacterial clearance. In addition to
assessing the clearance of IAV from the respiratory tract, we predict that the nanoplex construct will reduce the
morbidity and severity of symptoms of influenza from drug resistant seasonal and pandemic strains, the highly
pathogenic H1N1 swine-origin IAV virus (S-OIV) and H5N1 “bird flu”. These nano-technological approaches
can also potentially treat other infectious (i.e., Ebola) o...

## Key facts

- **NIH application ID:** 10133140
- **Project number:** 5R01HL151498-02
- **Recipient organization:** STATE UNIVERSITY OF NEW YORK AT BUFFALO
- **Principal Investigator:** PAUL R KNIGHT III
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $436,772
- **Award type:** 5
- **Project period:** 2020-04-01 → 2024-03-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10133140

## Citation

> US National Institutes of Health, RePORTER application 10133140, Immunotherapy for acute lung injury secondary to influenza (5R01HL151498-02). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/10133140. Licensed CC0.

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