# The development of a transcriptional inhibitor for lung fibrosis.

> **NIH NIH R43** · ALTAY THERAPEUTICS, INC. · 2022 · $299,068

## Abstract

Abstract/Summary
Idiopathic Pulmonary Fibrosis (IPF) affects 100,000 people in the US with total incidences to increase 5% every
year. The 5-year survival rate of patients suffering from IPF is between 20-40%. Esbriet and Nintedanib are
clinically approved treatments for IPF. Esbriet reduces risk of disease progression by 50% however, the
mechanism of action is currently unknown. Nintedanib is an angiokinase inhibitor that targets more than 30
kinases including platelet-derived growth factor receptor, fibroblasts growth factor receptor and vascular
endothelial growth factor receptor and in clinical trials Nintedanib reduced the decline of IPF by 50% after one
year of treatment. Although Esbriet and Nintedanib are marketed to treat IPF, all patients progress despite
therapy, develop advanced disease requiring oxygen and either succumb to the disease or undergo lung
transplantation. Therefore, finding new treatments that both prevent and reverse fibrotic tissue are in great need.
Transcriptional profiles in progressive IPF patient tissues have demonstrated significant activation of the master
transcriptional regulator STAT3 determined by increased phosphorylation in SH2-dimerization domain (pSTAT3-
Y705). Active STAT3 in IPF correlated with poor patient survival driven by inflammation and ECM. Furthermore,
genetic evidence shows polymorphisms within IL6, STAT3 activator, was independently associated with disease
progression. We hypothesize that targeting STAT3 will block multiple profibrogenic pathways and reduce
inflammation and collagen accumulation in the lung. Although TFs like STAT3 are attractive therapeutic targets,
they are challenging to target with small molecules because they lack clear binding pockets, have large surface
areas important for protein-protein interactions and contain large intrinsically disordered domains. At Altay
Therapeutics, we developed a platform that enables identification of small binding pockets within intrinsically
disordered domains in previously undruggable TFs, allowing a novel druggable approach for targeting STAT3
with specific and development of potent and highly specific STAT3 inhibitors (STAT3i). We completed in-silico
screening and identified inhibitors that reduced STAT3 DNA binding. Importantly, these STAT3i had minimal
STAT1 inhibitory activity, low cytotoxicity and demonstrated potent inhibition of STAT3 targets and fibrosis
genes. We propose three aims to identify and characterize the most promising lead and continue our efforts to
develop a viable treatment for IPF based on inhibiting STAT3. In Aim 1, we will measure cellular cytotoxicity in
a panel of normal cells as well as measure STAT3 target gene inhibition with Altay’s novel STAT3is. In Aim 2,
we will carry out bleomycin induced IPF mouse studies with our lead STAT3is. In Aim 3, we will determine
antifibrotic activity of STAT3i in precision cut lung slices isolated from IPF patients as well as measure cytokine
secretion. The proposed studies ...

## Key facts

- **NIH application ID:** 10489942
- **Project number:** 1R43HL162149-01A1
- **Recipient organization:** ALTAY THERAPEUTICS, INC.
- **Principal Investigator:** Ali Rayet Ozes
- **Activity code:** R43 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2022
- **Award amount:** $299,068
- **Award type:** 1
- **Project period:** 2022-06-01 → 2024-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10489942

## Citation

> US National Institutes of Health, RePORTER application 10489942, The development of a transcriptional inhibitor for lung fibrosis. (1R43HL162149-01A1). Retrieved via AI Analytics 2026-05-26 from https://api.ai-analytics.org/grant/nih/10489942. Licensed CC0.

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