STAR-TEL | Stratified Therapeutic Assessment Platform for Short Telomere related Lung Fibrosis using Patient-Derived iPSC

Summary
Idiopathic pulmonary fibrosis (IPF) is a lethal scarring lung disease often leading to death within 3 years of diagnosis. New antifibrotic medications slow disease progression but they are poorly tolerated by patients. Telomeres, protective structures or caps at the ends of chromosomes, governed by the enzyme telomerase are shortened in type 2 alveolar epithelial cells (AT2)s in sporadic IPF but particularly so in inherited mutations of telomere related genes causing severe disease with early onset. Early clinical studies indicate that danazol modulates telomere length and prevents the progression of pulmonary fibrosis but it is poorly tolerated by patients, causing liver toxicity. Gene therapies including mRNAs which target telomerase have potential but human preclinical models do not exist to test their efficacy. Thus, a new human preclinical model is required to better understand pathogenesis and find new treatments. In preliminary work, I demonstrate that AT2 cells generated from patient-iPSC (iAT2) can replicate elements of pulmonary fibrosis pathogenesis and that telomere length in these cells undergoes heterogenous shortening over time, analogous to the shortening which occurs in vivo. Based on this data and previously published mouse studies, I hypothesise that telomere shortening in AT2 cells causes senescence, DNA damage and inflammation in both sporadic and inherited forms of IPF. Furthermore, I hypothesise that specific gene stratified mRNA-nanomedicines delivered to the lung can modulate telomere length in a precise manner avoiding toxicity. I will compare iAT2 and hepatic cells generated from patients recruited to a clinical trial of danazol to their own clinical outcomes from the study, thereby performing the first ‘clinical trial in a dish’ in pulmonary fibrosis - to a) better understand the role of telomere shortening in IPF and to b) identify and test gene stratified mRNA-nanomedicines and delivery chemistries leading to improved patient survival.
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More information & hyperlinks
Web resources: https://cordis.europa.eu/project/id/101078300
Start date: 01-10-2023
End date: 30-09-2028
Total budget - Public funding: 1 499 420,00 Euro - 1 499 420,00 Euro
Cordis data

Original description

Idiopathic pulmonary fibrosis (IPF) is a lethal scarring lung disease often leading to death within 3 years of diagnosis. New antifibrotic medications slow disease progression but they are poorly tolerated by patients. Telomeres, protective structures or caps at the ends of chromosomes, governed by the enzyme telomerase are shortened in type 2 alveolar epithelial cells (AT2)s in sporadic IPF but particularly so in inherited mutations of telomere related genes causing severe disease with early onset. Early clinical studies indicate that danazol modulates telomere length and prevents the progression of pulmonary fibrosis but it is poorly tolerated by patients, causing liver toxicity. Gene therapies including mRNAs which target telomerase have potential but human preclinical models do not exist to test their efficacy. Thus, a new human preclinical model is required to better understand pathogenesis and find new treatments. In preliminary work, I demonstrate that AT2 cells generated from patient-iPSC (iAT2) can replicate elements of pulmonary fibrosis pathogenesis and that telomere length in these cells undergoes heterogenous shortening over time, analogous to the shortening which occurs in vivo. Based on this data and previously published mouse studies, I hypothesise that telomere shortening in AT2 cells causes senescence, DNA damage and inflammation in both sporadic and inherited forms of IPF. Furthermore, I hypothesise that specific gene stratified mRNA-nanomedicines delivered to the lung can modulate telomere length in a precise manner avoiding toxicity. I will compare iAT2 and hepatic cells generated from patients recruited to a clinical trial of danazol to their own clinical outcomes from the study, thereby performing the first ‘clinical trial in a dish’ in pulmonary fibrosis - to a) better understand the role of telomere shortening in IPF and to b) identify and test gene stratified mRNA-nanomedicines and delivery chemistries leading to improved patient survival.

Status

SIGNED

Call topic

ERC-2022-STG

Update Date

31-07-2023
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Horizon Europe
HORIZON.1 Excellent Science
HORIZON.1.1 European Research Council (ERC)
HORIZON.1.1.0 Cross-cutting call topics
ERC-2022-STG ERC STARTING GRANTS
HORIZON.1.1.1 Frontier science
ERC-2022-STG ERC STARTING GRANTS