# Frataxin deficiency as a cause of endothelial senescence in multiple subtypes of pulmonary hypertension

> **NIH NIH R01** · UNIVERSITY OF PITTSBURGH AT PITTSBURGH · 2021 · $617,569

## Abstract

Background: Endothelial cell (EC) pathobiology drives pulmonary hypertension (PH), but confusion over the
evolution of EC phenotypes in this disease has persisted for decades. EC senescence, a state of stable cell
cycle arrest, has been reported in PH, but the regulatory features are unknown. Led by our prior work showing
deficiency of iron-sulfur (Fe-S) clusters in PH, we found that a Fe-S biogenesis protein, frataxin (FXN), controls
senescence in pulmonary ECs. This may occur in Friedreich’s ataxia (FRDA), a disease marked by genetic
FXN deficiency, cardiomyopathy, and often PH. Here, we offer a new model of EC biology in PH, where FXN
loss promotes genotoxic stress and senescence in a pulmonary EC subset with low enough FXN. Senescent
ECs then promote inflammation and drive many PH subtypes, including PH of FRDA and left heart disease.
Hypothesis: We propose FXN deficiency, driven by genetic or acquired means, orchestrates Fe-S-dependent
genotoxic stress, enforcing EC senescence and multiple PH subtypes. Aim 1. Determine if FXN deficiency
drives DNA damage to enforce EC senescence. By study of human pulmonary artery and microvascular ECs
and via genome editing of FXN mutations in inducible pluripotent stem cell (iPSC)-derived ECs from FRDA
patients, we will study the role of FXN in genomic stress and EC senescence. Via study of circulating factors,
histology, and single cell RNA sequencing, we will assess EC senescence in plasma and rare lung specimens
from PAH patients and FRDA and HCM patients with pulmonary vascular disease. We expect to see a dose-
dependent orchestration of FXN activities converging on EC senescence and PH. Aim 2. Determine if EC FXN
deficiency depends upon senescence and myeloid inflammation to drive PH. In mice models of Groups 1
PAH and Group 2 PH due to FRDA, by using EC FXN-/- (KO) technology and adeno-associated virus delivery
of FXN and its binding partner ISCU to pulmonary ECs in vivo, we will assess EC genomic stress, senescence,
inflammation, and PH. EC-specific p16 KO mice and CX3CR1 KO mice will be used to define if EC FXN depends
upon senescence and downstream myeloid inflammation to control PH. Thus, we aim to prove a new causative
model of EC biology in PH – one that deconvolutes the confusion over EC heterogeneity that has plagued this
field for decades. Aim 3. Determine if a novel GSTP1 inhibitor increases FXN and reverses multiple PH
subtypes. We found that a GSTP1 inhibitor increases FXN and ISCU and improves PH. We will define this
drug’s efficacy for ameliorating Groups 1-2 PH models and if FXN and GSTP1 are crucial for its function (via
FXN and GSTP1/2 KO mice). If so, we could define an entirely new Fe-S-specific therapy for PH and FRDA.
Significance: Via unique human and rodent discovery platforms, we will investigate an EC Fe-S cluster-
senescence axis controlling multiple PH subtypes. Our work could explain the evolution of EC biology in PH
and shift molecular paradigms, particularly for FRDA and...

## Key facts

- **NIH application ID:** 10235339
- **Project number:** 2R01HL122596-07A1
- **Recipient organization:** UNIVERSITY OF PITTSBURGH AT PITTSBURGH
- **Principal Investigator:** Stephen Y Chan
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $617,569
- **Award type:** 2
- **Project period:** 2015-09-01 → 2025-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10235339

## Citation

> US National Institutes of Health, RePORTER application 10235339, Frataxin deficiency as a cause of endothelial senescence in multiple subtypes of pulmonary hypertension (2R01HL122596-07A1). Retrieved via AI Analytics 2026-05-25 from https://api.ai-analytics.org/grant/nih/10235339. Licensed CC0.

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