Cellular profiling identifies an early profibrotic alveolar type 2 cell signature in lung fibrosis

Ram P. Naikawadi
Alexey Bazarov
Michael Wax
Kaveh Boostanpour
Jasleen Kukreja
Michela Traglia
Ayushi Agrawal
Reuben Thomas
Mallar Bhattacharya
Paul J. Wolters

Read the full article

Listed in

This article is not in any list yet, why not save it to one of your lists.

Abstract

Rationale

Idiopathic pulmonary fibrosis (IPF) is a progressive, age-associated, lung disease characterized by short telomeres in alveolar type 2 (AT2) cells, epithelial remodeling, and fibrosis.

Objectives

This study investigated how telomere dysfunction in AT2 cells lacking Telomere Repeat Binding Factor 1 (TRF1) drives lung remodeling in SPC-creTRF1 ^flox/flox mice and its relevance to IPF.

Methods

Mouse model of telomere dysfunction was used to conditionally delete TRF1 in AT2 cells. SPC-creTRF1 ^flox/flox mouse lung epithelial cells were used to perform single cell RNA sequencing. AT2 cells from IPF lungs were analyzed by single cell RNA sequencing in an organoid model.

Measurements and Main Results

Single cell RNA-sequencing revealed distinct pathological AT2 cells enriched in DNA damage, senescence, oxidative stress, and pro-fibrotic genes, along with fewer “normal” AT2 cells and increased club cells in SPC-creTRF1 ^flox/flox mice. Pathological AT2 cells showed different early and late-stage gene signatures, with a prominent p53 signature at both time-points. Genetic deletion of p53 in SPC-creTRF1 ^flox/flox AT2 cells improved survival and prevented lung fibrosis. p53 deletion or inhibition improved organoid formation, surfactant protein C expression, and reduced pro-fibrotic gene expression in AT2 cells isolated from SPC-creTRF1 ^flox/flox mice or IPF lungs.

Conclusions

These data suggest that the DNA damage response to AT2 cell telomere dysfunction, driven by enhanced p53 activity, mediates early AT2 cell transdifferentiation and senescence, leading to epithelial cell remodeling and fibrosis and that reversing this reprogramming is a potential therapeutic approach for managing IPF.

Version published to 10.1101/2025.05.22.655638v1 on bioRxiv
May 23, 2025

Transcriptomic Signature-Guided Depletion of Intermediate Alveolar Epithelial Cells Ameliorates Pulmonary Fibrosis in Mice

This article has 11 authors:
1. Yong Zhou
2. Fei Peng
3. Chun-sun jiang
4. Zhen Zheng
5. Shahram Aliyari
6. Dan Shan
7. Aaryan Sabharwal
8. Qinyan Yin
9. Chao He
10. Joseph Lasky
11. Victor Thannickal
This article has no evaluationsLatest version May 21, 2025
Wilms’ tumor 1 impairs apoptotic clearance of fibroblasts in distal fibrotic lung lesions

This article has 14 authors:
1. Harshavardhana H. Ediga
2. Chanukya P. Vemulapalli
3. Vishwaraj Sontake
4. Pradeep K. Patel
5. Hikaru Miyazaki
6. Dimitry Popov
7. Martin B Jensen
8. Anil G. Jegga
9. Steve K. Huang
10. Christoph Englert
11. Andreas Schedl
12. Nishant Gupta
13. Francis X. McCormack
14. Satish K. Madala
This article has no evaluationsLatest version May 22, 2025
Type I IFN-activated lung monocytes and macrophages as initiators and drivers of fibrosis at the alveolar barrier in IPF

This article has 17 authors:
1. Vishal Nathwani
2. Praveen Weeratunga
3. Jeongmin Woo
4. Laura Denney
5. Chaitanya Vuppusetty
6. Tian Hu
7. Sabrina Zulfikar
8. Andrew Achaiah
9. Harriet Parker
10. Huei-Wen Chuang
11. Michalina Mazurczyk
12. Aleksandr Fedorov
13. Alison Simmons
14. Colin Clelland
15. Jan Rehwinkel
16. Agne Antanaviciute
17. Ling-Pei Ho
This article has no evaluationsLatest version May 11, 2025

Listed in

Abstract

Rationale

Objectives

Methods

Measurements and Main Results

Conclusions

Article activity feed

Related articles

Transcriptomic Signature-Guided Depletion of Intermediate Alveolar Epithelial Cells Ameliorates Pulmonary Fibrosis in Mice

Wilms’ tumor 1 impairs apoptotic clearance of fibroblasts in distal fibrotic lung lesions

Type I IFN-activated lung monocytes and macrophages as initiators and drivers of fibrosis at the alveolar barrier in IPF