Regulation of epithelial transitional states in murine and human pulmonary fibrosis
Fa Wang, … , M. Bishr Omary, Rachel L. Zemans
Fa Wang, … , M. Bishr Omary, Rachel L. Zemans
Published September 28, 2023
Citation Information: J Clin Invest. 2023;133(22):e165612. https://doi.org/10.1172/JCI165612.
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Research Article Pulmonology

Regulation of epithelial transitional states in murine and human pulmonary fibrosis

Abstract

Idiopathic pulmonary fibrosis (IPF) is a progressive scarring disease arising from impaired regeneration of the alveolar epithelium after injury. During regeneration, type 2 alveolar epithelial cells (AEC2s) assume a transitional state that upregulates multiple keratins and ultimately differentiate into AEC1s. In IPF, transitional AECs accumulate with ineffectual AEC1 differentiation. However, whether and how transitional cells cause fibrosis, whether keratins regulate transitional cell accumulation and fibrosis, and why transitional AECs and fibrosis resolve in mouse models but accumulate in IPF are unclear. Here, we show that human keratin 8 (KRT8) genetic variants were associated with IPF. Krt8–/– mice were protected from fibrosis and accumulation of the transitional state. Keratin 8 (K8) regulated the expression of macrophage chemokines and macrophage recruitment. Profibrotic macrophages and myofibroblasts promoted the accumulation of transitional AECs, establishing a K8-dependent positive feedback loop driving fibrogenesis. Finally, rare murine transitional AECs were highly senescent and basaloid and may not differentiate into AEC1s, recapitulating the aberrant basaloid state in human IPF. We conclude that transitional AECs induced and were maintained by fibrosis in a K8-dependent manner; in mice, most transitional cells and fibrosis resolved, whereas in human IPF, transitional AECs evolved into an aberrant basaloid state that persisted with progressive fibrosis.

Authors

Fa Wang, Christopher Ting, Kent A. Riemondy, Michael Douglas, Kendall Foster, Nisha Patel, Norihito Kaku, Alexander Linsalata, Jean Nemzek, Brian M. Varisco, Erez Cohen, Jasmine A. Wilson, David W.H. Riches, Elizabeth F. Redente, Diana M. Toivola, Xiaofeng Zhou, Bethany B. Moore, Pierre A. Coulombe, M. Bishr Omary, Rachel L. Zemans

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Figure 4

K8 is necessary for macrophage chemokine expression and macrophage recruitment during fibrosis.

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K8 is necessary for macrophage chemokine expression and macrophage recru...
Krt8+/+ and Krt8–/– mice were treated with bleomycin. (A) CCL2 ELISA on day 21 bronchoalveolar lavage (BAL). n = 3 mice/group. (B) BAL cells and differentials. n = 3 mice/group except for day 4 (n = 6 mice/group) and day 12 (n = 2 mice/group). Macs, macrophages; Lymphs, lymphocytes; PMN, polymorphonuclear neutrophils. (A and B) Violin plots show minimum to maximum values with the line at the median. *P < 0.05, by ratio paired t test. n = 4–5 mice/group. (C) Immunostaining on day-12 tissue. The top left image of the left panel and the top left image of the right panel in C are also shown in Figure 1E (macrophage recruitment control, left and middle images). n = 3 mice/group. Scale bar: 100 μm. Original magnification, ×20 (enlarged insets in C).