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COVID-19 and influenza infections mediate distinct pulmonary cellular and transcriptomic changes
Medicine and HealthCommunications Biology

COVID-19 and influenza infections mediate distinct pulmonary cellular and transcriptomic changes

C. Wang, M. S. Khatun, et al.

This groundbreaking study, conducted by Chenxiao Wang and colleagues, uncovers how COVID-19 may disrupt lung repair mechanisms compared to influenza. The research reveals distinct cellular and transcriptional responses in infected mice, highlighting a reduced capacity for lung recovery after SARS-CoV-2 infection. Discover the implications for treatment and recovery in this compelling investigation.... show more
Abstract
SARS-CoV-2 infection can cause persistent respiratory sequelae. However, the underlying mechanisms remain unclear. Here we report that sub-lethally infected K18-human ACE2 mice show patchy pneumonia associated with histiocytic inflammation and collagen deposition at 21 and 45 days post infection (DPI). Transcriptomic analyses revealed that compared to influenza-infected mice, SARS-CoV-2-infected mice had reduced interferon-gamma/alpha responses at 4 DPI and failed to induce keratin 5 (Krt5) at 6 DPI in lung, a marker of nascent pulmonary progenitor cells. Histologically, influenza- but not SARS-CoV-2-infected mice showed extensive Krt5+ "pods" structure co-stained with stem cell markers Trp63/NGFR proliferated in the pulmonary consolidation area at both 7 and 14 DPI, with regression at 21 DPI. These Krt5+ "pods" structures were not observed in the lungs of SARS-CoV-2-infected humans or nonhuman primates. These results suggest that SARS-CoV-2 infection fails to induce nascent Krt5+ cell proliferation in consolidated regions, leading to incomplete repair of the injured lung.
Publisher
Communications Biology
Published On
Dec 13, 2023
Authors
Chenxiao Wang, Mst Shamima Khatun, Zhe Zhang, Michaela J. Allen, Zheng Chen, Calder R. Ellsworth, Joshua M. Currey, Guixiang Dai, Di Tian, Konrad Bach, Xiao-Ming Yin, Vicki Traina-Dorge, Jay Rappaport, Nicholas J. Maness, Robert V. Blair, Jay K. Kolls, Derek A. Pociask, Xuebin Qin
Tags
COVID-19influenzalung repairtranscriptomic analysisKrt5immune responsemouse model
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