Highlights d AI system that can diagnose COVID-19 pneumonia using CT scans d Prediction of progression to critical illness d Potential to improve performance of junior radiologists to the senior level d Can assist evaluation of drug treatment effects with CT quantification
It was recently brought to our attention that our paper was missing information regarding when the patient chest computed tomography (CT) scans were obtained and that there were some discrepancies in the clinical metadata, associated with the very large image dataset, that we made publicly available through the China National Center for Bioinformation (http://ncov-ai.big.ac.cn/ download?lang=en). All of the chest CT and clinical metadata used in our prognostic analysis were collected from patients at the time of hospital admission, and we have now added this statement to the STAR Methods section of our paper. We believe that the errors in the clinical metadata were introduced when the chest CT images, clinical metadata, and codes were transferred to the web server, and we have now corrected the errors manually. Although these corrections do not alter any of the conclusions made in the paper, we do apologize for these errors and any confusion that they may have caused.
Macrophages play a pivotal role in tissue fibrogenesis, which underlies the pathogenesis of many end-stage chronic inflammatory diseases. MicroRNAs are key regulators of immune cell functions, but their roles in macrophage's fibrogenesis have not been characterized. Here we show that IL-4 and IL-13 induce miR-142-5p and downregulate miR-130a-3p in macrophages; these changes sustain the profibrogenic effect of macrophages. In vitro, miR-142-5p mimic prolongs STAT6 phosphorylation by targeting its negative regulator, SOCS1. Blocking miR-130a relieves its inhibition of PPARγ, which coordinates STAT6 signalling. In vivo, inhibiting miR-142-5p and increasing miR-130a-3p expression with locked nucleic acid-modified oligonucleotides inhibits CCL4-induced liver fibrosis and bleomycin-induced lung fibrosis in mice. Furthermore, macrophages from the tissue samples of patients with liver cirrhosis and idiopathic pulmonary fibrosis display increased miR-142-5p and decreased miR-130a-3p expression. Therefore, miR-142-5p and miR-130a-3p regulate macrophage profibrogenic gene expression in chronic inflammation.
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