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DYRK1A promotes viral entry of highly pathogenic human coronaviruses in a kinase-independent manner

PLoS biology. 2023-04; 
Madison S. Strine; Wesley L. Cai; Jin Wei; Mia Madel Alfajaro; Renata B. Filler; Scott B. Biering; Sylvia Sarnik; Ryan D. Chow; Ajinkya Patil; Kasey S. Cervantes; Clayton K. Collings; Peter C. DeWeirdt; Ruth E. Hanna; Kevin Schofield; Christopher Hulme; Silvana Konermann; John G. Doench; Patrick D. Hsu; Cigall Kadoch; Qin Yan; Craig B. Wilen
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摘要

Identifying host genes essential for Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) has the potential to reveal novel drug targets and further our understanding of Coronavirus Disease 2019 (COVID-19). We previously performed a genome-wide CRISPR/Cas9 screen to identify proviral host factors for highly pathogenic human coronaviruses. Few host factors were required by diverse coronaviruses across multiple cell types, but DYRK1A was one such exception. Although its role in coronavirus infection was previously undescribed, DYRK1A encodes D ual Specificity T y rosine Phosphorylation R egulated K inase 1A and is known to regulate cell proliferation and neuronal development. Here, we demonstrate that DYR... More

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