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The membrane (M) glycoprotein of coronaviruses (CoVs) serves as the nidus for virion assembly. Using a yeast two-hybrid screen, we identified the interaction of the cytosolic tail of Murine Hepatitis Virus (MHV-CoV) M protein with Myosin Vb (MYO5B), specifically with the alternative splice variant of cellular MYO5B including exon D (MYO5B+D), which mediates interaction with Rab10. When co-expressed in human lung epithelial A549 and canine kidney epithelial MDCK cells, MYO5B+D co-localized with the MHV-CoV M protein, as well as with the M proteins from Porcine Epidemic Diarrhea Virus (PEDV-CoV), Middle East Respiratory Syndrome (MERS-CoV) and Severe Acute Respiratory Syndrome 2 (SARS-CoV-2). Co-expressed M proteins and MYO5B+D co-localized with endogenous Rab10 and Rab11a. We identified point mutations in MHV-CoV M that blocked the interaction with MYO5B+D in yeast 2-hybrid assays. One of these point mutations (E121K) was previously shown to block MHV-CoV virion assembly and its interaction with MYO5B+D. The E to K mutation at homologous positions in PEDV-CoV, MERS-CoV and SARS-CoV-2 M proteins also blocked colocalization with MYO5B+D. The knockdown of Rab10 blocked the co-localization of M proteins with MYO5B+D and was rescued by re-expression of CFP-Rab10. Our results suggest that CoV M proteins traffic through Rab10-containing systems, in association with MYO5B+D.more » « less
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Remedios, Lucas W.; Bao, Shunxing; Kerley, Cailey I.; Cai, Leon Y.; Rheault, Francois; Deng, Ruining; Cui, Can; Chiron, Sophie; Lau, Ken S.; Roland, Joseph T.; et al (, SPIE Medical Imaging)Tomaszewski, John E.; Ward, Aaron D. (Ed.)
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Bao, Shunxing; Cui, Can; Li, Jia; Tang, Yucheng; Lee, Ho Hin; Deng, Ruining; Remedios, Lucas W.; Yu, Xin; Yang, Qi; Chiron, Sophie; et al (, SPIE Medical Imaging)Tomaszewski, John E.; Ward, Aaron D. (Ed.)
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Rozenblatt-Rosen, Orit; Regev, Aviv; Oberdoerffer, Philipp; Nawy, Tal; Hupalowska, Anna; Rood, Jennifer E.; Ashenberg, Orr; Cerami, Ethan; Coffey, Robert J.; Demir, Emek; et al (, Cell)
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