Heparan sulfate is a binding molecule but not a receptor for CEACAM1-independent infection of murine coronavirus

A highly neurovirulent mouse hepatitis virus (MHV) JHMV strain (wt) with receptor (MHVR)-independent infection activity and its low-virulent mutant srr7 without such activity were found to attach to MHVR-negative, non-permissive BHK cells. To identify the molecule that interacts with JHMV, we focused on heparan sulfate (HS) since it works as a receptor of a mutant MHV-rec1 that infects in an MHVR-independent fashion. The present study indicates that HS interacts with both wt JHMV and srr7 but it does not function as an entry receptor as it apparently does for MHV-rec1. Furthermore, HS failed to serve as an entry receptor in the MHVR-independent infection of wt JHMV, indicating that HS is not a host factor that wt JHMV utilizes in an MHVR-independent infection. © 2007 Elsevier Inc.

keywords 🔗 present study (186) 🔗 hepatitis virus (437) 🔗 mouse hepatitis (371)

author 👤 Watanabe, Rie 👤 Sawicki, Stanley G. 👤 Taguchi, Fumihiro

year ⏰ 2007

journal 📚 Virology

issn 🗄 00426822 10960341

volume 366

number 1

page 16-22

doi 📄 10.1016/j.virol.2007.06.034 ⤴

citedbycount 6

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