2003
DOI: 10.1111/j.1348-0421.2003.tb03458.x
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Characterization of a Slow‐Migrating Component of the Rabies Virus Matrix Protein Strongly Associated with the Viral Glycoprotein

Abstract: The envelope of the rabies virus (a prototype of the Rhabdoviridae) contains two species of virus-coded major polypeptides; a transmembrane glycoprotein (G) and a matrix protein (M; formerly called M2), and some host-derived minor components including CD44 and a CD99-related glycoprotein (VAP21) (20,36,37,40). The M protein is a small non-glycosylated internal virion protein (Mr.ϭ24 kDa), and is thought to be located underneath the lipid bilayer of the envelope, where the M protein is thought to associate with… Show more

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Cited by 7 publications
(6 citation statements)
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“…These results were well consistent with the data obtained in our previous report of a similar two-step IP assay (26), in which we compared the coprecipitated G proteins recovered with anti-M mAb (#3-9-16) and pAb, showing that similar amounts of G protein were coprecipitated with either anti-M mAb or pAb. To be noted specially is that anti-M mAb #3-9-16 recognizes only the β-form of M protein (Mβ), one of the two forms of M protein that exposes the 3-9-16 epitopecontaining N-terminus, and is present mostly in a dimer form in the virion as well as in the cell (26). From these observations and considerations, we assumed that the acid-resistant fraction of the B form of G proteins was intimately associated with the M protein (probably the dimer form).…”
Section: Interaction With the M Protein Dimersupporting
confidence: 92%
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“…These results were well consistent with the data obtained in our previous report of a similar two-step IP assay (26), in which we compared the coprecipitated G proteins recovered with anti-M mAb (#3-9-16) and pAb, showing that similar amounts of G protein were coprecipitated with either anti-M mAb or pAb. To be noted specially is that anti-M mAb #3-9-16 recognizes only the β-form of M protein (Mβ), one of the two forms of M protein that exposes the 3-9-16 epitopecontaining N-terminus, and is present mostly in a dimer form in the virion as well as in the cell (26). From these observations and considerations, we assumed that the acid-resistant fraction of the B form of G proteins was intimately associated with the M protein (probably the dimer form).…”
Section: Interaction With the M Protein Dimersupporting
confidence: 92%
“…A portion of those G proteins, however, seemed to be limited in such changes, probably due to the intimate association of a dimer form of M protein, resulting in preserving its ability to keep the 1-30-44 epitope-positive conformation even when exposed to acidic conditions. These results are consistent with our previous reports describing the strong (i.e., NP-40/DOC-resistant) G-M association, for which a C-terminal-sided small region of M protein is essential (25), and for which a dimer form of the M protein was also suggested to be responsible (26). Possible role(s) of such an intimate G-M association will be discussed.…”
supporting
confidence: 92%
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“…The M protein binds to the RNP core, and collaborates with the viral G protein in the infected cells to produce progeny virions by budding at the cell membrane [34,35]. The M protein is also required for the development of a typical bullet-shaped rhabdovirus [29].…”
Section: Discussionmentioning
confidence: 99%