Literature DB >> 20200243

Binding site on the transferrin receptor for the parvovirus capsid and effects of altered affinity on cell uptake and infection.

Laura B Goodman1, Sangbom M Lyi, Natalie C Johnson, Javier O Cifuente, Susan L Hafenstein, Colin R Parrish.   

Abstract

Canine parvovirus (CPV) and its relative feline panleukopenia virus (FPV) bind the transferrin receptor type 1 (TfR) to infect their host cells but show differences in the interactions with the feline and canine TfRs that determine viral host range and tissue tropism. We changed apical and protease-like domain residues by introducing point mutations and adding or removing glycosylation signals, and we then examined the interactions of those mutant TfRs with the capsids. Most substitutions had little effect on virus binding and uptake. However, mutations of several sites in the apical domain of the receptor either prevented binding to the capsids or reduced the affinity of receptor binding to various degrees. Glycans within the virus binding face of the apical domain also controlled capsid binding. CPV, but not the related feline parvovirus, could use receptors containing a canine TfR-specific glycosylation to mediate efficient infection, while addition of other N-linked glycosylation sites into the virus binding face of the feline apical domain reduced or eliminated both binding and infection. Replacement of critical feline TfR residue 221 with every amino acid had effects on binding and infection which were significantly associated with the biochemical properties of the residue replaced. Receptors with reduced affinities mostly showed proportional changes in their ability to mediate infection. Testing feline TfR variants for their binding and uptake patterns in cells showed that low-affinity versions bound fewer capsids and also differed in attachment to the cell surface and filopodia, but transport to the perinuclear endosome was similar.

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Year:  2010        PMID: 20200243      PMCID: PMC2863798          DOI: 10.1128/JVI.02623-09

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  47 in total

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Authors:  C M Lawrence; S Ray; M Babyonyshev; R Galluser; D W Borhani; S C Harrison
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Authors:  Maija Vihinen-Ranta; Dai Wang; Wendy S Weichert; Colin R Parrish
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7.  Canine and feline parvoviruses can use human or feline transferrin receptors to bind, enter, and infect cells.

Authors:  J S Parker; W J Murphy; D Wang; S J O'Brien; C R Parrish
Journal:  J Virol       Date:  2001-04       Impact factor: 5.103

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  23 in total

1.  Role of multiple hosts in the cross-species transmission and emergence of a pandemic parvovirus.

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Review 2.  Crossing the Iron Gate: Why and How Transferrin Receptors Mediate Viral Entry.

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Review 4.  Parvovirus glycan interactions.

Authors:  Lin-Ya Huang; Sujata Halder; Mavis Agbandje-McKenna
Journal:  Curr Opin Virol       Date:  2014-07-19       Impact factor: 7.090

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Authors:  Heather M Callaway; Kurtis H Feng; Donald W Lee; Andrew B Allison; Melissa Pinard; Robert McKenna; Mavis Agbandje-McKenna; Susan Hafenstein; Colin R Parrish
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6.  Permissivity of Dipeptidyl Peptidase 4 Orthologs to Middle East Respiratory Syndrome Coronavirus Is Governed by Glycosylation and Other Complex Determinants.

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7.  Transferrin receptor binds virus capsid with dynamic motion.

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8.  Select membrane proteins modulate MNV-1 infection of macrophages and dendritic cells in a cell type-specific manner.

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9.  Complex and Dynamic Interactions between Parvovirus Capsids, Transferrin Receptors, and Antibodies Control Cell Infection and Host Range.

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Journal:  J Virol       Date:  2018-06-13       Impact factor: 5.103

10.  Parvovirus particles and movement in the cellular cytoplasm and effects of the cytoskeleton.

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