Abstract |
Many viruses initiate interaction with target cells by binding to cell surface glycosaminoglycans (GAGs). Heparan sulfate (HS) appears to be particularly important in fibroblasts, epithelial cells and endothelial cells, where it represents the dominant GAG. How GAGs influence viral infectivity in HS-poor target cells such as macrophages has not been clearly defined. Here, we show that mouse cytomegalovirus (MCMV) targets HS in susceptible fibroblasts and cultured salivary gland acinar cells (SGACs), but not in macrophage cell lines and primary bone marrow-derived macrophages, where chondroitin sulfate was the dominant virus-binding GAG. MCK-2, an MCMV-encoded GAG-binding chemokine that promotes infection of macrophages as part of a gH/gL/MCK-2 entry complex, was dispensable for MCMV attachment to the cell surface and for direct infection of SGACs. Thus, MCMV tropism for target cells is markedly influenced by differential GAG expression, suggesting that the specificity of anti-GAG peptides now under development as HCMV therapeutics may need to be broadened for effective application as anti-viral agents.
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Authors | Sergio M Pontejo, Philip M Murphy |
Journal | Viruses
(Viruses)
Vol. 12
Issue 1
(12 27 2019)
ISSN: 1999-4915 [Electronic] Switzerland |
PMID | 31892128
(Publication Type: Journal Article, Research Support, N.I.H., Intramural)
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Chemical References |
- Chemokines, CC
- MCK-2 protein, Mouse cytomegalovirus 1
- Viral Proteins
- Chondroitin Sulfates
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Topics |
- Animals
- Cell Line
- Chemokines, CC
(genetics, immunology)
- Chondroitin Sulfates
(metabolism)
- Fibroblasts
(virology)
- Host Microbial Interactions
- Macrophages
(virology)
- Mice
- Mice, Inbred BALB C
- Muromegalovirus
(physiology)
- RAW 264.7 Cells
- Viral Proteins
(genetics, immunology, metabolism)
- Viral Tropism
- Virus Internalization
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