Dengue virus infectivity depends on envelope protein binding to target cell heparan sulfate

被引:0
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作者
Yaping Chen
Terry Maguire
Ronald E. Hileman
Jonathan R. Fromm
Jeffrey D. Esko
Robert J. Linhardt
Rory M. Marks
机构
[1] University of Michigan,Division of Rheumatology, Department of Internal Medicine
[2] Health Research Council of New Zealand's Virus Research Group and Centre for Gene Research,Division of Medicinal and Natural Products Chemistry and Department of Chemical and Biochemical Engineering
[3] University of Otago,Division of Cellular and Molecular Medicine Glycobiology Program
[4] University of Iowa,undefined
[5] UCSD Cancer Center,undefined
[6] University of California San Diego,undefined
来源
Nature Medicine | 1997年 / 3卷
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摘要
Dengue virus is a human pathogen that has reemerged as an increasingly important public health threat. We found that the cellular receptor utilized by dengue envelope protein to bind to target cells is a highly sulfated type of heparan sulfate. Heparin, highly sulfated heparan sulfate, and the polysulfonate pharmaceutical Suramin effectively prevented dengue virus infection of target cells, indicating that the envelope protein-target cell receptor interaction is a critical determinant of infectivity. The dengue envelope protein sequence includes two putative glycosaminoglycan-binding motifs at the carboxy terminus; the first could be structurally modeled and formed an unusual extended binding surface of basic amino acids. Similar motifs were also identified in the envelope proteins of other flaviviridae. Developing pharmaceuticals that inhibit target cell binding may be an effective strategy for treating flavivirus infections.
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页码:866 / 871
页数:5
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