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Structural basis of oligosaccharide receptor recognition by human papillomavirus.


ABSTRACT: High risk human papillomavirus types 16 (HPV16) and 18 (HPV18) can cause cervical cancer. Efficient infection by HPV16 and HPV18 pseudovirions requires interactions of particles with cell-surface receptor heparan sulfate oligosaccharide. To understand the virus-receptor interactions for HPV infection, we determined the crystal structures of HPV16 and HPV18 capsids bound to the oligosaccharide receptor fragment using oligomeric heparin. The HPV-heparin structures revealed multiple binding sites for the highly negatively charged oligosaccharide fragment on the capsid surface, which is different from previously reported virus-receptor interactions in which a single type of binding pocket is present for a particular receptor. We performed structure-guided mutagenesis to generate mutant viruses, and cell binding and infectivity assays demonstrated the functional role of viral residues involved in heparin binding. These results provide a basis for understanding virus-heparan sulfate receptor interactions critical for HPV infection and for the potential development of inhibitors against HPV infection.

SUBMITTER: Dasgupta J 

PROVIDER: S-EPMC3024757 | biostudies-literature | 2011 Jan

REPOSITORIES: biostudies-literature

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Structural basis of oligosaccharide receptor recognition by human papillomavirus.

Dasgupta Jhimli J   Bienkowska-Haba Malgorzata M   Ortega Marcos E ME   Patel Hetalkumar D HD   Bodevin Sabrina S   Spillmann Dorothe D   Bishop Brooke B   Sapp Martin M   Chen Xiaojiang S XS  

The Journal of biological chemistry 20101129 4


High risk human papillomavirus types 16 (HPV16) and 18 (HPV18) can cause cervical cancer. Efficient infection by HPV16 and HPV18 pseudovirions requires interactions of particles with cell-surface receptor heparan sulfate oligosaccharide. To understand the virus-receptor interactions for HPV infection, we determined the crystal structures of HPV16 and HPV18 capsids bound to the oligosaccharide receptor fragment using oligomeric heparin. The HPV-heparin structures revealed multiple binding sites f  ...[more]

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