Structural basis for murine norovirus engagement of bile acids and the CD300lf receptor

被引:86
作者
Nelson, Christopher A. [1 ]
Wilen, Craig B. [1 ,5 ,6 ]
Dai, Ya-Nan [1 ]
Orchard, Robert C. [1 ,7 ]
Kim, Arthur S. [1 ]
Stegeman, Roderick A. [1 ]
Hsieh, Leon L. [1 ]
Smith, Thomas J. [2 ]
Virgin, Herbert W. [1 ,3 ,8 ]
Fremont, Daved H. [1 ,3 ,4 ]
机构
[1] Washington Univ, Sch Med, Dept Pathol & Immunol, St Louis, MO 63110 USA
[2] Univ Texas Med Branch, Dept Biochem & Mol Biol, Galveston, TX 77555 USA
[3] Washington Univ, Sch Med, Dept Mol Microbiol, St Louis, MO 63110 USA
[4] Washington Univ, Sch Med, Dept Biochem & Mol Biophys, St Louis, MO 63110 USA
[5] Yale Univ, Dept Lab Med, New Haven, CT 06520 USA
[6] Yale Univ, Dept Immunobiol, New Haven, CT 06520 USA
[7] Univ Texas Southwestern Med Ctr Dallas, Dept Immunol, Dallas, TX 75390 USA
[8] Vir Biotechnol, San Francisco, CA 94158 USA
关键词
norovirus; virus receptor; bile acid; crystallography; CAPSID PROTEIN; P2; DOMAIN; MONOCLONAL-ANTIBODIES; FUNCTIONAL RECEPTOR; BINDING; FLEXIBILITY; TROPISM; PHOSPHATIDYLSERINE; IDENTIFICATION; REPLICATION;
D O I
10.1073/pnas.1805797115
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Murine norovirus (MNoV) is closely related to human norovirus (HNoV), an infectious agent responsible for acute gastroenteritis worldwide. Here we report the X-ray crystal structure of the dimeric MNoV VP1 protruding (P) domain in complex with its cellular receptor CD300lf. CD300lf binds the P domain with a 2: 2 stoichiometry, engaging a cleft between the AB and DE loops of the P2 subdomain at a site that overlaps the epitopes of neutralizing antibodies. We also identify that bile acids are cofactors enhancing MNoV cell-binding and infectivity. Structures of CD300lf-P domain in complex with glycoche-nodeoxycholic acid (GCDCA) and lithocholic acid (LCA) reveal two bile acid binding sites at the P domain dimer interface distant from receptor binding sites. The structural determinants for receptor and bile acid binding are supported by numerous biophysical assays utilizing interface residue mutations. We find that the monomeric affinity of CD300lf for the P domain is low and is divalent cation dependent. We have also determined the crystal structure of CD300lf in complex with phosphocholine, revealing that MNoV engages its receptor in a manner mimicking host ligands including similar metal coordination. Docking of the cocomplex structures onto a cryo-EM-derivedmodel of MNoV suggests that each virion can make multiple CD300lf engagements, and thus, infection may be driven by the avidity of cell surface clustered CD300lf. These studies identify multiple potential modulators of norovirus infection that may act to regulate the interaction between the viral capsid P domain and its cognate cellular receptor.
引用
收藏
页码:E9201 / E9210
页数:10
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