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Structure of the Extracellular Domain of Matrix Protein 2 of Influenza A Virus in Complex with a Protective Monoclonal Antibody

Authors
Cho, Ki JoonSchepens, BertSeok, Jong HyeonKim, SellaRoose, KennyLee, Ji-HyeGallardo, RodrigoVan Hamme, EvelienSchymkowitz, JoostRousseau, FredericFiers, WalterSaelens, XavierKim, Kyung Hyun
Issue Date
4월-2015
Publisher
AMER SOC MICROBIOLOGY
Citation
JOURNAL OF VIROLOGY, v.89, no.7, pp.3700 - 3711
Indexed
SCIE
SCOPUS
Journal Title
JOURNAL OF VIROLOGY
Volume
89
Number
7
Start Page
3700
End Page
3711
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/93951
DOI
10.1128/JVI.02576-14
ISSN
0022-538X
Abstract
The extracellular domain of influenza A virus matrix protein 2 (M2e) is conserved and is being evaluated as a quasiuniversal influenza A vaccine candidate. We describe the crystal structure at 1.6 angstrom resolution of M2e in complex with the Fab fragment of an M2e-specific monoclonal antibody that protects against influenza A virus challenge. This antibody binds M2 expressed on the surfaces of cells infected with influenza A virus. Five out of six complementary determining regions interact with M2e, and three highly conserved M2e residues are critical for this interaction. In this complex, M2e adopts a compact U-shaped conformation stabilized in the center by the highly conserved tryptophan residue in M2e. This is the first description of the three-dimensional structure of M2e. IMPORTANCE M2e of influenza A is under investigation as a universal influenza A vaccine, but its three-dimensional structure is unknown. We describe the structure of M2e stabilized with an M2e-specific monoclonal antibody that recognizes natural M2. We found that the conserved tryptophan is positioned in the center of the U-shaped structure of M2e and stabilizes its conformation. The structure also explains why previously reported in vivo escape viruses, selected with a similar monoclonal antibody, carried proline residue substitutions at position 10 in M2.
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