Polyvalent vaccines for optimal coverage of potential T-cell epitopes in global HIV-1 variants

被引:358
作者
Fischer, Will
Perkins, Simon
Theiler, James
Bhattacharya, Tanmoy
Yusim, Karina
Funkhouser, Robert
Kuiken, Carla
Haynes, Barton
Letvin, Norman L.
Walker, Bruce D.
Hahn, Beatrice H.
Korber, Bette T.
机构
[1] Los Alamos Natl Lab, Los Alamos, NM 87545 USA
[2] Santa Fe Inst, Santa Fe, NM 87501 USA
[3] Duke Univ, Dept Med, Durham, NC 27710 USA
[4] Harvard Univ, Beth Israel Deaconess Med Ctr, Boston, MA 02115 USA
[5] Harvard Univ, Massachusetts Gen Hosp, Sch Med, Charlestown, MA 02129 USA
[6] Univ Alabama, Birmingham, AL 35294 USA
关键词
D O I
10.1038/nm1461
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
HIV-1/AIDS vaccines must address the extreme diversity of HIV-1. We have designed new polyvalent vaccine antigens comprised of sets of 'mosaic' proteins, assembled from fragments of natural sequences via a computational optimization method. Mosaic proteins resemble natural proteins, and a mosaic set maximizes the coverage of potential T-cell epitopes (peptides of nine amino acids) for a viral population. We found that coverage of viral diversity using mosaics was greatly increased compared to coverage by natural-sequence vaccine candidates, for both variable and conserved proteins; for conserved HIV-1 proteins, global coverage may be feasible. For example, four mosaic proteins perfectly matched 74% of 9-amino-acid potential epitopes in global Gag sequences; 87% of potential epitopes matched at least 8 of 9 positions. In contrast, a single natural Gag protein covered only 37% (9 of 9) and 67% (8 of 9). Mosaics provide diversity coverage comparable to that afforded by thousands of separate peptides, but, because the fragments of natural proteins are compressed into a small number of native-like proteins, they are tractable for vaccines.
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收藏
页码:100 / 106
页数:7
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