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SEROTYPING HIV TYPE-1 BY ANTIBODY-BINDING TO THE V3 LOOP - RELATIONSHIP TO VIRAL GENOTYPE

被引:88
作者
CHEINGSONGPOPOV, R
LISTER, S
CALLOW, D
KALEEBU, P
BEDDOWS, S
WEBER, J
OSMANOV, S
BELSEY, EM
HEYWARD, W
ESPARZA, J
GALVAOCASTRO, B
VANDEPERRE, P
KARITA, E
WASI, C
SEMPALA, S
TUGUME, B
BIRYAHWAHO, B
RUBSAMENWAIGMANN, H
VONBRIESEN, H
ESSER, R
GREZ, M
HOLMES, H
NEWBERRY, A
RANJBAR, S
TOMLINSON, P
BRADAC, J
MCCUTCHAN, F
LOUWAGIE, J
HEGERICH, P
LOPEZGALINDEZ, C
OLIVARES, I
DOPAZO, J
MULLINS, JI
DELWART, EL
BACHMANN, HM
GOUDSMIT, J
DEWOLF, F
HAHN, BH
GAO, F
YUE, L
SARAGOSTI, S
SCHOCHETMAN, G
KALISH, M
LUO, CC
GEORGE, R
PAU, CP
NARA, P
FENYO, EM
ALBERT, J
MYERS, G
机构
[1] WHO,GLOBAL PROGRAMME AIDS,WHO NETWORK HIV ISOLAT & CHARACT,CH-1211 GENEVA,SWITZERLAND
[2] GEORG SPEYER HAUS CHEMOTHERAPEUT FORSCHUNGSINST,FRANKFURT,GERMANY
[3] NATL INST BIOL STAND & CONTROLS,LONDON NW3 6RB,ENGLAND
[4] NIAID,DIV AIDS,BETHESDA,MD 20892
[5] WALTER REED ARMY INST RES,HENRY M JACKSON FDN RES LAB,ROCKVILLE,MD
[6] INST SALUD CARLOS 3,CTR NACL BIOL CELULAR & RETROVIRUS,MADRID,SPAIN
[7] STANFORD UNIV,SCH MED,DEPT MICROBIOL & IMMUNOL,STANFORD,CA 94305
[8] UNIV AMSTERDAM,HUMAN RETROVIRUS LAB,AMSTERDAM,NETHERLANDS
[9] UNIV ALABAMA,DEPT MED,BIRMINGHAM,AL 35294
[10] INST COCHIN GENET MOLEC,F-75014 PARIS,FRANCE
[11] CTR DIS CONTROL & PREVENT,ATLANTA,GA 30341
[12] ST MARYS HOSP,SCH MED,LONDON,ENGLAND
[13] NCI,VIRUS BIOL UNIT,FREDERICK,MD 21701
[14] KAROLINSKA INST,STOCKHOLM,SWEDEN
[15] SWEDISH INST INFECT DIS CONTROL,STOCKHOLM,SWEDEN
[16] LOS ALAMOS NATL LAB,LOS ALAMOS,NM
来源
AIDS RESEARCH AND HUMAN RETROVIRUSES | 1994年 / 10卷 / 11期
关键词
D O I
10.1089/aid.1994.10.1379
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
We have investigated whether peptides representing the HIV-1 principal neutralization domain (V3) can be used as antigens in antibody-binding assays to predict the genotypes of the subjects' virus. Serum samples collected from HIV-1-infected subjects from the four WHO-sponsored vaccine evaluation sites (Uganda, Rwanda, Thailand, and Brazil) were characterized by antibody binding to a panel of synthetic V3 peptides that were derived from the consensus sequences of the V3 region of the HIV-1 subgroups according to the env phylogenetic analysis (A-E). An indirect V3 peptide-binding assay was used for primary screening, and a V3 peptide antigen-limiting ELISA was then used as a secondary assay to discriminate cross-reactivity if the screening assay was equivocal. In general, V3 peptide serology could predict HIV-1 genotypes. In sera for which the genotype of the virus was known, peptide assays could predict the correct genotype in approximately 90% of cases for genotypes A, B, C, and E; Ugandan sera of genotype D were more broadly reactive. There was considerable serological cross-reactivity between some HIV-1 genotypes, in particular between A and C, and, to a lesser extent, B and D subtypes. Owing to polymorphism at the crown of the V3 loop, an additional B peptide (B') was required to type Brazilian B genotype sera. These simple assays may help facilitate the determination and distribution of HIV-1 genotypes circulating in populations.
引用
收藏
页码:1379 / 1386
页数:8
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