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HUMAN AND MURINE MONOCLONAL-ANTIBODIES DIRECTED AGAINST A CONSERVED SEQUENCE FROM GP41 (AA583-599) OF HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1

被引:9
作者
EBERSOLD, A
BOYER, V
KLASSE, PJ
HOLNIGUE, M
FRAISIER, C
COCCHI, JM
PIPKORN, R
BLOMBERG, J
DESGRANGES, C
机构
[1] UNIV LUND,VIROL SECT,S-22101 LUND,SWEDEN
[2] CTR REG TRANSFUS SANGUINE,F-59000 LILLE,FRANCE
[3] NOVABIOCHEM AG,HEIDELBERG,GERMANY
来源
RESEARCH IN VIROLOGY | 1992年 / 143卷 / 03期
关键词
LYMPHOCYTE; PEPTIDE; HIV; AIDS; MAB; IGM; IMMUNOTHERAPY; GP41; IMMUNOSUPPRESSION; SYNCYTIA; PHIVIS; HEPTALYSINE;
D O I
10.1016/S0923-2516(06)80102-0
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
Human spleen cells from an HIV-seropositive donor were immunized in vitro with the aa583-599 peptide conjugated to an heptalysyl core. This sequence was derived from the putatively HIV-immunosuppressive region of HIV1 gp41. The same conjugated peptide was used to immunize mice. One human and one mouse IgM monoclonal antibody (mAb) directed against the aa583-599 peptide were obtained. The two mAb had distinct patterns of reactivity against a panel of 42 peptides with modified sequences. Neither of the mAb inhibited the immunosuppressive effect of aa583-599 octopus-lys-conjugated peptide on anti-CD3 Ab-induced lymphoproliferation. In addition, both mAb did not neutralize cell-free virus transmission or enhance HIV infection. However, HmAb inhibited formation of syncytia between HIV 1 -infected (but not HIV2-infected cells) and non-infected target cells at concentrations above 20-mu-g/ml, whereas MmAb did not have any effect. The degree of conservation of the aa583-599 region makes HmAb a candidate for use as a group-specific reagent in future HIV1 passive immunotherapy protocols.
引用
收藏
页码:179 / 191
页数:13
相关论文
共 31 条
[1]   HUMAN MONOCLONAL-ANTIBODIES PRODUCED BY PRIMARY INVITRO IMMUNIZATION OF PERIPHERAL-BLOOD LYMPHOCYTES [J].
BORREBAECK, CAK ;
DANIELSSON, L ;
MOLLER, SA .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1988, 85 (11) :3995-3999
[2]  
BOYER V, 1991, CLIN EXP IMMUNOL, V83, P452
[3]   ANTIBODY RAISED AGAINST SOLUBLE CD4-RGP120 COMPLEX RECOGNIZES THE CD4 MOIETY AND BLOCKS MEMBRANE-FUSION WITHOUT INHIBITING CD4-GP120 BINDING [J].
CELADA, F ;
CAMBIAGGI, C ;
MACCARI, J ;
BURASTERO, S ;
GREGORY, T ;
PATZER, E ;
PORTER, J ;
MCDANAL, C ;
MATTHEWS, T .
JOURNAL OF EXPERIMENTAL MEDICINE, 1990, 172 (04) :1143-1150
[4]   ANTIBODIES TO A PUTATIVE HIV GP41 IMMUNOSUPPRESSIVE PEPTIDE, PHIVIS (583-599), DO NOT CORRELATE SIGNIFICANTLY WITH OUTCOME IN HIV-INFECTION [J].
CHEINGSONGPOPOV, R ;
PANAGIOTIDI, C ;
CAUN, K ;
KLASSE, PJ ;
PIPKORN, R ;
BLOMBERG, J ;
WEBER, J .
AIDS, 1990, 4 (03) :251-253
[5]   HUMAN RETROVIRUS-RELATED SYNTHETIC PEPTIDES INHIBIT LYMPHOCYTE-T PROLIFERATION [J].
CIANCIOLO, GJ ;
BOGERD, H ;
SNYDERMAN, R .
IMMUNOLOGY LETTERS, 1988, 19 (01) :7-13
[6]   RAT MONOCLONAL-ANTIBODIES TO NONOVERLAPPING EPITOPES OF HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 GP120 BLOCK CD4 BINDING INVITRO [J].
CORDELL, J ;
MOORE, JP ;
DEAN, CJ ;
KLASSE, PJ ;
WEISS, RA ;
MCKEATING, JA .
VIROLOGY, 1991, 185 (01) :72-79
[7]   NEUTRALIZATION OF DIVERSE HIV-1 STRAINS BY MONOCLONAL-ANTIBODIES RAISED AGAINST A GP41 SYNTHETIC PEPTIDE [J].
DALGLEISH, AG ;
CHANH, TC ;
KENNEDY, RC ;
KANDA, P ;
CLAPHAM, PR ;
WEISS, RA .
VIROLOGY, 1988, 165 (01) :209-215
[8]   FINE MAPPING OF AN IMMUNODOMINANT REGION OF THE TRANSMEMBRANE PROTEIN OF THE HUMAN IMMUNODEFICIENCY VIRUS (HIV-1) [J].
DOPEL, SH ;
PORSTMANN, T ;
HENKLEIN, P ;
VONBAEHR, R .
JOURNAL OF VIROLOGICAL METHODS, 1989, 25 (02) :167-178
[9]   HIV-1 NEUTRALIZING MONOCLONAL-ANTIBODIES INDUCED BY A SYNTHETIC PEPTIDE [J].
DURDA, PJ ;
BACHELER, L ;
CLAPHAM, P ;
JENOSKI, AM ;
LEECE, B ;
MATTHEWS, TJ ;
MCKNIGHT, A ;
POMERANTZ, R ;
RAYNER, M ;
WEINHOLD, KJ .
AIDS RESEARCH AND HUMAN RETROVIRUSES, 1990, 6 (09) :1115-1123
[10]  
HAMMOND SA, 1991, J IMMUNOL, V146, P1470
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