A HUMAN MONOCLONAL-ANTIBODY AGAINST VARICELLA-ZOSTER VIRUS GLYCOPROTEIN-III

被引:26
|
作者
SUGANO, T
TOMIYAMA, T
MATSUMOTO, Y
SASAKI, S
KIMURA, T
FORGHANI, B
MASUHO, Y
机构
[1] TEIJIN INST BIOMED RES, ASAHIGAOKA 4-3-2, HINO, TOKYO 191, JAPAN
[2] STATE CALIF DEPT HLTH SERV, DIV LABS, RICKETTSIAL DIS LAB, BERKELEY, CA 94704 USA
来源
关键词
D O I
10.1099/0022-1317-72-9-2065
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
Hybridomas producing human monoclonal antibodies (HMAbs) against varicella-zoster virus (VZV) were generated by fusing murine myeloma cells with human lymphocytes immunized in vitro. An assay system was developed to select anti-glycoprotein (gp)III HMAbs from the pool of anti-VZV HMAbs. A murine anti-gpIII MAb, 4B7, did not react with a VZV-infected cell homogenate, but did react with a VZV-infected cell monolayer, whereas anti-gpI and anti-gpII MAbs reacted with both antigens. Hybridomas were screened to obtain HMAbs having a reaction profile similar to that of 4B7 and one such clone, V3, stably produces human IgG1 (kappa). HMAb V3 immunoprecipitated a VZV antigen of 115K to 120K, which was not immunoabsorbed by an anti-gpII HMAb, implying that V3 recognizes gpIII. V3 neutralized VZV independently of complement, unlike anti-gpI and anti-gpII HMAbs. All five strains of VZV tested were completely neutralized by V3, and the dose of V3 required to reduce the number of virus plaques by 50% ranged from 0.027 to 0.15-mu-g/ml. V3 was also able to inhibit the spread of virus infection from infected to uninfected cells, whereas anti-gpI and anti-gpII HMAbs could not. In addition, V3 mediated antibody-dependent cellular cytotoxicity but not complement-dependent cytotoxicity of VZV-infected cells. The results suggest that an anti-gpIII HMAb may provide a new means of passive immunoprophylaxis and also help to identify an antigenic epitope appropriate for a subunit vaccine.
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页码:2065 / 2073
页数:9
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