VACCINIA VIRUS MUC1 IMMUNIZATION OF MICE - IMMUNE-RESPONSE AND PROTECTION AGAINST THE GROWTH OF MURINE TUMORS BEARING THE MUC1 ANTIGEN

被引:82
|
作者
ACRES, RB
HAREUVENI, M
BALLOUL, JM
KIENY, MP
机构
[1] TEL AVIV UNIV, DEPT CELL RES, IL-69978 TEL AVIV, ISRAEL
[2] TEL AVIV UNIV, DEPT CELL RES & IMMUNOL, IL-69978 TEL AVIV, ISRAEL
关键词
MUC1; TUMOR IMMUNIZATION; MURINE TUMOR MODEL; VACCINIA VIRUS TUMOR ANTIGEN;
D O I
10.1097/00002371-199308000-00009
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
MUC1 is a mucin found on the apical surfaces of some normal mammalian mucin-secreting cells. It is characterized by heavy glycosylation and a 20-amino-acid tandem repeat segment. In most cases of human breast adenocarcinoma, this antigen is overexpressed. Moreover, abnormal glycosylation exposes a novel peptide epitope within the tandem repeat, such that antibodies to this epitope can distinguish normal from malignant adenocarcinomatous breast tissue. We have constructed a vaccinia virus (VV) that carries the cDNA for the MUC1 antigen. Murine and human cells infected with this virus express the MUC1 molecule, with three to four tandem repeats per molecule and with the tumor-associated epitopes exposed. Mice immunized with this virus produce antibodies that recognize MUC1 outside the tandem repeat, within the tandem repeat, and within the tumor-associated protein core epitope. Tumorogenic P815 (DBA) and 3T3 (BALB/c) cells have been transfected with MUC1. Thirty percent of DBA mice immunized with VV-MUC1 are protected from growth of P815-MUC1 tumors when implanted with 10(5) cells. Immunized BALB/c mice show a late development of transfected 3T3 tumor cells. Immunized mice show a moderate MUC1-specific IgG titer, but it cannot be correlated with subsequent tumor rejection. No evidence for a MUC1-specific cytotoxic T lymphocyte response has been found after immunization with VV-MUC1.
引用
收藏
页码:136 / 143
页数:8
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