TUMOR-CELLS TRANSFECTED WITH A BACTERIAL HEAT-SHOCK GENE LOSE TUMORIGENICITY AND INDUCE PROTECTION AGAINST TUMORS

被引：81

作者：

LUKACS, KV ^{[1
]}

LOWRIE, DB ^{[1
]}

STOKES, RW ^{[1
]}

COLSTON, MJ ^{[1
]}

机构：

[1] NATL INST MED RES, LEPROSY & MYCOBACTERIAL RES, RIDGEWAY, MILL HILL, LONDON NW7 1AA, ENGLAND

来源：

JOURNAL OF EXPERIMENTAL MEDICINE | 1993年 / 178卷 / 01期

关键词：

D O I：

10.1084/jem.178.1.343

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

The gene encoding a highly immunogenic mycobacterial heat-shock protein (hsp65) was transfected into the murine macrophage tumor cell line J774. The resulting hsp65-expressing cells (J774-hsp65) were no longer able to produce tumors in syngeneic mice. This loss of tumorigenicity was not mediated through T cells since the transfected cells did not produce tumors in athymic mice. If mice are first immunized with the J774-hsp65 cells and then challenged with the parent J774 cells, the mice do not develop tumors, indicating that the presence of the mycobacterial hsp65 protein greatly enhances immunological recognition of unique structures expressed by the parent tumor cells. This is further confirmed by the demonstration in vitro of T cells derived from J774-hsp65-immunized mice that are cytotoxic for the parent J774 cells. The results provide the basis for a novel strategy for enhancing the immunological recognition and decreasing the tumorigenicity of transformed cells.

引用

页码：343 / 348

页数：6

共 34 条

[1]

ADAMS DJ, 1983, CANCER RES, V43, P4297

[2] MYCOBACTERIAL HEAT-SHOCK PROTEINS AS CARRIER MOLECULES .2. THE USE OF THE 70-KDA MYCOBACTERIAL HEAT-SHOCK PROTEIN AS CARRIER FOR CONJUGATED VACCINES CAN CIRCUMVENT THE NEED FOR ADJUVANTS AND BACILLUS-CALMETTE-GUERIN PRIMING [J].

BARRIOS, C ;

LUSSOW, AR ;

VANEMBDEN, J ;

VANDERZEE, R ;

RAPPUOLI, R ;

COSTANTINO, P ;

LOUIS, JA ;

LAMBERT, PH ;

DELGIUDICE, G .

EUROPEAN JOURNAL OF IMMUNOLOGY, 1992, 22 (06) :1365-1372

[3] SPONTANEOUS HIGH EXPRESSION OF HEAT-SHOCK PROTEINS IN MOUSE EMBRYONAL CARCINOMA-CELLS AND ECTODERM FROM DAY 8 MOUSE EMBRYO [J].

BENSAUDE, O ;

MORANGE, M .

EMBO JOURNAL, 1983, 2 (02) :173-177

[4] AUTOIMMUNITY, MICROBIAL IMMUNITY AND THE IMMUNOLOGICAL HOMUNCULUS [J].

COHEN, IR ;

YOUNG, DB .

IMMUNOLOGY TODAY, 1991, 12 (04) :105-110

[5] THE HEAT-SHOCK RESPONSE [J].

CRAIG, EA .

CRC CRITICAL REVIEWS IN BIOCHEMISTRY, 1985, 18 (03) :239-280

[6] INVIVO GENE-TRANSFER WITH RETROVIRAL VECTOR PRODUCER CELLS FOR TREATMENT OF EXPERIMENTAL BRAIN-TUMORS [J].

CULVER, KW ;

RAM, Z ;

WALLBRIDGE, S ;

ISHII, H ;

OLDFIELD, EH ;

BLAESE, RM .

SCIENCE, 1992, 256 (5063) :1550-1552

[7] INTERLEUKIN-2 PRODUCTION BY TUMOR-CELLS BYPASSES T-HELPER FUNCTION IN THE GENERATION OF AN ANTITUMOR RESPONSE [J].

FEARON, ER ;

PARDOLL, DM ;

ITAYA, T ;

GOLUMBEK, P ;

LEVITSKY, HI ;

SIMONS, JW ;

KARASUYAMA, H ;

VOGELSTEIN, B ;

FROST, P .

CELL, 1990, 60 (03) :397-403

[8] ACTIVATING MUTATIONS FOR TRANSFORMATION BY P53 PRODUCE A GENE-PRODUCT THAT FORMS AN HSC70-P53 COMPLEX WITH AN ALTERED HALF-LIFE [J].

FINLAY, CA ;

HINDS, PW ;

TAN, TH ;

ELIYAHU, D ;

OREN, M ;

LEVINE, AJ .

MOLECULAR AND CELLULAR BIOLOGY, 1988, 8 (02) :531-539

[9] HIGH-FREQUENCY OF CORD BLOOD-LYMPHOCYTES AGAINST MYCOBACTERIAL 65-KDA HEAT-SHOCK PROTEIN [J].

FISCHER, HP ;

SHARROCK, CEM ;

PANAYI, GS .

EUROPEAN JOURNAL OF IMMUNOLOGY, 1992, 22 (06) :1667-1669

[10]

FUQUA SAW, 1989, CANCER RES, V49, P4126

← 1 2 3 4 →