SUPPRESSION OF TUMOR-GROWTH AND METASTASIS OF MURINE RENAL ADENOCARCINOMA BY SYNGENEIC FIBROBLASTS GENETICALLY-ENGINEERED TO SECRETE THE JE/MCP-1 CYTOKINE

被引：30

作者：

HUANG, SY ^{[1
]}

XIE, KP ^{[1
]}

SINGH, RK ^{[1
]}

GUTMAN, M ^{[1
]}

BARELI, M ^{[1
]}

机构：

[1] UNIV TEXAS,MD ANDERSON CANCER CTR,DEPT CELL BIOL,HOUSTON,TX 77030

来源：

JOURNAL OF INTERFERON AND CYTOKINE RESEARCH | 1995年 / 15卷 / 07期

关键词：

D O I：

10.1089/jir.1995.15.655

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The murine monocyte chemoattractant protein 1, JE/MCP-1, like its human counterpart monocyte chemotactic and activating factor (MCAF), attracts monocytes-macrophages to tumor tissues, In previous studies we reported that expression of the JE/MCP-1 gene in murine colon carcinoma cells reduced their tumorigenicity and suppressed their metastatic potential, We now demonstrate that the growth and metastasis of the renal adenocarcinoma cell line RENCA are reduced when it was admired with syngeneic fibroblasts engineered to secrete the JE/MCP-1 cytokine before injection. Culture supernatants of JE/MCP-1-expressing cells plus lipopolysaccharide (LPS) synergistically activated tumoricidal properties in syngeneic macrophages against RENCA cells, This activity was blocked by anti-JE/MCP-1 antibody, indicating that JE/MCP-1 was involved in priming the macrophages to respond to LPS, Moreover, alveolar macrophages isolated shortly after iv injections of JE/MCP-1-transfected cells were cytotoxic to RENCA cells in vitro, Collectively, these data suggest that in addition to its chemotactic properties, JE/MCP-1 can synergize with bacterial endotoxins to activate macrophages, thus providing a rationale for the use of the JE/MCP-1 protein as a modality for treatment of metastasis.

引用

页码：655 / 665

页数：11

共 45 条

[1]

BARELI M, 1975, J RETICULOENDOTH SOC, V18, P317

[2] A CHEMOATTRACTANT EXPRESSED IN HUMAN SARCOMA-CELLS (TUMOR-DERIVED CHEMOTACTIC FACTOR, TDCF) IS IDENTICAL TO MONOCYTE CHEMOATTRACTANT PROTEIN-1 MONOCYTE CHEMOTACTIC AND ACTIVATING FACTOR (MCP-1/MCAF) [J].

BOTTAZZI, B ;

COLOTTA, F ;

SICA, A ;

NOBILI, N ;

MANTOVANI, A .

INTERNATIONAL JOURNAL OF CANCER, 1990, 45 (04) :795-797

[3]

BOTTAZZI B, 1992, J IMMUNOL, V148, P1280

[4] MOLECULAR-CLONING OF GENE-SEQUENCES REGULATED BY PLATELET-DERIVED GROWTH-FACTOR [J].

COCHRAN, BH ;

REFFEL, AC ;

STILES, CD .

CELL, 1983, 33 (03) :939-947

[5]

DINNEY CPN, 1991, CANCER RES, V51, P3741

[6]

FIDLER IJ, 1988, ADV DRUG DELIVERY RE, V1, P69

[7]

FOLKMAN J, 1987, SCIENCE, V235, P444

[8] CLONING AND SEQUENCING OF THE CDNA FOR HUMAN MONOCYTE CHEMOTACTIC AND ACTIVATING FACTOR (MCAF) [J].

FURUTANI, Y ;

NOMURA, H ;

NOTAKE, M ;

OYAMADA, Y ;

FUKUI, T ;

YAMADA, M ;

LARSEN, CG ;

OPPENHEIM, JJ ;

MATSUSHIMA, K .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1989, 159 (01) :249-255

[9] STUDIES ON RELATIONSHIPS BETWEEN IMMUNOGENICITY AND CATABOLISM OF ANTIGENS AND THEIR BINDING TO SURFACE OF MACROPHAGES [J].

GALLILY, R ;

BARELI, M .

EUROPEAN JOURNAL OF IMMUNOLOGY, 1976, 6 (11) :789-794

[10]

HUANG S, 1992, AM J PATHOL, V141, P981

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