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INDUCTION OF VASCULAR ENDOTHELIAL TUBULAR MORPHOGENESIS BY HUMAN GLIOMA-CELLS - A MODEL SYSTEM FOR TUMOR ANGIOGENESIS

被引:87
作者
ABE, T
OKAMURA, K
ONO, M
KOHNO, K
MORI, T
HORI, S
KUWANO, M
机构
[1] KYUSHU UNIV, SCH MED, DEPT BIOCHEM, FUKUOKA 812, JAPAN
[2] OITA MED UNIV, DEPT BIOCHEM, OTTA 87955, JAPAN
[3] OITA MED UNIV, DEPT NEUROSURG, OITA 87955, JAPAN
来源
JOURNAL OF CLINICAL INVESTIGATION | 1993年 / 92卷 / 01期
关键词
TUMOR ANGIOGENESIS; HUMAN GLIOMA CELLS; TUBULAR MORPHOGENESIS; BASIC FIBROBLAST GROWTH FACTOR; BOVINE AORTIC ENDOTHELIAL CELLS;
D O I
10.1172/JCI116599
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
We have developed two different models of tumor angiogenesis by human brain tumors: one being tube formation by bovine aortic endothelial (BAE) cells cocultured with tumor cells in vitro, and other being in vivo angiogenesis in mice when tumor cells are transplanted into the dorsal sac. We investigated whether tube formation could be induced in BAE cells in type I collagen gel when these cells were cocultured with seven human glioma cell lines. Four of the seven glioma cell lines, which had high levels of basic fibroblast growth factor (BFGF) MRNA, induced tube formation by BAE cells. The tube formation was blocked by coadministration of anti-BFGF antibody. In vivo model system of tumor angiogenesis in mice, these four cell lines were highly angiogenic. In contrast, with the other three glioma cell lines, which had poor expression of BFGF, BAE cells showed no apparent tube formation. These three cell lines did not efficiently develop capillary networks in mice. The results demonstrated a correlative relationship in the tubulogenesis of BAE cells, BFGF MRNA levels and angiogenesis in mice. The present study with two model systems of tumor angiogenesis suggests that the angiogenesis of some human glioma cell lines is mediated by BFGF, possibly via paracrine control.
引用
收藏
页码:54 / 61
页数:8
相关论文
共 48 条
[1]   A NEW CLASS OF STEROIDS INHIBITS ANGIOGENESIS IN THE PRESENCE OF HEPARIN OR A HEPARIN FRAGMENT [J].
CRUM, R ;
SZABO, S ;
FOLKMAN, J .
SCIENCE, 1985, 230 (4732) :1375-1378
[2]   MODES OF FGF RELEASE INVIVO AND INVITRO [J].
DAMORE, PA .
CANCER AND METASTASIS REVIEWS, 1990, 9 (03) :227-238
[3]  
DELARCO JE, 1978, P NATL ACAD SCI USA, V75, P4001
[4]   TRANSFORMING GROWTH FACTOR-ALPHA [J].
DERYNCK, R .
CELL, 1988, 54 (05) :593-595
[5]   HUMAN TRANSFORMING GROWTH FACTOR-BETA COMPLEMENTARY-DNA SEQUENCE AND EXPRESSION IN NORMAL AND TRANSFORMED-CELLS [J].
DERYNCK, R ;
JARRETT, JA ;
CHEN, EY ;
EATON, DH ;
BELL, JR ;
ASSOIAN, RK ;
ROBERTS, AB ;
SPORN, MB ;
GOEDDEL, DV .
NATURE, 1985, 316 (6030) :701-705
[6]   INDUCTION OF ANGIOGENESIS DURING THE TRANSITION FROM HYPERPLASIA TO NEOPLASIA [J].
FOLKMAN, J ;
WATSON, K ;
INGBER, D ;
HANAHAN, D .
NATURE, 1989, 339 (6219) :58-61
[7]   ANGIOGENIC FACTORS [J].
FOLKMAN, J ;
KLAGSBRUN, M .
SCIENCE, 1987, 235 (4787) :442-447
[8]   WHAT IS THE EVIDENCE THAT TUMORS ARE ANGIOGENESIS DEPENDENT [J].
FOLKMAN, J .
JNCI-JOURNAL OF THE NATIONAL CANCER INSTITUTE, 1990, 82 (01) :4-6
[9]   ISOLATION OF PITUITARY FIBROBLAST GROWTH-FACTOR BY FAST PROTEIN LIQUID-CHROMATOGRAPHY (FPLC) - PARTIAL CHEMICAL AND BIOLOGICAL CHARACTERIZATION [J].
GOSPODAROWICZ, D ;
MASSOGLIA, S ;
CHENG, J ;
LUI, GM ;
BOHLEN, P .
JOURNAL OF CELLULAR PHYSIOLOGY, 1985, 122 (02) :323-332
[10]   MOLECULAR AND BIOLOGICAL CHARACTERIZATION OF FIBROBLAST GROWTH-FACTOR, AN ANGIOGENIC FACTOR WHICH ALSO CONTROLS THE PROLIFERATION AND DIFFERENTIATION OF MESODERM AND NEUROECTODERM DERIVED CELLS [J].
GOSPODAROWICZ, D ;
NEUFELD, G ;
SCHWEIGERER, L .
CELL DIFFERENTIATION, 1986, 19 (01) :1-17
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