MECHANISM OF ANGIOGENIC EFFECTS OF SAPONIN FROM GINSENG RADIX-RUBRA IN HUMAN UMBILICAL VEIN ENDOTHELIAL-CELLS

被引：53

作者：

MORISAKI, N ^{[1
]}

WATANABE, S ^{[1
]}

TEZUKA, M ^{[1
]}

ZENIBAYASHI, M ^{[1
]}

SHIINA, R ^{[1
]}

KOYAMA, N ^{[1
]}

KANZAKI, T ^{[1
]}

SAITO, Y ^{[1
]}

机构：

[1] YAMAGATA UNIV,SCH MED,DEPT LAB MED,YAMAGATA 99023,JAPAN

来源：

BRITISH JOURNAL OF PHARMACOLOGY | 1995年 / 115卷 / 07期

关键词：

GINSENG; SAPONIN; ANGIOGENESIS; TISSUE-TYPE PLASMINOGEN ACTIVATOR; PLASMINOGEN ACTIVATOR INHIBITOR-1; PROLIFERATION; MIGRATION; ENDOTHELIAL CELLS; WOUND HEALING;

D O I：

10.1111/j.1476-5381.1995.tb15023.x

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

1 The effects of saponin from Ginseng Radix rubra on angiogenesis (tube formation) and its key steps (protease secretion, proliferation and migration) in human umbilical vein endothelial cells (HUVEC) were examined to elucidate the mechanism of the tissue repairing effects of Ginseng Radix rubra. The effect on a wound healing model was also studied. 2 Tube formation was measured by an in vitro system. The activity and immunoreactivity of tissue-type plasminogen activator OPA) as a protease for angiogenesis and the immunoreactivity of its inhibitor, plasminogen activator inhibitor-1 (PAI-1), were measured in conditioned medium of HUVEC stimulated for 24 h with saponin. Cell proliferation was measured by counting the cell numbers at 2-7 days after seeding. Migration was measured by Boyden's chamber method. The effect on wound healing was studied in the skin of diabetic rats. 3 Saponin at 10-100 mu g ml(-1) significantly stimulated tube formation by HUVEC in a dose-dependent manner. Saponin in a similar concentration-range increased the secretion of tPA from HUVEC as estimated by immunoreactivity and enzyme activity. On the other hand, PAI-1 immunoreactivity was slightly increased at 10 mu g ml(-1) of saponin, but then was significantly decreased at 50 and 100 mu g ml(-1). Cell proliferation was only slightly enhanced by 1-100 mu g ml(-1) of saponin, but migration was significantly enhanced by 10-100 mu ml(-1) in a dose-dependent manner. Moreover, saponin stimulated wound healing with enhanced angiogenesis in vivo. 4 These results indicate that saponin stimulates tube formation mainly by modifying the balance of protease/protease inhibitor secretion from HUVEC and enhancing the migration of HUVEC, and that it is effective in vivo.

引用

页码：1188 / 1193

页数：6

共 30 条

[1] THE HEPARIN-BINDING (FIBROBLAST) GROWTH-FACTOR FAMILY OF PROTEINS [J].

BURGESS, WH ;

MACIAG, T .

ANNUAL REVIEW OF BIOCHEMISTRY, 1989, 58 :575-606

[2]

Cawston T.E., 1986, PROTEINASE INHIBITOR, P589

[3] DETERMINATION OF PLASMINOGEN-ACTIVATOR INHIBITOR IN PLASMA USING T-PA AND A CHROMOGENIC SINGLE-POINT POLY-D-LYSINE STIMULATED ASSAY [J].

ERIKSSON, E ;

RANBY, M ;

GYZANDER, E ;

RISBERG, B .

THROMBOSIS RESEARCH, 1988, 50 (01) :91-101

[4] PRIMARY STRUCTURE OF BOVINE PITUITARY BASIC FIBROBLAST GROWTH-FACTOR (FGF) AND COMPARISON WITH THE AMINO-TERMINAL SEQUENCE OF BOVINE BRAIN ACIDIC FGF [J].

ESCH, F ;

BAIRD, A ;

LING, N ;

UENO, N ;

HILL, F ;

DENOROY, L ;

KLEPPER, R ;

GOSPODAROWICZ, D ;

BOHLEN, P ;

GUILLEMIN, R .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1985, 82 (19) :6507-6511

[5] MOLECULAR AND BIOLOGICAL PROPERTIES OF THE VASCULAR ENDOTHELIAL GROWTH-FACTOR FAMILY OF PROTEINS [J].

FERRARA, N ;

HOUCK, K ;

JAKEMAN, L ;

LEUNG, DW .

ENDOCRINE REVIEWS, 1992, 13 (01) :18-32

[6] TUMOR-NECROSIS-FACTOR TYPE-ALPHA, A POTENT INHIBITOR OF ENDOTHELIAL-CELL GROWTH-INVITRO, IS ANGIOGENIC INVIVO [J].

FRATERSCHRODER, M ;

RISAU, W ;

HALLMANN, R ;

GAUTSCHI, P ;

BOHLEN, P .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (15) :5277-5281

[7]

JAFFE EA, 1972, J CLIN INVEST, V52, P2745

[8]

KANZAKI T, 1989, LIPIDS, V22, P704

[9] DIABETES-MELLITUS INDUCES ACCELERATED-GROWTH OF AORTIC SMOOTH-MUSCLE CELLS - ASSOCIATION WITH OVEREXPRESSION OF PDGF BETA-RECEPTORS [J].

KAWANO, M ;

KOSHIKAWA, T ;

KANZAKI, T ;

MORISAKI, N ;

SAITO, Y ;

YOSHIDA, S .

EUROPEAN JOURNAL OF CLINICAL INVESTIGATION, 1993, 23 (02) :84-90

[10]

KITAGAWA I, 1989, CHEM PHARM BULL, V37, P2961, DOI 10.1248/cpb.37.2961

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