INHIBITION OF METASTATIC CELL COLONIZATION IN MURINE LUNGS AND TUMOR-INDUCED MORBIDITY BY NONPEPTIDIC ARG-GLY-ASP MIMETICS

被引:41
作者
HARDAN, I
WEISS, L
HERSHKOVIZ, R
GREENSPOON, N
ALON, R
CAHALON, L
REICH, S
SLAVIN, S
LIDER, O
机构
[1] WEIZMANN INST SCI,DEPT CELL BIOL,IL-76100 REHOVOT,ISRAEL
[2] CHAIM SHEBA MED CTR,DEPT HEMATOL,IL-52621 TEL HASHOMER,ISRAEL
[3] HADASSAH MED CTR,CANC IMMUNOL LAB,JERUSALEM,ISRAEL
[4] WEIZMANN INST SCI,DEPT MEMBRANE RES & BIOPHYS,IL-76100 REHOVOT,ISRAEL
[5] WEIZMANN INST SCI,DEPT ORGAN CHEM,IL-76100 REHOVOT,ISRAEL
来源
INTERNATIONAL JOURNAL OF CANCER | 1993年 / 55卷 / 06期
关键词
D O I
10.1002/ijc.2910550624
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
The spreading and colonization of tumor cells require their migration to metastatic sites via blood vessels. To penetrate blood-vessel walls, cells, including malignant ones, must recognize and associate with the sub-endothelium extracellular matrix (ECM) and its glycoproteins. Recognition of ECM-glycoproteins, such as fibronectin (FN) and vitronectin (VN), is mediated by integrin receptors expressed on various cell types, including platelets, leukocytes and tumor cells. The Arg-Gly-Asp (RGD)-containing peptide, a major adhesive ligand of ECM, is present in various plasma and matrix glycoproteins, such as FN and VN. Non-peptidic mimetics of RGD, consisting of carboxylate and guanidinium groups of Asp and Arg divided by a linear atom spacer, express a high affinity for the alpha(IIb)-beta3 integrin and inhibit platelet aggregation. Herein, the ability of RGD mimetics to inhibit adhesive interactions between tumor cells and RGD, and tumor progression in vivo, was examined. RGD-containing peptides and the RGD mimetic, compound SF-6,5, but not the Arg-Gly-Glu (RGE) peptide or the corresponding mimetic, specifically inhibited B16-F10 melanoma cell adhesion to immobilized VN and FN. Daily administration in vivo of SF-6,S to mice inhibited the formation of B16-F10 colonies in experimental and spontaneous models of metastases. Moreover, SF-6,5 could prevent mouse death caused by massive colonization of tumor cells in the lungs. The therapeutic effect of RGD-containing peptides on tumor metastasis formation was marginal, probably due to the small amounts used, and its susceptibility to proteolysis in situ. Thus, non-peptidic mimetics of small adhesive epitopes may provide a novel therapeutic tool to prevent an adverse pathological event involving integrin-dependent cell-cell and cell-ECM interactions. (C) 199-3 Wiley-Liss, Inc.
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收藏
页码:1023 / 1028
页数:6
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