OTX008, a selective small-molecule inhibitor of galectin-1, downregulates cancer cell proliferation, invasion and tumour angiogenesis

被引:109
作者
Astorgues-Xerri, Lucile [1 ,2 ]
Riveiro, Maria E. [1 ,2 ,3 ]
Tijeras-Raballand, Annemilai [1 ,2 ]
Serova, Maria [1 ,2 ]
Rabinovich, Gabriel A. [4 ,5 ]
Bieche, Ivan [6 ]
Vidaud, Michel [6 ]
de Gramont, Armand [1 ,2 ]
Martinet, Mathieu [1 ,2 ]
Cvitkovic, Esteban [7 ]
Faivre, Sandrine [1 ,2 ]
Raymond, Eric [1 ,2 ]
机构
[1] Beaujon Univ Hosp, AP HP, PRES Paris Diderot 7, INSERM,U728, F-92110 Clichy, France
[2] Beaujon Univ Hosp, AP HP, PRES Paris Diderot 7, Dept Med Oncol, F-92110 Clichy, France
[3] Oncol Therapeut Dev, F-92110 Clichy, France
[4] Univ Buenos Aires, Lab Inmunopatol, Inst Biol & Med Expt IBYME, Consejo Nacl Invest Cient & Tecnol CONICET, Buenos Aires, DF, Argentina
[5] Univ Buenos Aires, Fac Ciencias Exactas & Nat, Dept Quim Biol, Buenos Aires, DF, Argentina
[6] Univ Paris 05, UMR745, INSERM, Fac Sci Pharmaceut & Biol, Paris, France
[7] Oncoethix, CH-1000 Lausanne, Switzerland
关键词
Galectin-1; Calixarene compounds; Anginex; Cell proliferation; Cell invasion; Neuropilin-1; ANTIANGIOGENESIS THERAPY; PROGNOSTIC-SIGNIFICANCE; LUNG-CANCER; BETA-SHEET; ANGINEX; PROGRESSION; GROWTH; EXPRESSION; RECEPTOR; PEPTIDE;
D O I
10.1016/j.ejca.2014.06.015
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background: Galectin-1 (Gal1), a carbohydrate-binding protein is implicated in cancer cell proliferation, invasion and tumour angiogenesis. Several Gal1-targeting compounds have recently emerged. OTX008 is a calixarene derivative designed to bind the Gal1 amphipathic beta-sheet conformation. Our study contributes to the current understanding of the role of Gal1 in cancer progression, providing mechanistic insights into the anti-tumoural activity of a novel small molecule Gal1-inhibitor. Methods: We evaluated in vitro OTX008 effects in a panel of human cancer cell lines. For in vivo studies, an ovarian xenograft model was employed to analyse the antitumour activity. Finally, combination studies were performed to analyse potential synergistic effects of OTX008. Results: In cultured cancer cells, OTX008 inhibited proliferation and invasion at micromolar concentrations. Antiproliferative effects correlated with Gal1 expression across a large panel of cell lines. Furthermore, cell lines expressing epithelial differentiation markers were more sensitive than mesenchymal cells to OTX008. In SQ20B and A2780-1A9 cells, OTX008 inhibited Gal1 expression and ERK1/2 and AKT-dependent survival pathways, and induced G2/M cell cycle arrest through CDK1. OTX008 enhanced the antiproliferative effects of Semaphorin-3A (Sema3A) in SQ20B cells and reversed invasion induced by exogenous Gal1. In vivo, OTX008 inhibited growth of A2780-1A9 xenografts. OTX008 treatment was associated with downregulation of Gal1 and Ki67 in treated tumours, as well as decreased microvessel density and VEGFR2 expression. Finally, combination studies showed OTX008 synergy with several cytotoxic and targeted therapies, principally when OTX008 was administered first. Conclusion: This study provides insights into the role of Gal1 in cancer progression as well as OTX008 mechanism of action, and supports its further development as an anticancer agent. (C) 2014 Elsevier Ltd. All rights reserved.
引用
收藏
页码:2463 / 2477
页数:15
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