| Literature DB >> 28875379 |
Lena-Christin Conradi1,2, Aleksandra Brajic1,2, Anna Rita Cantelmo1,2, Ann Bouché1,2, Joanna Kalucka1,2, Andreas Pircher1,2, Ulrike Brüning1,2, Laure-Anne Teuwen1,2, Stefan Vinckier1,2, Bart Ghesquière3,4, Mieke Dewerchin1,2, Peter Carmeliet5,6.
Abstract
Blockade of the glycolytic activator PFKFB3 in cancer cells (using a maximum tolerable dose of 70 mg/kg of the PFKFB3 blocker 3PO) inhibits tumor growth in preclinical models and is currently being tested as a novel anticancer treatment in phase I clinical trials. However, a detailed preclinical analysis of the effects of such maximum tolerable dose of a PFKFB3 blocker on the tumor vasculature is lacking, even though tumor endothelial cells are hyper-glycolytic. We report here that a high dose of 3PO (70 mg/kg), which inhibits cancer cell proliferation and reduces primary tumor growth, causes tumor vessel disintegration, suppresses endothelial cell growth for protracted periods, (model-dependently) aggravates tumor hypoxia, and compromises vascular barrier integrity, thereby rendering tumor vessels more leaky and facilitating cancer cell intravasation and dissemination. These findings contrast to the effects of a low dose of 3PO (25 mg/kg), which induces tumor vessel normalization, characterized by vascular barrier tightening and maturation, but reduces cancer cell intravasation and metastasis. Our findings highlight the importance of adequately dosing a glycolytic inhibitor for anticancer treatment.Entities:
Keywords: Angiogenesis; Anti-angiogenic therapy; Glycolysis; Metabolism; PFKFB3
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Year: 2017 PMID: 28875379 DOI: 10.1007/s10456-017-9573-6
Source DB: PubMed Journal: Angiogenesis ISSN: 0969-6970 Impact factor: 9.596