| Literature DB >> 22245726 |
Kosuke Akiyama1, Noritaka Ohga2, Yasuhiro Hida3, Taisuke Kawamoto2, Yoshihiro Sadamoto2, Shuhei Ishikawa2, Nako Maishi2, Tomoshige Akino4, Miyako Kondoh2, Aya Matsuda5, Nobuo Inoue6, Masanobu Shindoh5, Kyoko Hida7.
Abstract
Tumor endothelial cells (TECs) are therapeutic targets in anti-angiogenic therapy. Contrary to the traditional assumption, TECs can be genetically abnormal and might also acquire drug resistance. In this study, mouse TECs and normal ECs were isolated to investigate the drug resistance of TECs and the mechanism by which it is acquired. TECs were more resistant to paclitaxel with the up-regulation of multidrug resistance (MDR) 1 mRNA, which encodes the P-glycoprotein, compared with normal ECs. Normal human microvascular ECs were cultured in tumor-conditioned medium (CM) and became more resistant to paclitaxel through MDR1 mRNA up-regulation and nuclear translocation of Y-box-binding protein 1, which is an MDR1 transcription factor. Vascular endothelial growth factor (VEGF) receptor 2 (VEGFR2) and Akt were activated in human microvascular ECs by tumor CM. We observed that tumor CM contained a significantly high level of VEGF. A VEGFR kinase inhibitor, Ki8751, and a phosphatidylinositol 3-kinase-Akt inhibitor, LY294002, blocked tumor CM-induced MDR1 up-regulation. MDR1 up-regulation, via the VEGF-VEGFR pathway in the tumor microenvironment, is one of the mechanisms of drug resistance acquired by TECs. We observed that VEGF secreted from tumors up-regulated MDR1 through the activation of VEGFR2 and Akt. This process is a novel mechanism of the acquisition of drug resistance by TECs in the tumor microenvironment. Copyright ÂEntities:
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Year: 2012 PMID: 22245726 DOI: 10.1016/j.ajpath.2011.11.029
Source DB: PubMed Journal: Am J Pathol ISSN: 0002-9440 Impact factor: 4.307