| Literature DB >> 23356224 |
Kosuke Akiyama1, Noritaka Ohga, Nako Maishi, Yasuhiro Hida, Kazuko Kitayama, Taisuke Kawamoto, Takahiro Osawa, Yuko Suzuki, Nobuo Shinohara, Katsuya Nonomura, Masanobu Shindoh, Kyoko Hida.
Abstract
Tumor angiogenesis is necessary for tumor progression and metastasis; therefore, tumor blood vessels are potential therapeutic targets in anticancer therapy. We previously reported that tumor endothelial cells (TECs) exhibit different phenotypes compared with normal endothelial cells (NECs), and microarray analyses of mouse TECs and NECs have shown that several genes are upregulated in TECs compared with NECs. Among these genes, the expression levels of prostaglandin F receptor (PTGFR) mRNA, which encodes the prostaglandin F receptor (FP), were higher in TECs than in NECs. It has been reported that FP and its ligand, prostaglandin F(2α) , are involved in tumor angiogenesis. However, there have been no reports of the expression of PTGFR in the tumor vessels of renal cell carcinoma (RCC). Thus, we isolated human TECs (hTECs) from RCCs. The expression levels of PTGFR mRNA were also upregulated in hTECs. In addition, immunostaining showed that the PTGFR was expressed in human tumor blood vessels in vivo. These findings suggested that PTGFR is a novel TEC marker and that it may be a novel target for antiangiogenic therapy for RCC.Entities:
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Year: 2013 PMID: 23356224 DOI: 10.1111/pin.12031
Source DB: PubMed Journal: Pathol Int ISSN: 1320-5463 Impact factor: 2.534