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Synergistic inhibitory effect of gemcitabine and angiotensin type-1 receptor blocker, losartan, on murine pancreatic tumor growth via anti-angiogenic activities.

Authors :
Noguchi, Ryuichi
Yoshiji, Hitoshi
Ikenaka, Yasuhide
Namisaki, Tadashi
Kitade, Mitsuteru
Kaji, Kosuke
Yoshii, Junichi
Yanase, Koji
Yamazaki, Masaharu
Tsujimoto, Tatsuhiro
Kawaratani, Hideto
Fukui, Hiroshi
Noguchi, Ryuichi
Yoshiji, Hitoshi
Ikenaka, Yasuhide
Namisaki, Tadashi
Kitade, Mitsuteru
Kaji, Kosuke
Yoshii, Junichi
Yanase, Koji
Yamazaki, Masaharu
Tsujimoto, Tatsuhiro
Kawaratani, Hideto
Fukui, Hiroshi
Publication Year :
2012

Abstract

Pancreatic cancer is one of the leading causes of cancer death, and represents a challenging chemotherapeutic problem. The crucial role of angiogenesis in tumor growth has been widely recognized, and several reports have revealed that the combination treatment of the conventional chemotherapeutic drugs and anti-angiogenic agents exerted synergistic anti-cancerous effects. It has been reported that the clinically used angiotensin type-1 receptor blocker (ARB) exerted potent anti-angiogenic activity. The aim of our current study was to examine the combination effect of gemcitabine (GEM), a widely used conventional chemotherapeutic drug against pancreas cancer, and losartan (Lo), an ARB, on murine pancreatic tumor growth, especially in conjunction with angiogenesis. When used individually, GEM and Lo at clinically comparable low doses moderately suppressed pancreatic tumor development. The combination treatment with GEM and Lo exerted a marked inhibitory effect as compared with single agent treatments even after the tumor was fully established. Neovascularization and the expression of the vascular endothelial growth factor (VEGF), a central angiogenic factor, in the tumor were both markedly suppressed in a magnitude similar to the inhibitory effects against the tumor growth. Since both agents are widely used in the clinical practice, the combination regimen of GEM and Lo may represent a potential new therapeutic strategy for pancreatic cancer in the future.

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.ocn829850465
Document Type :
Electronic Resource