![[Feedback]](/icons/banner/feedbackACT.gif){kind=icon}
![[For Subscribers]](/icons/banner/subscriberACT.gif){kind=icon}
![[Archive]](/icons/banner/archiveACT.gif){kind=icon}
![[Search]](/icons/banner/searchACT.gif){kind=icon}
![[Contents]](/icons/banner/tocACT.gif){kind=icon}
|
|
|
|
|
||
Vol. 285, Issue 3, 1280-1286, June 1998
Cardiovascular Science Research Laboratory (Y.M., Y.Y., H.T., Y.T.,
N.O., H.M.),
Pharmacological Research Laboratory (Y.N., N.M.) and
Chemistry Laboratory (A.S., T.A.), Taiho Pharmaceutical Co. Ltd.,
Hanno-City, Saitama 357, Japan
The purpose of this study was to determine the efficacy and the
possible mechanism of action of a recently synthesized drug, TAS-301
[3-bis (4-methoxyphenyl)methylene-2-indolinone], on intimal formation
in comparison with those of tranilast, the clinical efficacy of which
was reported earlier. Rat carotid arteries were injured using a balloon
catheter. Neointimal thickening, measured 14 days after injury, was
reduced by the oral administration of TAS-301 in a dose-dependent
fashion (3-100 mg/kg), and the effect of TAS-301 at a dose of 100 mg/kg was significantly greater than that of tranilast (300 mg/kg).
Fewer cells were found on the intima of balloon-injured arteries of
TAS-301-treated rats than on arteries of tranilast-treated rats. In an
in vitro assay, TAS-301 inhibited the migration of
smooth muscle cells (SMCs) stimulated by platelet-derived growth
factor-BB, insulin-like growth factor-1 or heparin-binding epidermal
growth factor-like growth factor. In addition, TAS-301 and tranilast
reduced the proliferation of medial and intimal SMCs at 4 and 8 days,
respectively, after the injury. In vitro, TAS-301
inhibited basic fibroblast growth factor-induced proliferation of SMCs
dose dependently. These findings indicate that TAS-301 shows a higher
inhibitory potency on intimal formation than tranilast due to
inhibition of both migration of medial SMCs and proliferation of medial
and intimal SMCs. Our results suggest that further evaluation of
TAS-301 as an inhibitor of postangioplasty intimal thickening is
warranted.
This article has been cited by other articles:
|
|
 |
|
  H. C. Lowe, S. N. Oesterle, and L. M. Khachigian Coronary in-stent restenosis: Current status and future strategies J. Am. Coll. Cardiol., January 16, 2002; 39(2): 183 - 193. [Abstract] [Full Text] [PDF]
|
|
|
|
 |
|
 Y. Yamasaki, K. Miyoshi, N. Oda, M. Watanabe, H. Miyake, J. Chan, X. Wang, L. Sun, C. Tang, G. McMahon, et al. Weekly Dosing With the Platelet-Derived Growth Factor Receptor Tyrosine Kinase Inhibitor SU9518 Significantly Inhibits Arterial Stenosis Circ. Res., March 30, 2001; 88(6): 630 - 636. [Abstract] [Full Text] [PDF]
|
|
|
|
 |
|
 E. Sasaki, Y. Tanahashi, Y. Yamasaki, N. Oda, Y. Nozawa, H. Terakawa, K. Miyoshi, Y. Muranaka, H. Miyake, and N. Matsuura Inhibitory Effect of TAS-301, a New Synthesized Constrictive Remodeling Regulator, on Renarrowing after Balloon Overstretch Injury of Porcine Coronary Artery J. Pharmacol. Exp. Ther., December 1, 2000; 295(3): 1043 - 1050. [Abstract] [Full Text]
|
|
|
|
|
|
S. Ishiwata, S. Verheye, K. A. Robinson, M. Y. Salame, H. de Leon, S. B. King III, and N. A. F. Chronos Inhibition of neointima formation by tranilast in pig coronary arteries after balloon angioplasty and stent implantation J. Am. Coll. Cardiol., April 1, 2000; 35(5): 1331 - 1337. [Abstract] [Full Text] [PDF]
|
|
 |
 |
 |
|
 |
 |
 |
