Rivaroxaban, a specific FXa inhibitor, improved endothelium-dependent relaxation of aortic segments in diabetic mice 特異的活性化第X因子阻害薬であるリバーロキサバンは、糖尿病マウス大動脈の血管内皮依存性弛緩反応を改善した

著者
    • Pham, Tran Phuong
    • Fukuda, Daiju
    • Yagi, Shusuke
    • Kusunose, Kenya
    • Yamada, Hirotsugu
    • Soeki, Takeshi
    • Shimabukuro, Michio
    • Sata, Masataka
書誌事項
タイトル

Rivaroxaban, a specific FXa inhibitor, improved endothelium-dependent relaxation of aortic segments in diabetic mice

タイトル別名

特異的活性化第X因子阻害薬であるリバーロキサバンは、糖尿病マウス大動脈の血管内皮依存性弛緩反応を改善した

著者名

Pham, Tran Phuong

著者名

Fukuda, Daiju

著者名

Yagi, Shusuke

著者名

Kusunose, Kenya

著者名

Yamada, Hirotsugu

著者名

Soeki, Takeshi

著者名

Shimabukuro, Michio

著者名

Sata, Masataka

学位授与大学

徳島大学

取得学位

博士(医学)

学位授与番号

甲第3432号

学位授与年月日

2019-08-01

注記・抄録

Activated factor X (FXa) plays a central role in the coagulation cascade, while it also mediates vascular function through activation of protease-activated receptors (PARs). Here, we examined whether inhibition of FXa by rivaroxaban, a direct FXa inhibitor, attenuates endothelial dysfunction in streptozotocin (STZ)-induced diabetic mice. Induction of diabetes increased the expression of a major FXa receptor, PAR2, in the aorta (P < 0.05). Administration of rivaroxaban (10 mg/kg/day) to diabetic wild-type (WT) mice for 3 weeks attenuated endothelial dysfunction as determined by acetylcholine-dependent vasodilation compared with the control (P < 0.001), without alteration of blood glucose level. Rivaroxaban promoted eNOSSer1177 phosphorylation in the aorta (P < 0.001). Induction of diabetes to PAR2-deficient (PAR2−/−) mice did not affect endothelial function and eNOSSer1177 phosphorylation in the aorta compared with non-diabetic PAR2−/− mice. FXa or a PAR2 agonist significantly impaired endothelial function in aortic rings obtained from WT mice, but not in those from PAR2−/− mice. FXa promoted JNK phosphorylation (P < 0.01) and reduced eNOSSer1177 phosphorylation (P < 0.05) in human coronary artery endothelial cells (HCAEC). FXa-induced endothelial dysfunction in aortic rings (P < 0.001) and eNOSSer1177 phosphorylation (P < 0.05) in HCAEC were partially ameliorated by a JNK inhibitor. Rivaroxaban ameliorated diabetes-induced endothelial dysfunction. Our results suggest that FXa or PAR2 is a potential therapeutic target.

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各種コード
  • NII論文ID(NAID)
    500001418088
  • NII著者ID(NRID)
    • 8000001752256
    • 8000001752257
    • 8000001752258
    • 8000001752259
    • 8000001752260
    • 8000001752261
    • 8000001752262
    • 8000001752263
  • DOI(出版社)
  • DOI
  • 本文言語コード
    • eng
  • データ提供元
    • 機関リポジトリ
    • NDLデジタルコレクション
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