TGFβ1—Smad3—ILK信号转导通路与大鼠肝纤维化的相关性研究(4)
| 第1页 |
| 第2页 |
参见附件。
[14] Yokote K,Kobayashi K,Saito Y.The role of Smad3 dependent TGF-beta signal in vascular response to injury[J].Trends Cardiovasc Med,2006,16(7):240-245.
[15] 张国,王天才,唐望先,等.Smad3、Smad7基因表达与肝纤维化发病关系研究[J].中华消化杂志,2002,22(11):647-650.
[16] 俞蕾敏,吕宾,李善高.大鼠肝硬化形成过程中肝组织TGFβ1、Smad3、Smad7水平动态的变化[J].世界华人消化杂志,2007,15(30):3163-3167.
[17] Cho IJ,Kim SH,Kim SG.Inhibition of TGFβ2 mediated PAI21 induction by oltipraz through selective interruption of Smad3 activation[J].Cytokine,2006,35(5-6):284-294.
[18] Masayuki UE,Scott S.Smad2 and Smad3 play different roles inrat hepatic stellate cell function and α-2 smooth muscle actin organization[J].Mol Biol Cell,2005,16(9):4214-4224.
[19] Li Y,Yang J,Dai C,et al.Role of integrin-linked kinase in mediating tubular epithelial to mesenhchymal transition and renal interstitial fibrogenesis[J].J Clin Invest,2003,112(4):503-516.
[20] Li Y,Kang YS,Dai C,et al.Epithelial-to-messenchymal transition is a potential pathway leading to podocyte dysfunction and proteinuria[J].Am J Pathol,2008,172(2):299-308.
(收稿日期:2013-09-28 本文编辑:林利利)
您现在查看是摘要介绍页,详见PDF附件。