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抑制同种异体移植炎症因子-1的表达可减少新生内膜增生的发展及p38激酶活性。

Inhibition of allograft inflammatory factor-1 expression reduces development of neointimal hyperplasia and p38 kinase activity.

作者信息

Sommerville Laura J, Xing Chen, Kelemen Sheri E, Eguchi Satoru, Autieri Michael V

机构信息

Department of Physiology, Independence Blue Cross Cardiovascular Research Center, Temple University School of Medicine, 810, MRB, 3420 North Broad Street, Philadelphia, PA 19140, USA.

出版信息

Cardiovasc Res. 2009 Jan 1;81(1):206-15. doi: 10.1093/cvr/cvn242. Epub 2008 Sep 8.

DOI:10.1093/cvr/cvn242

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2721640/

Abstract

AIMS

Allograft inflammatory factor-1 (AIF-1) is a calcium-binding, scaffold-signalling protein expressed in vascular smooth muscle cells (VSMCs) in response to injury. The effects of AIF-1 attenuation on development of intimal hyperplasia are unknown, and the molecular mechanisms of these effects remain uncharacterized. The goals of the present study were to determine whether AIF-1 knockdown reduced VSMC proliferation, migration, and intimal hyperplasia, and determine AIF-1 effects on signal transduction in VSMCs.

METHODS AND RESULTS

Balloon angioplasty-injured rat carotid arteries transduced with adenovirus to overexpress AIF-1 (AdAIF-1) significantly increased, and adenovirus to knock down AIF-1 (AdsiRNA) expression significantly decreased neointimal formation compared with green fluorescent protein (AdGFP) and Adscrambled controls (P < 0.05 and P < 0.01, n = 6). Primary rat VSMCs transduced with AdAIF-1 displayed a significant increase in proliferation, and AdsiRNA-transduced VSMCs proliferated significantly more slowly than controls (P < 0.05). VSMCs transduced with AdAIF-1 show increased migration when compared with control VSMCs (P < 0.01). Rat VSMCs transduced with AdAIF-1 showed constitutive and prolonged activation of the mitogen-activated protein kinase p38, whereas AdsiRNA-treated VSMCs showed decreased p38 activation compared with AdGFP (P < 0.05). Immunohistochemical analysis of AdAIF-1-transduced carotid arteries showed increased staining with a phospho-specific p38 antibody compared with AdGFP-transduced arteries. A specific p38 inhibitor abrogated AIF-1-induced VSMC proliferation, but not AIF-1-induced migration.

CONCLUSION

Taken together, AIF-1 expression plays a key role in the development of neointimal hyperplasia. AIF-1 expression enhances the activation of p38 MAP kinase. AIF-1-enhanced proliferation is p38 kinase dependent, but AIF-1-enhanced VSMC migration is p38 independent.

摘要

目的

同种异体移植炎症因子-1（AIF-1）是一种钙结合支架信号蛋白，在血管平滑肌细胞（VSMC）受到损伤时表达。AIF-1表达减弱对内膜增生发展的影响尚不清楚，且这些影响的分子机制仍未明确。本研究的目的是确定AIF-1基因敲低是否能减少VSMC增殖、迁移和内膜增生，并确定AIF-1对VSMC信号转导的影响。

方法与结果

与绿色荧光蛋白（AdGFP）和Ad乱序对照相比，用腺病毒转导以过表达AIF-1（AdAIF-1）的球囊血管成形术损伤大鼠颈动脉显著增加了新生内膜形成，而用腺病毒敲低AIF-1（AdsiRNA）表达则显著减少了新生内膜形成（P<0.05和P<0.01，n=6）。用AdAIF-1转导的原代大鼠VSMC增殖显著增加，而用AdsiRNA转导的VSMC增殖比对照慢得多（P<0.05）。与对照VSMC相比，用AdAIF-1转导的VSMC迁移增加（P<0.01）。用AdAIF-1转导的大鼠VSMC显示有丝分裂原活化蛋白激酶p38的组成性和持续性激活，而与AdGFP相比，AdsiRNA处理的VSMC显示p38激活减少（P<0.05）。对用AdAIF-1转导的颈动脉进行免疫组织化学分析显示，与用AdGFP转导的动脉相比，磷酸化特异性p38抗体染色增加。一种特异性p38抑制剂消除了AIF-1诱导的VSMC增殖，但未消除AIF-1诱导的迁移。

结论

综上所述，AIF-1表达在内膜增生发展中起关键作用。AIF-1表达增强p38丝裂原活化蛋白激酶的激活。AIF-1增强的增殖是p38激酶依赖性的，但AIF-1增强的VSMC迁移是p38非依赖性的。