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《心脏杂志》[ISSN:1009-7236/CN:61-1268/R]

期数:

2013年第4期

页码:

482-485

栏目:

综述

出版日期:

2013-07-25

文章信息/Info

Title:

Roles of platelet-derived growth factors and platelet-derived growth factor receptors in cardiovascular diseases

作者:

范 彬 综述; 马礼坤 审校

(安徽医科大学附属省立医院心血管内科，安徽 合肥 230001)

Author(s):

FAN Bin;  MA Li-kun

(Department of Cardiology, Affiliated Anhui Provincial Hospital, Anhui Medical University, Hefei 230001, Anhui, China)

关键词:

受体; 血小板源性生长因子; 心血管疾病; 动脉粥样硬化

Keywords:

receptors;  platelet-derived growth factors;  atherosclerosis;  angiogenesis;  myocardial fibrosis

分类号:

Q592.1

DOI:

-

文献标识码:

A

摘要:

血小板源性生成因子（PDGFs）及其受体（PDGFRs）在心血管疾病中发挥着重要作用，二者不仅参与了动脉粥样硬化（AS）的形成，而且在血管生成、心肌纤维化过程中也扮演了重要角色。PDGFRs被其配体PDGFs激活后，在血管平滑肌细胞、纤维母细胞、内皮细胞等中的表达上调，通过细胞内信号转导通路，促使该类靶细胞增殖分化，从而参与AS、血管生成和心肌纤维化的发生。本文就PDGFs/PDGFRs在心血管疾病中的研究进展做一综述。

Abstract:

Platelet-derived growth factors (PDGFs) and platelet-derived growth factor receptors (PDGFRs) both play some important roles in the cardiovascular diseases, including atherosclerosis (AS), angiogenesis and myocardial fibrosis. PDGFRs which are activated by their ligand PDGFs up-regulate in cells, such as vascular smooth muscle cells, fibroblasts and endothelial cells, thus resulting in the proliferation and differentiation of target cells. PDGFs/PDGFRs participate in AS angiogenesis and myocardial fibrosis. This review will discuss the research progress of PDGFs/PDGFRs in the cardiovascular diseases.

参考文献/References

[1]Andrae J,Gallini R,Betsholtz C. Role of platelet-derived growth factors in physiology and medicine[J].Genes Dev,2008,22(10):1276-1312.

[2]Yang Y,Yuzawa S,Schlessinger J.Contacts between membrane proximal regions of the PDGF receptor ectodomain are required for receptor activation but not for receptor dimerization[J].Proc Natl Acad Sci USA,2008,105(22):7681-7686.

[3]Chintalgattu V,Ai D,Langley RR,et al.Cardiomyocyte PDGFR-β signaling is an essential component of the mouse cardiac response to load-induced stress[J].J Clin Invest,2010,120(2):472-484.

[4]Zhang H,Bajraszewski N,Wu E,et al.PDGFRs are critical for PI3K/Akt activation and negatively regulated by mTOR[J].J Clin Invest,2007,117(3):730-738.

[5]Jurek A,Heldin CH,Lennartsson J.Platelet-derived growth factor-induced signaling pathways interconnect to regulate the temporal pattern of Erk1/2 phosphorylation[J].Cell Signal,2011,23(1):280-287.

[6]Rhen T,Jangula A,Schroeder A,et al.The platelet-derived growth factor signaling system in snapping turtle embryos, Chelydra serpentina: potential role in temperature-dependent sex determination and testis development[J].Gen Comp Endocrinol,2009,161(3):335-343.

[7]Wyler von Ballmoos M,Yang Z,Volzmann J,et al.Endothelial progenitor cells induce a phenotype shift in differentiated endothelial cells towards PDGF/PDGFRβ axis-mediated angiogenesis[J].PLoS One,2010,5(11):e14107.

[8]Wang H,Yin Y,Li W,et al.Over-expression of PDGFR-β promotes PDGF-induced proliferation, migration,and angiogenesis of EPCs through PI3K/Akt signaling pathway[J].PLoS One,2012, 7(2):e30503.

[9]Zymek P,Bujak M,Chatila K,et al.The role of platelet-derived growth factor signaling in healing myocardial infarcts[J].JACC,2006,48(11):2315-2323.

[10]Deguchi JO,Aikawa M,Tung CH,et al.Inflammation in atherosclerosis: visualizing matrix metalloproteinase action in macrophages in vivo[J].Circulation,2006,114:55-62.

[11]Moore KJ,Tabas I. Macrophages in the pathogenesis of atherosclerosis［J］. Cell, 2011, 145:341-355.

[12]Visel A,Zhu Y,May D,et al.Targeted deletion of the 9p21 non-coding coronary artery disease risk interval in mice[J].Nature,2010,464(7287):409-412.

[13]Friedland JC,Lee MH,Boettiger D.Mechanically activated integrin switch controls alpha5beta1 function[J].Science,2009,323(5914):642-644.

[14]Isenberg BC,DiMilla PA,Walker M,et al.Vascular smooth muscle cell durotaxis depends on substrate stiffness gradient strength[J].Biophys J,2009,97(5):1313-1322.

[15]Olson LE,Soriano P.PDGFRβ signaling regulates mural cell plasticity and inhibits fat development[J].Dev Cell,2011,20(6):815-26.

[16]Keramati AR,Singh R,Lin A,et al.Wild-type LRP6 inhibits,whereas atherosclerosis-linked LRP6R611C increases PDGF-dependent vascular smooth muscle cell proliferation[J].Proc Natl Acad Sci USA,2011,108(5):1914-1918.

[17]Shimizu H,Nakagawa Y, Murakami C,et al.Protein tyrosine phosphatase PTPepsilonM negatively regulates PDGF beta-receptor signaling induced by high glucose and PDGF in vascular smooth muscle cells[J].Am J Physiol Cell Physiol,2010,299(5):1144-1152.

[18]Skaggs BJ,Hahn BH,Sahakian L,et al.Dysfunctional,pro-inflammatory HDL directly upregulates monocyte PDGFRβ, chemotaxis and TNFα production[J].Clin Immunol,2010,137(1):147-156.

[19]Porter KE,Turner NA.Cardiac fibroblasts:At the heart of myocardial remodeling[J].Pharmaco Ther,2009,123(5):255-278.

[20]Krenning G,Zeisberg EM,Kalluri R.The origin of fibroblasts and mechanism of cardiac fibrosis[J].J Cell Physiol,2011,225(3):631-637.

[21]Yue L,Xie J,Nattel S.Molecular determinants of cardiac fibroblast electrical function and therapeutic implications for atrial fibrillation[J]. Cardiovascular Research,2011,89(4):744-753.

[22]Wynn TA.Cellular and molecular mechanisms of fibrosis[J].J Pathol,2008,214(2):199-210.

[23]Pontén A,Li X,Thorén P,et al.Transgenic overexpression of platelet-derived growth factor-C in the mouse heart induces cardiacfibrosis, hypertrophy,and dilated cardiomyopathy[J].Am J Pathol,2003,163(2):673-682.

[24]Zhao W,Zhao T,Huang V,et al.Platelet-derived growth factor involvement in myocardial remodeling following infarction[J].J Mol Cell Cardiol,2011,51(5):830-838.

[25]Vantler M,Karikkineth BC,Naito H,et al.PDGF-BB protects cardiomyocytes from apoptosis and improves contractile function of engineered heart tissue[J].J Mol Cell Cardiol,2010,48(6):1316-1323.

备注/Memo

备注/Memo:

收稿日期：2012-09-24.通讯作者：马礼坤，主任医师，主要从事冠状动脉粥样硬化 研究 Email：lkma08@yahoo.cn 作者简介：范彬，硕士生 Email：fanbin414@163.com

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更新日期/Last Update: 2013-07-29