Cathepsin S expression is up-regulated following balloon angioplasty in the hypercholesterolemic rabbit

doi:10.1016/j.cardiores.2004.02.002

Cardiovascular Research 2004 62(3):610-620; doi:10.1016/j.cardiores.2004.02.002
© 2004 by European Society of Cardiology

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Cathepsin S expression is up-regulated following balloon angioplasty in the hypercholesterolemic rabbit

Cynthia L Burns-Kurtis^*^,a, Alan R Olzinski^a, Saul Needle^a, Josephine H Fox^b, Elizabeth A Capper^b, Fiona M Kelly^c, Michael S McQueney^d and Anne M Romanic^a

^aDepartment of Vascular Inflammatory Diseases, GlaxoSmithKline Pharmaceuticals, 709 Swedeland Road, P.O. Box 1539, King of Prussia, PA 19406, USA
^bDepartment of Respiratory and Inflammatory Diseases, GlaxoSmithKline Pharmaceuticals, 709 Swedeland Road, P.O. Box 1539, King of Prussia, PA 19406, USA
^cDepartment of Quantitative Expression, GlaxoSmithKline Pharmaceuticals, Stevenage, Hertfordshire, SG1 2NY, UK
^dAssay Development and Compound Profiling, GlaxoSmithKline Pharmaceuticals, 709 Swedeland Road, P.O. Box 1539, King of Prussia, PA 19406, USA

^* Corresponding author. Tel.: +1-610-270-4170; fax: +1-610-270-6206. Email address: cynthia_l_kurtis{at}gsk.com

Objective: Neointimal development following balloon angioplastyinvolves many factors including smooth muscle cell (SMC) migrationand proliferation and extracellular matrix (ECM) remodeling.Further, in hypercholesterolemic (HC) conditions, there is aninflux of macrophage foam cells (FCs) into the restenotic lesion,which also involves degradation of the basement membrane andsurrounding ECM. The ECM remodeling that occurs during restenosishas been shown to be mediated by various proteases. Here wehave investigated the role of cathepsin S (CatS), a cysteineprotease, in this process. Methods and results: We have demonstratedby Taqman quantitative PCR, Western blot, and immunohistochemistrythat CatS is up-regulated in restenotic lesions of HC rabbitsfollowing balloon injury of the iliofemoral artery. CatS mRNAexpression was elevated 28-fold in balloon-injured vessels relativeto uninjured contralateral vessels in HC rabbits 8 weeks post-angioplasty(p<0.05). CatS protein expression was detected within 1 daypost-injury, persisted throughout the entire time course evaluated(60 days post-injury), and was co-localized with SMCs, macrophages,and FCs. In contrast, cystatin C (CysC), the endogenous inhibitorof cathepsins, was only minimally up-regulated following injury.CysC mRNA expression was elevated 3.5-fold in balloon-injuredvessels relative to uninjured contralateral vessels in HC rabbits8 weeks post-angioplasty (p<0.005), and up-regulation ofprotein expression was not detected until days 28 and 60 post-injury.Additional biochemical studies using recombinant rabbit CatSrevealed that rabbit CatS digests laminin, fibronectin, andtype I collagen. Further, CatS expression was evaluated in SMCsthat were induced to migrate through a matrix-coated Boydenchamber upon platelet-derived growth factor (PDGF) stimulation.The addition of a selective CatS inhibitor reduced SMC migrationdose-dependently with an 80% reduction in migration at 30 nM(p<0.005). Additionally, we have shown that CatS proteinexpression by human macrophages was increased upon stimulationwith oxidized low density lipoprotein (ox-LDL), implying augmentationof CatS production during foam cell formation. Conclusion: Takentogether, our results indicate an enhanced expression of CatSduring neointima formation and it is associated with invadingSMCs, macrophages, and FCs, highlighting the importance of CatSin the pathogenesis of restenosis.

KEYWORDS Cathepsin; Restenosis; Atherosclerosis; Smooth muscle; Macrophage; Remodeling; Extracellular matrix

Time for primary review 26 days

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