Cardiovascular Pathology
Volume 21, Issue 1 , Pages 28-38, January 2012

Proteinase inhibitor 9 is reduced in human atherosclerotic lesion development

Received 30 July 2010; received in revised form 2 December 2010; accepted 12 December 2010. published online 08 February 2011.

Abstract 

Background

Granzyme B, a proapoptotic serine protease, is abundant in advanced, unstable atherosclerotic plaques, and it is suggested to contribute to plaque instability by inducing vascular smooth muscle cells apoptosis and by degrading plaque extracellular matrix. Proteinase inhibitor 9, the only known endogenous inhibitor of granzyme B in humans, confers protection against granzyme-B-induced apoptosis. However, the role of proteinase inhibitor 9 in atherosclerotic lesion development has yet to be determined. We hypothesized that atherosclerotic lesions have lower proteinase inhibitor 9 expression levels that will increase their susceptibility to granzyme-B-induced apoptosis.

Methods

Serial sections of human coronary arteries exhibiting different stages of lesion development were assessed by immunohistochemistry for proteinase inhibitor 9, α-smooth muscle cells actin, granzyme B, CD8, and active caspase-3. Frozen samples were analyzed by Western blot to evaluate total proteinase inhibitor 9 levels.

Results

Vascular smooth muscle cells express less proteinase inhibitor 9 as disease severity increases, and a significant difference in proteinase inhibitor 9 expression is observed between medial and intimal smooth muscle cells. High granzyme B levels colocalize with CD8+ cells and foam cells in the shoulder region and necrotic core area of advanced lesions. In advanced lesions, increased expression of activated caspase-3 in intimal SMC was associated with reduced proteinase inhibitor 9 expression in the presence of granzyme B.

Conclusion

Reduced proteinase inhibitor 9 expression in human vascular smooth muscle cells is associated with atherosclerotic disease progression and is inversely related to the extent of apoptosis within the intima. Reduced proteinase inhibitor 9 expression may contribute to increased smooth muscle cell susceptibility to granzyme-B-induced apoptosis within the plaque.

Keywords: Atherosclerosis, Proteinase inhibitor 9, Granzyme B, Vascular smooth muscle cells, Apoptosis

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 This research was funded in part from grants from the Heart and Stroke Foundation of British Columbia and Yukon (HSFBCY) (DJG) and the Canadian Institutes for Health Research (CIHR) (MFA, DJG). Funding sources: AH is grateful for the support from a CIHR Canada Graduate Scholarship Master's Award and the Vanier Canada Graduate Scholarship. DC is funded by the HSFBCY, CIHR/IMPACT, and NSERC Fellowship.

PII: S1054-8807(10)00198-5

doi:10.1016/j.carpath.2010.12.002

Cardiovascular Pathology
Volume 21, Issue 1 , Pages 28-38, January 2012

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