In Apolipoprotein E-deficient mice, blockade of PDGFR-beta with APB5 reduced aortic atherosclerotic lesion size by 67% and intimal VSMCs by 80%, whereas PDGFR-alpha blockade had minimal effect.
Does functional blockade of PDGFR-alpha or PDGFR-beta reduce atherosclerotic lesion size and VSMC accumulation in Apolipoprotein E-deficient mice?
Blockade of PDGFR-beta, but not PDGFR-alpha, significantly reduces atherosclerotic lesion size and vascular smooth muscle cell accumulation in ApoE-deficient mice, highlighting its role in atherogenesis.
BACKGROUND: The vascular smooth muscle cell (VSMC) is the central cell component involved in the fibroproliferative response in atherogenesis. As the lesion advances, VSMCs migrate from the media into the subendothelial space, thereby forming fibrous plaque lesions. Platelet-derived growth factor (PDGF) has been known to be a potent chemoattractant and mitogen for SMCs, but the pathophysiological role of the 2 PDGF receptors, receptor-alpha (PDGFR-alpha) and receptor-beta (PDGFR-beta) in atherogenesis is poorly understood. To clarify this problem, we prepared antagonistic rat monoclonal antibodies, APA5 and APB5, against murine PDGFR-alpha and PDGFR-beta, respectively. METHODS AND RESULTS: Apolipoprotein E-deficient mice were fed a high-fat diet containing 0.3% cholesterol from 6 weeks of age and subjected to injection with 1 mg/d IP of either antibody from 12 to 18 weeks every other day. In the mice injected with APB5, the aortic atherosclerotic lesion size and the number of intimal VSMCs were reduced by 67% and 80%, respectively, compared with the control mice injected with irrelevant rat IgG. In contrast, the mice that received APA5 showed only minimal reduction of lesion size, and a large number of VSMCs were observed in the intima. In the intima of advanced lesions, APB5 immunolabeled VSMCs, whereas APA5 could detect VSMCs mainly in the media. CONCLUSIONS: These results indicate that PDGFR-beta plays a significant role in formation of fibrous atherosclerotic lesions and that regulation of the signal transduction through PDGFR-beta could affect atherogenesis in mice.
Sano et al. (Tue,) conducted a other in Atherosclerosis. Antagonistic rat monoclonal antibodies APA5 (against PDGFR-alpha) and APB5 (against PDGFR-beta) vs. Irrelevant rat IgG was evaluated on Aortic atherosclerotic lesion size and number of intimal VSMCs. In Apolipoprotein E-deficient mice, blockade of PDGFR-beta with APB5 reduced aortic atherosclerotic lesion size by 67% and intimal VSMCs by 80%, whereas PDGFR-alpha blockade had minimal effect.
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