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PDGF-CC blockade inhibits pathological angiogenesis by acting on multiple cellular and molecular targets
Authors:Xu Hou  Anil Kumar  Chunsik Lee  Bin Wang  Pachiappan Arjunan  Lijin Dong  Arvydas Maminishkis  Zhongshu Tang  Yang Li  Fan Zhang  Shi-Zhuang Zhang  Piotr Wardega  Sagarika Chakrabarty  Baoying Liu  Zhijian Wu  Peter Colosi  Robert N Fariss  Johan Lennartsson  Robert Nussenblatt  J Silvio Gutkind  Yihai Cao  Xuri Li
Abstract:The importance of identifying VEGF-independent pathways in pathological angiogenesis is increasingly recognized as a result of the emerging drug resistance to anti-VEGF therapies. PDGF-CC is the third member of the PDGF family discovered after more than two decades of studies on PDGF-AA and PDGF-BB. The biological function of PDGF-CC and the underlying cellular and molecular mechanisms remain largely unexplored. Here, using different animal models, we report that PDGF-CC inhibition by neutralizing antibody, shRNA, or genetic deletion suppressed both choroidal and retinal neovascularization. Importantly, we revealed that PDGF-CC targeting acted not only on multiple cell types important for pathological angiogenesis, such as vascular mural and endothelial cells, macrophages, choroidal fibroblasts and retinal pigment epithelial cells, but also on the expression of other important angiogenic genes, such as PDGF-BB and PDGF receptors. At a molecular level, we found that PDGF-CC regulated glycogen synthase kinase (GSK)–3β phosphorylation and expression both in vitro and in vivo. Activation of GSK3β impaired PDGF-CC–induced angiogenesis, and inhibition of GSK3β abolished the antiangiogenic effect of PDGF-CC blockade. Thus, we identified PDGF-CC as an important candidate target gene for antiangiogenic therapy, and PDGF-CC inhibition may be of therapeutic value in treating neovascular diseases.
Keywords:choroidal neovascularization  glycogen synthase kinase-3β    vascular biology  retinal neovascularization  ocular disease
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