| Literature DB >> 30249667 |
Pachiappan Arjunan1, Xianchai Lin1, Zhongshu Tang1, Yuxiang Du1, Anil Kumar1, Lixian Liu1, Xiangke Yin1, Lijuan Huang1, Wei Chen1, Qishan Chen1, Zhimin Ye1, Shasha Wang1, Haiqing Kuang1, Linbin Zhou1, Kai Xu2, Xue Chen3, Haitao Zeng4, Weisi Lu1, Yihai Cao5, Yizhi Liu1, Chen Zhao6,3,7,8, Xuri Li9.
Abstract
VEGF-B was discovered a long time ago. However, unlike VEGF-A, whose function has been extensively studied, the function of VEGF-B and the mechanisms involved still remain poorly understood. Notwithstanding, drugs that inhibit VEGF-B and other VEGF family members have been used to treat patients with neovascular diseases. It is therefore critical to have a better understanding of VEGF-B function and the underlying mechanisms. Here, using comprehensive methods and models, we have identified VEGF-B as a potent antioxidant. Loss of Vegf-b by gene deletion leads to retinal degeneration in mice, and treatment with VEGF-B rescues retinal cells from death in a retinitis pigmentosa model. Mechanistically, we demonstrate that VEGF-B up-regulates numerous key antioxidative genes, particularly, Gpx1 Loss of Gpx1 activity largely diminished the antioxidative effect of VEGF-B, demonstrating that Gpx1 is at least one of the critical downstream effectors of VEGF-B. In addition, we found that the antioxidant function of VEGF-B is mediated mainly by VEGFR1. Given that oxidative stress is a crucial factor in numerous human diseases, VEGF-B may have therapeutic value for the treatment of such diseases.Entities:
Keywords: Gpx1; VEGF-B; antioxidant; oxidative stress; retinal degeneration
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Year: 2018 PMID: 30249667 PMCID: PMC6187152 DOI: 10.1073/pnas.1801379115
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205