VEGF Regulates Local Inhibitory Complement Proteins in the Eye and Kidney

Overview

Journal J Clin Invest

Specialty General Medicine

Date 2016 Dec 6

PMID 27918307

Citations 72

Authors

Lindsay S Keir

Rachel Firth

Lyndsey Aponik

Daniel Feitelberg

Susumu Sakimoto

Edith Aguilar

Gavin I Welsh

Anna Richards

Yoshihiko Usui

Simon C Satchell

Valeryia Kuzmuk

Richard J Coward

Jonathan Goult

Katherine R Bull

Ruchi Sharma

Kapil Bharti

Peter D Westenskow

Iacovos P Michael

Moin A Saleem

Martin Friedlander

Affiliations

Soon will be listed here.

Abstract

Outer retinal and renal glomerular functions rely on specialized vasculature maintained by VEGF that is produced by neighboring epithelial cells, the retinal pigment epithelium (RPE) and podocytes, respectively. Dysregulation of RPE- and podocyte-derived VEGF is associated with neovascularization in wet age-related macular degeneration (ARMD), choriocapillaris degeneration, and glomerular thrombotic microangiopathy (TMA). Since complement activation and genetic variants in inhibitory complement factor H (CFH) are also features of both ARMD and TMA, we hypothesized that VEGF and CFH interact. Here, we demonstrated that VEGF inhibition decreases local CFH and other complement regulators in the eye and kidney through reduced VEGFR2/PKC-α/CREB signaling. Patient podocytes and RPE cells carrying disease-associated CFH genetic variants had more alternative complement pathway deposits than controls. These deposits were increased by VEGF antagonism, a common wet ARMD treatment, suggesting that VEGF inhibition could reduce cellular complement regulatory capacity. VEGF antagonism also increased markers of endothelial cell activation, which was partially reduced by genetic complement inhibition. Together, these results suggest that VEGF protects the retinal and glomerular microvasculature, not only through VEGFR2-mediated vasculotrophism, but also through modulation of local complement proteins that could protect against complement-mediated damage. Though further study is warranted, these findings could be relevant for patients receiving VEGF antagonists.

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