Flt-1 Intraceptors Inhibit Hypoxia-Induced VEGF Expression In Vitro and Corneal Neovascularization In Vivo

doi:10.1167/iovs.04-1172

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(Investigative Ophthalmology and Visual Science. 2005;46:1647-1652.)
© 2005 by The Association for Research in Vision and Ophthalmology, Inc.
DOI: 10.1167/iovs.04-1172

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Flt-1 Intraceptors Inhibit Hypoxia-Induced VEGF Expression In Vitro and Corneal Neovascularization In Vivo

Nirbhai Singh,¹^,2 Shivan Amin,¹^,2 Elizabeth Richter,¹ Saadia Rashid,¹ Vincent Scoglietti,¹ Pooja D. Jani,¹ Jin Wang,³ Rajwinder Kaur,¹ Jayakrishna Ambati,⁴ Zheng Dong,³ and Balamurali K. Ambati¹

^¹From the Departments of Ophthalmology and ^³Cell Biology and Anatomy, Medical College of Georgia, Augusta, Georgia; and the ^⁴Department of Ophthalmology, University of Kentucky, Lexington, Kentucky.

PURPOSE. To determine whether subunits of VEGF receptor-1 coupledwith an endoplasmic reticulum retention signal can block hypoxia-inducedupregulation of VEGF secretion in corneal epithelial cells andblock murine corneal angiogenesis induced by corneal injury.

METHODS. Human corneal epithelial cells, transfected with plasmidsencoding Flt23K or Flt24K (the VEGF-binding domains of the Flt-1receptor coupled with the endoplasmic reticulum retention peptideKDEL), were subjected 2 days after transfection to 5% hypoxiafor 24 hours. Supernatant was sampled at 24 hours and assayedfor VEGF by ELISA. For in vivo models, mouse corneas underwentintrastromal injections of plasmids encoding Flt23K or Flt24K,and 2 days later, sustained injury induced by topical NaOH andmechanical scraping. Corneas were assessed 2 days later forVEGF ELISA and leukocyte counting or 1 week later for quantificationof neovascularization.

RESULTS. Hypoxia induced VEGF by human corneal epithelial cellswas sequestered by both Flt23K and Flt24K; Flt-1 23K suppressedVEGF secretion as well. Intrastromal delivery of plasmid Flt23Ksuppressed VEGF by 40.4% (P = 0.009), leukocytes by 49.4% (P< 0.001), and neovascularization by 66.8% (P = 0.001). Flt24Ksuppressed VEGF expression by 30.8% (P = 0.042), leukocytesby 25.8% (P < 0.001), and neovascularization by 49.5% (P= 0.015).

CONCLUSIONS. Flt-1 intraceptors, which are endoplasmic reticulumretention signal-coupled VEGF receptors, significantly suppresshypoxia-induced VEGF secretion by corneal epithelial cells invitro. In vivo, delivery of naked plasmids expressing theseintraceptors inhibits injury-induced upregulation of VEGF, leukocyteinfiltration, and corneal neovascularization.

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