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Sustained treatment of retinal vascular diseases with self-aggregating sunitinib microparticles

Author

Listed:
  • Hiroki Tsujinaka

    (Johns Hopkins University School of Medicine)

  • Jie Fu

    (Johns Hopkins University School of Medicine)

  • Jikui Shen

    (Johns Hopkins University School of Medicine)

  • Yun Yu

    (Graybug Vision, Inc.)

  • Zibran Hafiz

    (Johns Hopkins University School of Medicine)

  • Joshua Kays

    (Graybug Vision, Inc.)

  • David McKenzie

    (Graybug Vision, Inc.)

  • Delia Cardona

    (Graybug Vision, Inc.)

  • David Culp

    (Powered Research, LLC, Research Triangle Park)

  • Ward Peterson

    (Graybug Vision, Inc.)

  • Brian C. Gilger

    (Powered Research, LLC, Research Triangle Park)

  • Christopher S. Crean

    (Graybug Vision, Inc.)

  • Jin-Zhong Zhang

    (Graybug Vision, Inc.)

  • Yogita Kanan

    (Johns Hopkins University School of Medicine)

  • Weiling Yu

    (Graybug Vision, Inc.)

  • Jeffrey L. Cleland

    (Graybug Vision, Inc.)

  • Ming Yang

    (Graybug Vision, Inc.)

  • Justin Hanes

    (Johns Hopkins University School of Medicine)

  • Peter A. Campochiaro

    (Johns Hopkins University School of Medicine)

Abstract

Neovascular age-related macular degeneration and diabetic retinopathy are prevalent causes of vision loss requiring frequent intravitreous injections of VEGF-neutralizing proteins, and under-treatment is common and problematic. Here we report incorporation of sunitinib, a tyrosine kinase inhibitor that blocks VEGF receptors, into a non-inflammatory biodegradable polymer to generate sunitinib microparticles specially formulated to self-aggregate into a depot. A single intravitreous injection of sunitinib microparticles potently suppresses choroidal neovascularization in mice for six months and in another model, blocks VEGF-induced leukostasis and retinal nonperfusion, which are associated with diabetic retinopathy progression. After intravitreous injection in rabbits, sunitinib microparticles self-aggregate into a depot that remains localized and maintains therapeutic levels of sunitinib in retinal pigmented epithelium/choroid and retina for more than six months. There is no intraocular inflammation or retinal toxicity. Intravitreous injection of sunitinib microparticles provides a promising approach to achieve sustained suppression of VEGF signaling and improve outcomes in patients with retinal vascular diseases.

Suggested Citation

  • Hiroki Tsujinaka & Jie Fu & Jikui Shen & Yun Yu & Zibran Hafiz & Joshua Kays & David McKenzie & Delia Cardona & David Culp & Ward Peterson & Brian C. Gilger & Christopher S. Crean & Jin-Zhong Zhang & , 2020. "Sustained treatment of retinal vascular diseases with self-aggregating sunitinib microparticles," Nature Communications, Nature, vol. 11(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-14340-x
    DOI: 10.1038/s41467-020-14340-x
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