A sustained release formulation of novel quininib-hyaluronan microneedles inhibits angiogenesis and retinal vascular permeability in vivo

Orla Galvin; Akshay Srivastava; Oliver Carroll; Rajiv Kulkarni; Steve Dykes; Steven Vickers; Keith Dickinson; Alison L. Reynolds; Claire Kilty; Gareth Redmond; Rob Jones; Sharon Cheetham; Abhay Pandit; Breandán N. Kennedy

doi:10.1016/j.jconrel.2016.04.004

A sustained release formulation of novel quininib-hyaluronan microneedles inhibits angiogenesis and retinal vascular permeability in vivo

Orla Galvin
, Akshay Srivastava
, Oliver Carroll
, Rajiv Kulkarni
, Steve Dykes
, Steven Vickers
, Keith Dickinson
, Alison L. Reynolds
, Claire Kilty
, Gareth Redmond
, Rob Jones
, Sharon Cheetham
, Abhay Pandit
, Breandán N. Kennedy

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

33 Citations (Scopus)

Abstract

Pathologic neovascularisation and ocular permeability are hallmarks of proliferative diabetic retinopathy and age-related macular degeneration. Current pharmacologic interventions targeting VEGF are effective in only 30-60% of patients and require multiple intraocular injections associated with iatrogenic infection. Thus, our goal is to develop novel small molecule drugs that are VEGF-independent are amenable to sustained ocular-release, and which reduce retinal angiogenesis and retinal vascular permeability. Here, the anti-angiogenic drug quininib was formulated into hyaluronan (HA) microneedles whose safety and efficacy was evaluated in vivo. Quininib-HA microneedles were formulated via desolvation from quininib-HA solution and subsequent cross-linking with 4-arm-PEG-amine prior to freeze-drying. Scanning electron microscopy revealed hollow needle-shaped particle ultrastructure, with a zeta potential of - 35.5 mV determined by electrophoretic light scattering. The incorporation efficiency and pharmacokinetic profile of quininib released in vitro from the microneedles was quantified by HPLC. Quininib incorporation into these microneedles was 90%. In vitro, 20% quininib was released over 4 months; or in the presence of increasing concentrations of hyaluronidase, 60% incorporated quininib was released over 4 months. Zebrafish hyaloid vasculature assays demonstrated quininib released from these microneedles significantly (p < 0.0001) inhibited ocular developmental angiogenesis compared to control. Sustained amelioration of retinal vascular permeability (RVP) was demonstrated using a bespoke cysteinyl leukotriene induced rodent model. Quininib-HA microparticles significantly inhibited RVP in Brown Norway rats one month after administration compared to neat quininib control (p = 0.0071). In summary, quininib-HA microneedles allow for sustained release of quininib; are safe in vivo and quininib released from these microneedles effectively inhibits angiogenesis and RVP in vivo.

Original language	English
Pages (from-to)	198-207
Number of pages	10
Journal	Journal of Controlled Release
Volume	233
DOIs	https://doi.org/10.1016/j.jconrel.2016.04.004
Publication status	Published - 10 Jul 2016
Externally published	Yes

Keywords

Angiogenesis
Blindness
Novel drug therapy
Vascular permeability

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.jconrel.2016.04.004

Cite this

Galvin, O., Srivastava, A., Carroll, O., Kulkarni, R., Dykes, S., Vickers, S., Dickinson, K., Reynolds, A. L., Kilty, C., Redmond, G., Jones, R., Cheetham, S., Pandit, A., & Kennedy, B. N. (2016). A sustained release formulation of novel quininib-hyaluronan microneedles inhibits angiogenesis and retinal vascular permeability in vivo. Journal of Controlled Release, 233, 198-207. https://doi.org/10.1016/j.jconrel.2016.04.004

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title = "A sustained release formulation of novel quininib-hyaluronan microneedles inhibits angiogenesis and retinal vascular permeability in vivo",

abstract = "Pathologic neovascularisation and ocular permeability are hallmarks of proliferative diabetic retinopathy and age-related macular degeneration. Current pharmacologic interventions targeting VEGF are effective in only 30-60\% of patients and require multiple intraocular injections associated with iatrogenic infection. Thus, our goal is to develop novel small molecule drugs that are VEGF-independent are amenable to sustained ocular-release, and which reduce retinal angiogenesis and retinal vascular permeability. Here, the anti-angiogenic drug quininib was formulated into hyaluronan (HA) microneedles whose safety and efficacy was evaluated in vivo. Quininib-HA microneedles were formulated via desolvation from quininib-HA solution and subsequent cross-linking with 4-arm-PEG-amine prior to freeze-drying. Scanning electron microscopy revealed hollow needle-shaped particle ultrastructure, with a zeta potential of - 35.5 mV determined by electrophoretic light scattering. The incorporation efficiency and pharmacokinetic profile of quininib released in vitro from the microneedles was quantified by HPLC. Quininib incorporation into these microneedles was 90\%. In vitro, 20\% quininib was released over 4 months; or in the presence of increasing concentrations of hyaluronidase, 60\% incorporated quininib was released over 4 months. Zebrafish hyaloid vasculature assays demonstrated quininib released from these microneedles significantly (p < 0.0001) inhibited ocular developmental angiogenesis compared to control. Sustained amelioration of retinal vascular permeability (RVP) was demonstrated using a bespoke cysteinyl leukotriene induced rodent model. Quininib-HA microparticles significantly inhibited RVP in Brown Norway rats one month after administration compared to neat quininib control (p = 0.0071). In summary, quininib-HA microneedles allow for sustained release of quininib; are safe in vivo and quininib released from these microneedles effectively inhibits angiogenesis and RVP in vivo.",

keywords = "Angiogenesis, Blindness, Novel drug therapy, Vascular permeability",

author = "Orla Galvin and Akshay Srivastava and Oliver Carroll and Rajiv Kulkarni and Steve Dykes and Steven Vickers and Keith Dickinson and Reynolds, \{Alison L.\} and Claire Kilty and Gareth Redmond and Rob Jones and Sharon Cheetham and Abhay Pandit and Kennedy, \{Breand{\'a}n N.\}",

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doi = "10.1016/j.jconrel.2016.04.004",

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Galvin, O, Srivastava, A, Carroll, O, Kulkarni, R, Dykes, S, Vickers, S, Dickinson, K, Reynolds, AL, Kilty, C, Redmond, G, Jones, R, Cheetham, S, Pandit, A & Kennedy, BN 2016, 'A sustained release formulation of novel quininib-hyaluronan microneedles inhibits angiogenesis and retinal vascular permeability in vivo', Journal of Controlled Release, vol. 233, pp. 198-207. https://doi.org/10.1016/j.jconrel.2016.04.004

TY - JOUR

T1 - A sustained release formulation of novel quininib-hyaluronan microneedles inhibits angiogenesis and retinal vascular permeability in vivo

AU - Galvin, Orla

AU - Srivastava, Akshay

AU - Carroll, Oliver

AU - Kulkarni, Rajiv

AU - Dykes, Steve

AU - Vickers, Steven

AU - Dickinson, Keith

AU - Reynolds, Alison L.

AU - Kilty, Claire

AU - Redmond, Gareth

AU - Jones, Rob

AU - Cheetham, Sharon

AU - Pandit, Abhay

AU - Kennedy, Breandán N.

PY - 2016/7/10

Y1 - 2016/7/10

N2 - Pathologic neovascularisation and ocular permeability are hallmarks of proliferative diabetic retinopathy and age-related macular degeneration. Current pharmacologic interventions targeting VEGF are effective in only 30-60% of patients and require multiple intraocular injections associated with iatrogenic infection. Thus, our goal is to develop novel small molecule drugs that are VEGF-independent are amenable to sustained ocular-release, and which reduce retinal angiogenesis and retinal vascular permeability. Here, the anti-angiogenic drug quininib was formulated into hyaluronan (HA) microneedles whose safety and efficacy was evaluated in vivo. Quininib-HA microneedles were formulated via desolvation from quininib-HA solution and subsequent cross-linking with 4-arm-PEG-amine prior to freeze-drying. Scanning electron microscopy revealed hollow needle-shaped particle ultrastructure, with a zeta potential of - 35.5 mV determined by electrophoretic light scattering. The incorporation efficiency and pharmacokinetic profile of quininib released in vitro from the microneedles was quantified by HPLC. Quininib incorporation into these microneedles was 90%. In vitro, 20% quininib was released over 4 months; or in the presence of increasing concentrations of hyaluronidase, 60% incorporated quininib was released over 4 months. Zebrafish hyaloid vasculature assays demonstrated quininib released from these microneedles significantly (p < 0.0001) inhibited ocular developmental angiogenesis compared to control. Sustained amelioration of retinal vascular permeability (RVP) was demonstrated using a bespoke cysteinyl leukotriene induced rodent model. Quininib-HA microparticles significantly inhibited RVP in Brown Norway rats one month after administration compared to neat quininib control (p = 0.0071). In summary, quininib-HA microneedles allow for sustained release of quininib; are safe in vivo and quininib released from these microneedles effectively inhibits angiogenesis and RVP in vivo.

AB - Pathologic neovascularisation and ocular permeability are hallmarks of proliferative diabetic retinopathy and age-related macular degeneration. Current pharmacologic interventions targeting VEGF are effective in only 30-60% of patients and require multiple intraocular injections associated with iatrogenic infection. Thus, our goal is to develop novel small molecule drugs that are VEGF-independent are amenable to sustained ocular-release, and which reduce retinal angiogenesis and retinal vascular permeability. Here, the anti-angiogenic drug quininib was formulated into hyaluronan (HA) microneedles whose safety and efficacy was evaluated in vivo. Quininib-HA microneedles were formulated via desolvation from quininib-HA solution and subsequent cross-linking with 4-arm-PEG-amine prior to freeze-drying. Scanning electron microscopy revealed hollow needle-shaped particle ultrastructure, with a zeta potential of - 35.5 mV determined by electrophoretic light scattering. The incorporation efficiency and pharmacokinetic profile of quininib released in vitro from the microneedles was quantified by HPLC. Quininib incorporation into these microneedles was 90%. In vitro, 20% quininib was released over 4 months; or in the presence of increasing concentrations of hyaluronidase, 60% incorporated quininib was released over 4 months. Zebrafish hyaloid vasculature assays demonstrated quininib released from these microneedles significantly (p < 0.0001) inhibited ocular developmental angiogenesis compared to control. Sustained amelioration of retinal vascular permeability (RVP) was demonstrated using a bespoke cysteinyl leukotriene induced rodent model. Quininib-HA microparticles significantly inhibited RVP in Brown Norway rats one month after administration compared to neat quininib control (p = 0.0071). In summary, quininib-HA microneedles allow for sustained release of quininib; are safe in vivo and quininib released from these microneedles effectively inhibits angiogenesis and RVP in vivo.

KW - Angiogenesis

KW - Blindness

KW - Novel drug therapy

KW - Vascular permeability

UR - https://www.scopus.com/pages/publications/84971231403

U2 - 10.1016/j.jconrel.2016.04.004

DO - 10.1016/j.jconrel.2016.04.004

M3 - Article

SN - 0168-3659

VL - 233

SP - 198

EP - 207

JO - Journal of Controlled Release

JF - Journal of Controlled Release

ER -

A sustained release formulation of novel quininib-hyaluronan microneedles inhibits angiogenesis and retinal vascular permeability in vivo

Abstract

Keywords

UN SDGs

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