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This abstract is assigned to session FRO: Fund for Research in Ophthalmology
TitleFRO: The effect of AMA0428, a novel rock inhibitor, in a model of wet age-related macular degeneration
Abstract Nr.1029
PurposeRho kinase (ROCK) is associated with VEGF-driven angiogenesis and is involved in inflammation and fibrosis. Therefore, the effect of a novel ROCK inhibitor, AMA0428, was studied in wet age-related macular degeneration (AMD).
MethodsThe effect of AMA0428 on human brain microvascular endothelial cells (HBMEC), human brain vascular pericytes (HBVP) and human tenon fibroblasts (HTF) was determined by measuring cell viability (WST-1), apoptosis (caspase 3/7) and 2 migration assays (scratch and under-agarose) The in vivo response was investigated using a laser-induced choroidal neovascularization (CNV) mouse model. Intravitreal injections were given on day 0, 4, 10 and 20 with AMA0428, murine anti-VEGFR Ab (DC101) or placebo. Outcome was assessed by analysis of inflammation (CD45), angiogenesis (FITC-dextran), vessel leakage (Texas Red-conjugated Dextran and FITC-labeled lectin) and fibrosis (Collagen I).
ResultsAMA0428 dose-dependently reduced proliferation and VEGF-induced migration of HBMEC and HTF. No significant effect was seen on HBVP proliferation; however, migration and pericyte recruitment were increased. There was no apoptosis induction. AMA0428 significantly reduced CNV and vessel leakage 2 weeks after laser treatment, comparable to DC101. In addition, AMA0428 inhibited inflammation on day 5 by 20% and collagen deposition on day 30 by 39% while DC101 had no effect on inflammation nor fibrosis.
ConclusionOur data suggest that targeting ROCK with AMA0428 not only reduces neoangiogenesis, but also blocks inflammation and fibrosis (contrary to anti-VEGF). These results point to a potential therapeutic benefit of ROCK inhibition in wet AMD.
Authors 1
Last nameHOLLANDERS
InitialsK
DepartmentKUL
CityLeuven
Authors 2
Last nameVan Bergen
InitialsT
DepartmentKUL
CityLeuven
Authors 3
Last nameVandewalle
InitialsE
DepartmentKUL
CityLeuven
Authors 4
Last nameCastermans
InitialsK
DepartmentAmakem
CityDiepenbeek
Authors 5
Last nameKindt
InitialsN
DepartmentAmakem
CityDiepenbeek
Authors 6
Last nameMoons
InitialsL
DepartmentKUL
CityLeuven
Authors 7
Last nameStalmans
InitialsI
DepartmentKUL
CityLeuven
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