The inhibitory effect of small interference RNA protein kinase C-alpha on the experimental proliferative vitreoretinopathy induced by dispase in mice

Gao, Qiangying; Wang, Wencong; Lan, Yuqing; Chen, Xiaoqing; Yang, Wei; Yuan, Yongguang; Tan, Juan; Zong, Yao; Jiang, Zhaoxin

doi:10.2147/ijn.s37635

Cited by 5 publications

(3 citation statements)

References 32 publications

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“…27 Currently, the most popular mouse PVR model uses injection of the proteolytic enzyme dispase. [28][29][30][31] Although dispase injection may trigger events that lead to PVR formation, such as cells invading the vitreous cavity, retinal folds, and the appearance of intravitreal membranes, 28 the integrity of the retina is severely affected. The dispase enzyme breaks down the retina structure, producing marked hemorrhage, which does not mimic human PVR pathogenesis or progression.…”

Section: Introductionmentioning

confidence: 99%

A Mouse Model of Proliferative Vitreoretinopathy Induced by Intravitreal Injection of Gas and RPE Cells

Heffer

Wang

Sridhar

et al. 2020

Trans. Vis. Sci. Tech.

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Develop a reproducible proliferative vitreoretinopathy (PVR) mouse model that mimics human PVR pathology. Methods: Mice received intravitreal injections of SF 6 gas, followed by retinal pigment epithelial cells 1 week later. PVR progression was monitored using fundus photography and optical coherence tomography imaging, and histologic analysis of the retina as an endpoint. We developed a PVR grading scheme tailored for this model. Results: We report that mice that received gas before retinal pigment epithelial injection developed more severe PVR. In the 1 × 10 4 retinal pigment epithelial cell group, after 1 week, 0 of 11 mice in the no gas group developed grade 4 or greater PVR compared with 5 of 13 mice in the SF 6 gas group (P = 0.02); after 4 weeks, 3 of 11 mice in the no gas group developed grade 5 or greater PVR compared with 11 of 14 mice in the SF 6 gas group (P = 0.01). We were able to visualize contractile membranes both on the retinal surface as well as within the vitreous of PVR eyes, and demonstrated through immunohistochemical staining that these membranes expressed fibrotic markers alpha smooth muscle actin, vimentin, and fibronectin, as well as other markers known to be found in human PVR membranes. Conclusions: This mouse PVR model is reproducible and mimics aspects of PVR pathology reported in the rabbit PVR model and human PVR. The major advantage is the ability to study PVR development in different genetic backgrounds to further elucidate aspects of PVR pathogenesis. Additionally, large-scale experiments for testing pharmacologic agents to treat and prevent PVR progression is more feasible compared with other animal models. Translational Relevance: This model will provide a platform for screening potential drug therapies to treat and prevent PVR, as well as elucidate different molecular pathways involved in PVR pathogenesis.

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Section: Introductionmentioning

confidence: 99%

A Mouse Model of Proliferative Vitreoretinopathy Induced by Intravitreal Injection of Gas and RPE Cells

Heffer

Wang

Sridhar

et al. 2020

Trans. Vis. Sci. Tech.

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“…Downregulation of VEGFR2 might be a possible target of the anti-NV action of ART. PKCα is involved in the pathophysiological processes of DR 26 27 and was also found to promote retinal pigment epithelial (RPE) cell proliferation in proliferative vitreoretinopathy (PVR) in our previous study 28 29 . The PKCα inhibitor midostaurin (PKC412A) has been used in a phase IIA study of metastatic melanoma 30 .…”

Section: Discussionmentioning

confidence: 89%

Small Molecular-Sized Artesunate Attenuates Ocular Neovascularization via VEGFR2, PKCα and PDGFR Targets

Zong

Yuan

Qian

et al. 2016

Sci Rep

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Ocular neovascularization (NV) is the primary cause of blindness in many ocular diseases. Large molecular weight anti- vascular endothelial growth factor (VEGF) protein drugs, such as Avastin and Lucentis, have saved the vision of millions. However, approximately 20–30% of patients respond poorly to anti-VEGF treatment. We found that artesunate (ART), a small molecular derivative of artemisinin, had a significant inhibitory effect on ocular NV by downregulating the expression of VEGFR2, PKCα, and PDGFR. ART significantly inhibited retinal NV in rabbits and macular edema in monkeys with greater anterior chamber penetrability and more durable efficacy than Avastin. Our pilot study showed that intravitreal injection of 80 μg ART significantly inhibited iris and corneal NV in a severe retinal detachment case. Our results suggest that ART might be a potential persistent small-molecule drug to manage ocular NV via multi-targets.

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“…Corticosteroids [ 1 – 6 ] antiproliferative agents (5-fluoro-uracil and other fluoropyrimidines, taxol, doxorubicin, mycophenolate mofetil…, alone or in combination or with different delivery systems) [ 3 – 12 ], systemic, periocular, intraocular steroidal, and nonsteroidal anti-inflammatory agents [ 5 , 13 – 16 ], colchicine [ 8 ], daunomycin [ 8 ], tissue plasminogen activator [ 17 ], heparin [ 12 , 18 – 20 ], interferon-gamma [ 21 , 22 ], calcium channel blockers [ 23 ], prolyl and lysyl hydroxylase inhibitors [ 19 , 24 – 26 ], retinoic acid [ 27 , 28 ], alpha-tocopherol [ 29 – 31 ], disintegrins [ 32 ], siRNA-PKC α [ 33 ]… are some of the useful drugs that have been used in the treatment of conditions such as proliferative vitreoretinopathy, bleb scarring after trabeculectomy, and other disorders with cell proliferation (progressive conjunctival or extraocular cicatrization).…”

Section: Introductionmentioning

confidence: 99%

In VitroVitamin K₃Effect on Conjunctival Fibroblast Migration and Proliferation

Pinilla

Izaguirre²,

Gonzalvo

et al. 2014

The Scientific World Journal

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Purpose. To evaluate the dose effect of vitamin K3 on wound healing mechanisms. Methods. Conjunctival fibroblasts were incubated for 24 hours. An artificial wound was made and the cells were incubated with fresh medium plus doses of vitamin K3 to be tested. Wound repair was monitored at 0, 18, 24, and 48 hours. Proliferation was measured in actively dividing cells by [3H]thymidine uptake. Six different groups were tested: group 1/no drugs added, group 2/ethanol 0.1%, group 3/vitamin K3 1 mg/L, group 4/vitamin K3 2 mg/L, group 5/vitamin K3 4 mg/L, and group 6/vitamin K3 6 mg/L. Each experiment was carried out in triplicate and 4 times. Results. There were no differences among groups at the initial time. In vitro wound repair was slower in groups 4, 5, and 6. There were no differences between control and ethanol groups and between control and vitamin K3 1 mg/L groups. Fibroblast mitogenic activity was statistically decreased in all vitamin K groups; statistical differences were found among vitamin K3 1 mg/mL and higher doses too. In groups 5 and 6, cellular toxicity was presented. Conclusions. Vitamin K3 is able to inhibit fibroblast proliferation. Vitamin K3 2 mg/L or higher doses inhibit wound healing repair, exhibiting cellular toxicity at 4 and 6 mg/L.

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The inhibitory effect of small interference RNA protein kinase C-alpha on the experimental proliferative vitreoretinopathy induced by dispase in mice

Cited by 5 publications

References 32 publications

A Mouse Model of Proliferative Vitreoretinopathy Induced by Intravitreal Injection of Gas and RPE Cells

A Mouse Model of Proliferative Vitreoretinopathy Induced by Intravitreal Injection of Gas and RPE Cells

Small Molecular-Sized Artesunate Attenuates Ocular Neovascularization via VEGFR2, PKCα and PDGFR Targets

In VitroVitamin K₃Effect on Conjunctival Fibroblast Migration and Proliferation

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The inhibitory effect of small interference RNA protein kinase C-alpha on the experimental proliferative vitreoretinopathy induced by dispase in mice

Cited by 5 publications

References 32 publications

A Mouse Model of Proliferative Vitreoretinopathy Induced by Intravitreal Injection of Gas and RPE Cells

A Mouse Model of Proliferative Vitreoretinopathy Induced by Intravitreal Injection of Gas and RPE Cells

Small Molecular-Sized Artesunate Attenuates Ocular Neovascularization via VEGFR2, PKCα and PDGFR Targets

In VitroVitamin K3Effect on Conjunctival Fibroblast Migration and Proliferation

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In VitroVitamin K₃Effect on Conjunctival Fibroblast Migration and Proliferation