Hesperidin Prevents Retinal and Plasma Abnormalities in Streptozotocin-Induced Diabetic Rats

Shi, Xiupu; Liao, Sha; Mi, Huijuan; Guo, Chengjun; Qi, Dongli; Li, Fēi; Zhang, Chunfeng; Yang, Zhonglin

doi:10.3390/molecules171112868

Cited by 107 publications

(75 citation statements)

References 42 publications

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“…Not only was HFVC an independent predictor of diabetes-related biomarkers, but for each 10 U increase in HFVC index, participants had 33% lower odds to have retinopathy. This significant finding is supported in the literature via animal and in vitro work (Kim et al, 2012;Kumar et al, 2013;Shi et al, 2012). Importantly, our work, unlike these previous animal-related studies, demonstrates that flavonoid consumption achieved through normal fruit and vegetable intake, rather than supplementation, is associated with diabetesrelated biomarkers and diabetic retinopathy.…”

Section: Discussioncontrasting

confidence: 76%

Influence of flavonoid-rich fruit and vegetable intake on diabetic retinopathy and diabetes-related biomarkers

Mahoney

Loprinzi

2014

Journal of Diabetes and its Complications

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Section: Discussioncontrasting

confidence: 76%

Influence of flavonoid-rich fruit and vegetable intake on diabetic retinopathy and diabetes-related biomarkers

Mahoney

Loprinzi

2014

Journal of Diabetes and its Complications

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“…When evaluated using the retinal accumulation of Evans blue or other plasma tracers, BRBB was reported as early as 5 days and up to 10 weeks post-STZ treatment. 3,4,9,[11][12][13][14] Here, we confirmed the early and sustained damage of the BRB in this diabetes model by showing that a significant increase in the retinal accumulation of Evans blue-stained albumin occurs at 2 weeks AAV2 vectors reverse diabetic retinal alterations N Díaz-Lezama et al after STZ injection and is maintained at a similar level during the following 4 and 6 weeks (Figure 2a). To investigate the restoration of the BRB function, vehicle or 2.8 × 10 9 vg of the AAV2 vasoinhibin vector or the AAV2 sFlt-1 vector was injected intravitreally into non-diabetic or diabetic rats 2 weeks after treatment with STZ, and the BRBB was quantified 4 weeks after vector administration by the retinal accumulation of Evans blue.…”

Section: Discussionsupporting

confidence: 71%

Diabetes enhances the efficacy of AAV2 vectors in the retina: therapeutic effect of AAV2 encoding vasoinhibin and soluble VEGF receptor 1

Díaz‐Lezama

Adán‐Castro

et al. 2016

Laboratory Investigation

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Adeno-associated virus (AAV) vector-mediated delivery of inhibitors of blood-retinal barrier breakdown (BRBB) offers promise for the treatment of diabetic macular edema. Here, we demonstrated a reversal of blood-retinal barrier pathology mediated by AAV type 2 (AAV2) vectors encoding vasoinhibin or soluble VEGF receptor 1 (sFlt-1) when administered intravitreally to diabetic rats. Efficacy and safety of the AAV2 vasoinhibin vector were tested by monitoring its effect on diabetes-induced changes in the retinal vascular bed and thickness, and in the electroretinogram (ERG). Also, the transduction of AAV2 vectors and expression of AAV2 receptors and co-receptors were compared between the diabetic and the non-diabetic rat retinas. AAV2 vasoinhibin or AAV2 sFlt-1 vectors were injected intravitreally before or after enhanced BRBB due to diabetes induced by streptozotocin. The BRBB was examined by the Evans blue method, the vascular bed by fluorescein angiography, expression of the AAV2 EGFP reporter vector by confocal microscopy, and the AAV2 genome, expression of transgenes, receptors, and co-receptors by quantitative PCR. AAV2 vasoinhibin and sFlt-1 vectors inhibited the diabetes-mediated increase in BRBB when injected after, but not before, diabetes was induced. The AAV2 vasoinhibin vector decreased retinal microvascular abnormalities and the diabetes-induced reduction of the B-wave of the ERG, but it had no effect in non-diabetic controls. Also, retinal thickness was not altered by diabetes or by the AAV2 vasoinhibin vector. The AAV2 genome, vasoinhibin and sFlt-1 transgenes, and EGFP levels were higher in the retinas from diabetic rats and were associated with an elevated expression of AAV2 receptors (syndecan, glypican, and perlecan) and co-receptors (fibroblast growth factor receptor 1, αvβ5 integrin, and hepatocyte growth factor receptor). We conclude that retinal transduction and efficacy of AAV2 vectors are enhanced in diabetes, possibly due to their elevated cell entry. AAV2 vectors encoding vasoinhibin and sFlt-1 may be desirable gene therapeutics to target diabetic retinopathy and macular edema.

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“…The concept of ICAM-1 inhibition has become a potential therapeutic strategy for the prevention of diabetic retinopathy (Joussen et al, 2001;Miyamoto et al, 1999). Some flavonoid compounds, such as hesperidin, trans-chalcone, and minocycline, were reported to possess properties to inhibit diabetic-induced (Lamoke et al, 2011) or ischemia-induced (Abcouwer et al, 2013;Shi et al, 2012) ICAM-1 expression in retina. Our immunofluorescence and Western blot analysis also clearly supported that silybin effectively inhibited the up-regulated ICAM-1 protein (Fig.…”

Section: Discussionmentioning

confidence: 99%

Silybin reduces obliterated retinal capillaries in experimental diabetic retinopathy in rats

Zhang

Shi

Baskota

et al. 2014

European Journal of Pharmacology

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Hesperidin Prevents Retinal and Plasma Abnormalities in Streptozotocin-Induced Diabetic Rats

Cited by 107 publications

References 42 publications

Influence of flavonoid-rich fruit and vegetable intake on diabetic retinopathy and diabetes-related biomarkers

Influence of flavonoid-rich fruit and vegetable intake on diabetic retinopathy and diabetes-related biomarkers

Diabetes enhances the efficacy of AAV2 vectors in the retina: therapeutic effect of AAV2 encoding vasoinhibin and soluble VEGF receptor 1

Silybin reduces obliterated retinal capillaries in experimental diabetic retinopathy in rats

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