Steroid differentiation: the safety profile of various steroids on retinal cells in vitro and their implications for clinical use (an American Ophthalmological Society thesis).

Baruch D Kuppermann, Leandro Cabral Zacharias, M Cristina Kenney
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Abstract

Purpose: To determine if potentially viable alternatives to the clinical use of intravitreal triamcinolone acetonide should be considered based on a comparative assessment of the in vitro effects of five commercially available corticosteroids. We hypothesized that dexamethasone, betamethasone, methylprednisolone, loteprednol etabonate, and fluocinolone acetonide, at clinically relevant doses, may show different levels of in vitro cytotoxicity to retinal cells.

Methods: Cultures of human retinal pigment epithelial cells (ARPE-19) and rat embryonal neurosensory precursor retinal cells (R28) were treated with dexamethasone, betamethasone, methylprednisolone, loteprednol, or fluocinolone acetonide. Cell viability as a measure of cell death was determined by trypan blue dye exclusion assay. The mechanical effect of drug crystals was evaluated by solubilizing the steroid formulations. Mitochondrial dehydrogenase and membrane potential were assessed to measure cell damage.

Results: Betamethasone, loteprednol, and methylprednisolone, in commercially available forms, caused significant cytotoxic changes to retinal cells in vitro at clinically relevant doses. This effect was less pronounced with solubilized betamethasone. Dexamethasone at concentrations up to 5 times the clinical dose of free drug injections and 1000 times greater than a drug implant did not cause decreased cell viability. Fluocinolone acetonide at doses 1000 times higher than observed with drug delivery systems showed no cytotoxic effect.

Conclusions: Betamethasone, loteprednol, and methylprednisolone exhibited cytotoxicity at clinically relevant doses and do not appear to be good therapeutic options for intravitreal use. In comparison, dexamethasone and fluocinolone acetonide, which exhibited fewer cytotoxic effects than other steroids, may be potentially viable alternatives to triamcinolone acetonide for clinical use.

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类固醇分化:各种类固醇对体外视网膜细胞的安全性及其对临床使用的影响(美国眼科学会论文)。
目的:根据对五种市售皮质类固醇体外效应的比较评估,确定是否应考虑在临床上使用玻璃体内曲安奈德的潜在可行替代品。我们假设,在临床相关剂量下,地塞米松、倍他米松、甲基强的松龙、依他泼尼龙和氟西酮缩丙酮可能会对视网膜细胞表现出不同程度的体外细胞毒性:方法:用地塞米松、倍他米松、甲基强的松龙、乐特泼尼龙或氟西酮缩丙酮处理人视网膜色素上皮细胞(ARPE-19)和大鼠胚胎神经感觉前体视网膜细胞(R28)。细胞存活率通过胰蓝染料排阻试验来测定。通过溶解类固醇制剂来评估药物晶体的机械效应。通过评估线粒体脱氢酶和膜电位来衡量细胞损伤程度:结果:倍他米松、乐特泼尼龙和甲基泼尼松龙等市售药物在体外以临床相关剂量对视网膜细胞产生了明显的细胞毒性变化。这种效应在溶解的倍他米松中不太明显。地塞米松的浓度是临床免费药物注射剂量的 5 倍,是药物植入浓度的 1000 倍,但不会导致细胞活力下降。氟西诺龙-丙酮的剂量比药物输送系统的剂量高 1000 倍,也没有显示出细胞毒性作用:结论:倍他米松、乐特泼尼龙和甲基泼尼松龙在临床相关剂量下显示出细胞毒性,似乎不是玻璃体内使用的良好治疗选择。相比之下,地塞米松和氟西酮缩丙酮的细胞毒性作用比其他类固醇要小,有可能成为三苯氧胺缩丙酮的替代品,用于临床治疗。
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