首页> 外文期刊>Saudi Pharmaceutical Journal >Evaluation of the in vivo genotoxicity of liposomal formulation for delivering anticancer estrogenic derivative (ESC8) in a mouse model
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Evaluation of the in vivo genotoxicity of liposomal formulation for delivering anticancer estrogenic derivative (ESC8) in a mouse model

机译:评价脂质体制剂在小鼠模型中递送抗癌雌激素衍生物(ESC8)的体内遗传毒性

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The genotoxic potential of glucocorticoid receptor (GR)-targeted liposomal formulations of the anticancer drug molecule ESC8 was studied in vivo . A methodical literature review discovered no previous studies on the genotoxicity of ESC8. Genotoxicity was assessed in both male and female mice by various assay systems, such as comet assay, chromosomal aberrations and micronuclei assay, which detect different abnormalities. Eleven groups of male mice and eleven groups of female mice, containing six animals per group, were used in the present study: group I served as vehicle control; group II received the positive control (cyclophosphamide 40?mg/kg; CYP); and animals in group III to XI received free drug (ESC8), DX liposome and drug-associated DX liposomal formulation (DXE), respectively, dissolved in 5% solution of glucose at a drug-dose of 1.83, 3.67 and 7.34?mg/kg, respectively. Same drug treatments were followed for the female mice groups. The obtained data revealed the safety of DXE, which did not show substantial genotoxic effects at different dose levels. In contrast, the positive control, CYP, exhibited highly substantial irregular cytogenetic variations in comparison with the control group in different assays.
机译:在体内研究了以糖皮质激素受体(GR)为靶点的抗癌药物分子ESC8的脂质体制剂的遗传毒性潜力。有条理的文献综述未发现有关ESC8遗传毒性的先前研究。通过各种检测系统(如彗星检测,染色体畸变和微核检测)评估了雄性和雌性小鼠的基因毒性,这些系统可检测不同的异常情况。在本研究中使用了11组雄性小鼠和11组雌性小鼠,每组包含6只动物。 II组接受阳性对照(环磷酰胺40?mg / kg; CYP)。第III至XI组的动物分别接受了游离药物(ESC8),DX脂质体和与药物相关的DX脂质体制剂(DXE),它们分别以1.83、3.67和7.34?mg / mg的剂量溶解在5%葡萄糖溶液中公斤。对雌性小鼠组进行相同的药物治疗。获得的数据揭示了DXE的安全性,在不同剂量水平下并未显示出明显的遗传毒性作用。相反,在不同的试验中,与对照组相比,阳性对照组CYP表现出高度实质性的不规则细胞遗传学变异。

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