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Assessment of the efficacy of repeated instillations of mitomycin C mixed with a thermosensitive hydrogel in an orthotopic rat bladder cancer model

机译:在原位大鼠膀胱癌模型中评估丝裂霉素C与热敏水凝胶混合反复滴注的疗效

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We investigated a thermoreversible hydrogel that is highly viscous at body temperature, while fluid-like at a low temperature, thus aiming for a slow and prolonged intravesical drug release. Our study purposed to assess antitumor efficacy of mitomycin C (MMC) mixed with hydrogel in an orthotopic rat bladder cancer model. Bladders of female Fischer F344 rats were grafted with 1.5 × 106 AY-27 urothelial carcinoma cells. On day 5, tumor presence was assessed by cystoscopy and rats were divided into six groups (five treatment, one control, n = 10/group). Intravesical treatments (0.5 mg or 1 mg MMC-H2O or MMC-hydrogel, or 2 mg MMC-hydrogel) were administered on days 5, 8 and 11. Rats were sacrificed at day 14 and bladders were evaluated. Rats with tumor at cystoscopy (47/60) were evaluated for efficacy. At necropsy, all control animals (8/8) had tumors. No microscopic tumors were present in the 0.5 mg and 1 mg MMC-hydrogel groups compared with 2/8 and 1/8 rats in the 0.5 mg and 1 mg MMC-H2O groups (p = 0.47 and p = 1.00, respectively). Greater toxicity was seen in animals treated with MMC-hydrogel compared with MMC-H2O, as demonstrated by lower body weights at necropsy (p = 0.000) and a tendency for more severe clinical signs in the 1 and 2 mg MMC-hydrogel groups. Rats that died prematurely received 1 mg (4/10) or 2 mg (9/10) of MMC-hydrogel. Under the current model conditions it is unclear whether instillation of MMC-hydrogel is more effective than MMC-H2O. Nonetheless, the observed difference in toxicity, acting as a surrogate marker for systemic MMC exposure in the MMC-hydrogel-treated rats, supports the prolonged drug release mechanism of the hydrogel.
机译:我们研究了一种热可逆的水凝胶,它在体温下具有高粘性,而在低温下则呈流体状,因此旨在缓慢且延长膀胱内药物的释放。我们的研究旨在评估丝裂霉素C(MMC)与水凝胶混合在原位大鼠膀胱癌模型中的抗肿瘤功效。将雌性Fischer F344大鼠的膀胱移植1.5×106 AY-27尿路上皮癌细胞。在第5天,通过膀胱镜检查评估肿瘤的存在,并将大鼠分为六组(五种治疗,一个对照,n = 10 /组)。在第5、8和11天进行膀胱内治疗(0.5 mg或1 mg MMC-H2O或MMC-水凝胶,或2 mg MMC-水凝胶),在第14天处死大鼠并评估膀胱。评估膀胱镜检查肿瘤的大鼠(47/60)的功效。尸检时,所有对照动物(8/8)均患有肿瘤。与0.5 mg和1 mg MMC-H2O组的2/8和1/8大鼠相比,0.5 mg和1 mg MMC-水凝胶组中没有显微镜观察到的肿瘤(分别为p = 0.47和p = 1.00)。与MMC-H2O相比,用MMC-水凝胶治疗的动物毒性更高,尸检时体重较低(p = 0.000),并且在1和2 mg MMC-水凝胶组中有更严重的临床体征。过早死亡的大鼠接受1 mg(4/10)或2 mg(9/10)的MMC水凝胶。在当前模型条件下,尚不清楚MMC-水凝胶的滴注是否比MMC-H2O更有效。尽管如此,观察到的毒性差异作为MMC水凝胶治疗大鼠全身性MMC暴露的替代标志物,支持了水凝胶延长的药物释放机制。

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