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Growth inhibition of a human ovarian tumor by a novel paclitaxel derivative in SCID mice.

机译:一种新型紫杉醇衍生物在SCID小鼠中对人卵巢肿瘤的生长抑制作用。

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We report here the toxicity and therapeutic effects of 2'-alpha-bromohexadecanoyl paclitaxel (BrC16HT), a prodrug form of paclitaxel, in mice. Paclitaxel is the active ingredient of Taxol. The maximum tolerated dose, at a one dose per day for 5-day schedule, was 37.5 mg/kg for BrC16HT compared to 12.5 for Taxol administered IP, and was 12.5-25 mg/kg for either agent administered IV. Dose-dependent therapeutic effects were found for BrC16HT against a human ovarian tumor (OVCAR-3) grown in SCID mice. IP treatments with BrC16HT against early or established IP-implanted OVCAR-3 tumor increased mean survival times more than treatment with Taxol. Long-term survivors were found only in groups treated with BrC16HT. Intravenously administered BrC16HT was more effective than Taxol against SC OVCAR-3 tumor. Early treatment (25 mg/kg x 5) completely inhibited tumor growth through 120 days after tumor implantation. Pharmacokinetic studies suggest that BrC16HT is slowly hydrolyzed to paclitaxel and circulates longer than paclitaxel from Taxol. Thus, BrC16HT may provide sustained levels of paclitaxel, which may contribute to the increased efficacy of BrC16HT compared to Taxol.
机译:我们在这里报告2'-α-溴十六烷酰基紫杉醇(BrC16HT),紫杉醇的前药形式在小鼠中的毒性和治疗作用。紫杉醇是紫杉醇的活性成分。在5天的时间表中,每天一剂的最大耐受剂量对BrC16HT为37.5 mg / kg,而对IP的紫杉醇给药为12.5,对于任何一种IV给药为12.5-25 mg / kg。发现BrC16HT对SCID小鼠中生长的人类卵巢肿瘤(OVCAR-3)具有剂量依赖性的治疗作用。与早期使用紫杉醇治疗相比,用BrC16HT进行IP治疗能更早地治愈已建立IP的OVCAR-3肿瘤。长期幸存者仅在用BrC16HT治疗的组中发现。静脉内给予BrC16HT比紫杉醇对SC OVCAR-3肿瘤更有效。早期治疗(25 mg / kg x 5)在肿瘤植入后的120天内完全抑制了肿瘤的生长。药代动力学研究表明,BrC16HT缓慢水解为紫杉醇,并且比紫杉醇中的紫杉醇循环更长。因此,与紫杉醇相比,BrC16HT可以提供持续水平的紫杉醇,这可能有助于增加BrC16HT的功效。

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