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Combination of paclitaxel thermal gel depot with temozolomide and radiotherapy significantly prolongs survival in an experimental rodent glioma model

机译:紫杉醇热凝胶仓与替莫唑胺和放疗的组合显着延长了实验啮齿动物胶质瘤模型的存活

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OncoGel™ incorporates paclitaxel, a mitotic inhibitor, into ReGel™, a thermosensitive gel depot system to provide local delivery, enhance efficacy and limit systemic toxicity. In previous studies the alkylating agent temozolomide (TMZ) incorporated into a polymer, pCPP:SA, also for local delivery, and OncoGel were individually shown to increase efficacy in a rat glioma model. We investigated the effects of OncoGel with oral TMZ or locally delivered TMZ polymer, with and without radiotherapy (XRT) in rats with intracranial gliosarcoma. Eighty-nine animals were intracranially implanted with a 9L gliosarcoma tumor and divided into 12 groups that received various combinations of 4 treatment options; OncoGel 6.3 mg/ml (Day 0), 20 Gy XRT (Day 5), 50 % TMZ–pCPP:SA (Day 5), or oral TMZ (50 mg/kg, qd, Days 5–9). Animals were followed for survival for 120 days.Median survival for untreated controls, XRT alone or oral TMZ alone was 15, 19 and 28 days, respectively. OncoGel 6.3 or TMZ polymer alone extended median survival to 33 and 35 days, respectively (p = 0.0005; p < 0.0001, vs. untreated controls) with 50 % living greater than 120 days (LTS) in both groups. Oral TMZ/XRT extended median survival to 36 days (p = 0.0002), with no LTS. The group that received OncoGel and Oral TMZ did not reach median survival with 57 % LTS (p = 0.0002). All other combination groups [OncoGel/XRT], [TMZ polymer/XRT], [OncoGel/TMZ polymer], [OncoGel/TMZ polymer/XRT], and [OncoGel/oral TMZ/XRT] yielded greater than 50 % LTS (p < 0.0001 for each combination as compared to controls), therefore median survival was not reached. OncoGel/TMZ polymer and OncoGel/oral TMZ/XRT had 100 % LTS (p < 0.0001 and p = 0.0001 vs. oral TMZ/XRT, respectively). These results indicate that OncoGel given locally with oral or locally delivered TMZ and/or XRT significantly increased the number of LTS and improved median survival compared to oral TMZ and XRT given alone or in combination in a rodent intracranial gliosarcoma model.
机译:OncoGel™将紫杉醇(一种有丝分裂抑制剂)掺入了ReGel™(一种热敏凝胶储库系统)中,以提供局部递送,增强功效并限制全身毒性。在先前的研究中,烷基化剂替莫唑胺(TMZ)掺入聚合物pCPP:SA(也用于局部递送)和OncoGel分别显示在大鼠神经胶质瘤模型中提高疗效。我们研究了在有或没有放疗(XRT)的情况下,口服TMZ或局部递送的TMZ聚合物对OncoGel的影响。将89只动物颅内植入9L胶质肉瘤,并分为12组,分别接受4种治疗方案的不同组合。 OncoGel 6.3 mg / ml(第0天),20 Gy XRT(第5天),50%TMZ-pCPP:SA(第5天)或口服TMZ(50 mg / kg,每日一次,第5-9天)。追踪动物存活120天。未经治疗的对照,单独XRT或单独口服TMZ的中位存活分别为15、19和28天。单独使用OncoGel 6.3或TMZ聚合物可使中位生存期分别延长至33天和35天(与未经治疗的对照组相比,p = 0.0005; p <0.0001),两组的50%生存时间均大于120天(LTS)。口服TMZ / XRT,无LTS可使中位生存期延长至36天(p = 0.0002)。接受OncoGel和Oral TMZ治疗的组中LTS的中位生存期未达到57%(p = 0.0002)。所有其他组合组[OncoGel / XRT],[TMZ聚合物/ XRT],[OncoGel / TMZ聚合物],[OncoGel / TMZ聚合物/ XRT]和[OncoGel /口服TMZ / XRT]的LTS大于50%(p与对照相比,每种组合<0.0001),因此未达到中位生存期。 OncoGel / TMZ聚合物和OncoGel /口服TMZ / XRT具有100%的LTS(相对于口服TMZ / XRT分别为p <0.0001和p = 0.0001)。这些结果表明,与在啮齿类颅内眼睑肉瘤模型中单独或组合给予的口服TMZ和XRT相比,与口服或局部递送的TMZ和/或XRT局部给予的OncoGel显着增加了LTS的数量,并改善了中位生存期。

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