首页> 外文OA文献 >Combination of a long-acting delivery system for luteinizing hormone-releasing hormone agonist with Novantrone chemotherapy: increased efficacy in the rat prostate cancer model.
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Combination of a long-acting delivery system for luteinizing hormone-releasing hormone agonist with Novantrone chemotherapy: increased efficacy in the rat prostate cancer model.

机译:用于促黄体激素释放激素激动剂的长效递送系统与Novantrone化疗的组合:在大鼠前列腺癌模型中提高了疗效。

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摘要

The combination of hormonal treatment based on a long-acting delivery system for the agonist [6-D-tryptophan]luteinizing hormone-releasing hormone ([D-Trp6]-LH-RH) with the chemotherapeutic agent Novantrone (mitoxantrone dihydrochloride) was studied in the Dunning R3327H rat prostate cancer model. Microcapsules of [D-Trp6]-LH-RH formulated from poly(DL-lactide-co-glycolide) and calculated to release a controlled dose of 25 micrograms/day were injected intramuscularly once a month. Novantrone (0.25 mg/kg) was injected intravenously once every 3 weeks. Three separate experiments were carried out. When the therapy was started 45 days after transplantation and continued for 70 days, tumor volume in the presence of the microcapsules (966 +/- 219 mm3) or Novantrone (3606 +/- 785 mm3) given alone was significantly decreased compared to controls (14,476 +/- 3045 mm3). However, the combination of microcapsules and Novantrone caused a greater inhibition of tumor growth (189 +/- 31 mm3) than the single agents. Similar effects were seen when the percent increase in tumor volume was examined. Tumor volume increased 10,527 +/- 1803% for the control group. The inhibition of growth caused by the [D-Trp6]LH-RH microcapsules alone (672 +/- 153% increase in volume) was again greater than that caused by Novantrone alone (2722 +/- 421% increase). The combination of the two agents was again the most effective, resulting in an increase in tumor volume of only 105 +/- 29%. Control tumors weighed 30.0 +/- 6.5 g. Tumor weights were much less in the groups treated with either microcapsules (3.28 +/- 0.69 g) or Novantrone (19.53 +/- 3.3 g) alone. The lowest tumor weights after 70 days of treatment were obtained in the group that received the combination of [D-Trp6]LH-RH microcapsules and Novantrone (1.02 +/- 0.2 g). Testes and ventral prostate weights were significantly diminished by the administration of microcapsules of [D-Trp6]LH-RH alone or in combination with Novantrone. In both of these groups, luteinizing hormone and prolactin levels were reduced and serum testosterone was suppressed to undetectable levels. Similar results were obtained in two other experiments in which the duration of treatment was 60 or 105 days. These results suggest that the overall response could reflect the inhibition of proliferation of hormone-independent cancer cells by Novantrone in addition to the suppressive effect of [D-Trp6]LH-RH on the growth of androgen-dependent tumor cells. The administration of Novantrone in combination with microcapsules of [D-Trp6]LH-RH might produce a better clinical response than LH-RH analog alone in patients with advanced prostate carcinoma.
机译:研究了基于长效递送系统的激动剂[6-D-色氨酸]黄体生成激素释放激素([D-Trp6] -LH-RH)的激素治疗与化疗药物Novantrone(米托蒽醌二盐酸盐)的组合在Dunning R3327H大鼠前列腺癌模型中。每月一次肌内注射由聚(DL-丙交酯-共-乙交酯)配制并计算出可释放25微克/天的控制剂量的[D-Trp6] -LH-RH微胶囊。每3周静脉注射一次Novantrone(0.25 mg / kg)。进行了三个单独的实验。当在移植后45天开始治疗并持续70天时,与对照组相比,单独使用微胶囊(966 +/- 219 mm3)或Novantrone(3606 +/- 785 mm3)时的肿瘤体积显着减少( 14,476 +/- 3045毫米3)。然而,微胶囊和诺维酮的组合比单剂对肿瘤生长的抑制作用更大(189 +/- 31 mm3)。当检查肿瘤体积的增加百分比时,可以看到类似的效果。对照组的肿瘤体积增加了10,527 +/- 1803%。单独由[D-Trp6] LH-RH微胶囊引起的生长抑制(体积增加672 +/- 153%)再次大于单独由Novantrone引起的生长抑制(增加2722 +/- 421%)。两种药物的组合再次是最有效的,导致肿瘤体积仅增加105 +/- 29%。对照肿瘤重30.0 +/- 6.5g。单独用微胶囊(3.28 +/- 0.69 g)或诺伏酮(19.53 +/- 3.3 g)处理的组中的肿瘤重量要少得多。在接受[D-Trp6] LH-RH微胶囊和Novantrone(1.02 +/- 0.2 g)组合治疗的组中,治疗70天后的肿瘤重量最低。通过单独或与Novantrone组合使用[D-Trp6] LH-RH微胶囊,可显着减少睾丸和腹侧前列腺的重量。在这两个组中,黄体生成素和催乳激素水平均降低,血清睾丸激素水平降至无法检测的水平。在另外两个实验中获得了相似的结果,其中治疗时间为60天或105天。这些结果表明,除了[D-Trp6] LH-RH对雄激素依赖性肿瘤细胞生长的抑制作用外,总体反应还可能反映出Novantrone对激素非依赖性癌细胞增殖的抑制作用。在晚期前列腺癌患者中,将Novantrone与[D-Trp6] LH-RH微胶囊联合使用可能产生比单独的LH-RH类似物更好的临床反应。

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