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局部非病毒IL12基因治疗与全身紫杉醇治疗联合应用于转移性乳腺癌模型

Combination of local, nonviral IL12 gene therapy and systemic paclitaxel treatment in a metastatic breast cancer model.

作者信息

Janát-Amsbury Margit Maria, Yockman James W, Lee Minhyung, Kern Steven, Furgeson Darin Y, Bikram Malavosklish, Kim Sung Wan

机构信息

Center for Controlled Chemical Delivery, Department of Pharmaceutics and Pharmaceutical Chemistry, University of Utah, 20 South 2030 East, Salt Lake City, UT 84112, USA.

出版信息

Mol Ther. 2004 Jun;9(6):829-36. doi: 10.1016/j.ymthe.2004.03.015.

Abstract

Repeated, local, nonviral IL12 (interleukin-12) gene delivery decreased tumor progression and increased immunogenicity. We combined our IL12 gene delivery with systemic paclitaxel chemotherapy as a treatment for paclitaxel (PCT)-resistant 4T1 subcutaneous mouse mammary carcinomas and PCT-sensitive, immunogenic/nonimmunogenic tumors. We mixed PCT with either a biodegradable polymeric solubilizer, HySolv, or Cremophor EL for bimonthly systemic treatments and injected water-soluble lipopolymer (WSLP)/p2CMVmIL-12 (plasmid encoding IL12 gene) complexes locally every week. We compared treated subcutaneous tumor volume and lung metastasis with controls. HySolv alone performed better compared to Cremophor EL in combination with WSLP/p2CMVmIL-12. We showed inhibition of 4T1 tumor growth and lung metastases in the combined WSLP/p2CMVmIL-12/HySolv group compared to the controls and the paclitaxel-only treated groups. In parallel experiments we also demonstrated additive responses for tumor growth and number of lung metastases within other PCT-sensitive mammary tumor models using this combination strategy. Our combination therapy provides evidence for the efficacy and feasibility of improved drug delivery systems. Local cytokine gene delivery can augment local and systemic chemotherapy without placing the host at risk for further systemic toxicity.

摘要

重复进行局部非病毒白细胞介素12(IL12)基因递送可降低肿瘤进展并增强免疫原性。我们将IL12基因递送与全身紫杉醇化疗相结合,用于治疗对紫杉醇(PCT)耐药的4T1皮下小鼠乳腺癌以及对PCT敏感的免疫原性/非免疫原性肿瘤。我们将PCT与可生物降解的聚合物增溶剂HySolv或聚氧乙烯蓖麻油(Cremophor EL)混合,进行每两个月一次的全身治疗,并每周局部注射水溶性脂质聚合物(WSLP)/p2CMVmIL-12(编码IL12基因的质粒)复合物。我们将治疗后的皮下肿瘤体积和肺转移情况与对照组进行比较。与聚氧乙烯蓖麻油(Cremophor EL)联合WSLP/p2CMVmIL-12相比,单独使用HySolv效果更好。与对照组和仅接受紫杉醇治疗的组相比,我们发现联合WSLP/p2CMVmIL-12/HySolv组对4T1肿瘤生长和肺转移有抑制作用。在平行实验中,我们还证明了使用这种联合策略在其他对PCT敏感的乳腺肿瘤模型中对肿瘤生长和肺转移数量有相加反应。我们的联合疗法为改进药物递送系统的有效性和可行性提供了证据。局部细胞因子基因递送可以增强局部和全身化疗效果,而不会使宿主面临进一步的全身毒性风险。

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