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光激活紫杉醇前药对大鼠乳腺癌模型的局部和全身抗肿瘤作用。

Local and Systemic Antitumor Effects of Photo-activatable Paclitaxel Prodrug on Rat Breast Tumor Models.

机构信息

Department of Pharmaceutical Sciences, College of Pharmacy, University of Oklahoma Health Sciences Center, Oklahoma City, OK.

Clinical Pharmacology Program, National Cancer Institute, NIH, Bethesda, MD.

出版信息

Photochem Photobiol. 2020 May;96(3):668-679. doi: 10.1111/php.13202. Epub 2020 Mar 9.

Abstract

We demonstrated that a large primary and a small untreated distant breast cancer could be controlled by local treatment with our light-activatable paclitaxel (PTX) prodrug. We hypothesized that the treated tumor would be damaged by the combinational effects of photodynamic therapy (PDT) and locally released PTX and that the distant tumor would be suppressed by systemic antitumor effects. Syngeneic rat breast cancer models (single- and two-tumor models) were established on Fischer 344 rats by subcutaneous injection of MAT B III cells. The rats were injected with PTX prodrug (dose: 1 umole kg , i.v.), and tumors were treated with illumination using a 690-nm laser (75 or 140 mW cm for 30 min, cylindrical light diffuser, drug-light interval [DLI] 9 h). Larger tumors (16 mm) were effectively ablated (100%) without recurrence for >90 days. All cured rats rejected rechallenged tumor for up to 12 months. In the two-tumor model, the treatment of the local large tumor (16 mm) also cured the untreated tumor (4-6 mm) through adaptive immune activation. This is our first demonstration that local treatment with our PTX prodrug produces systemic antitumor effects. Further investigations are warranted to understand mechanisms and optimal conditions to achieve clinically translatable systemic antitumor effects.

摘要

我们证明,通过局部用光激活的紫杉醇(PTX)前药治疗,可以控制大原发性和未经治疗的小远处乳腺癌。我们假设,受治疗的肿瘤将受到光动力疗法(PDT)和局部释放的 PTX 的联合作用的破坏,而远处的肿瘤将受到全身抗肿瘤作用的抑制。通过皮下注射 MAT B III 细胞,在 Fischer 344 大鼠上建立了同源大鼠乳腺癌模型(单肿瘤和双肿瘤模型)。大鼠静脉注射 PTX 前药(剂量:1 μmol/kg),并使用 690nm 激光进行照射治疗(75 或 140 mW/cm,30 分钟,圆柱形光扩散器,药物-光间隔[DLI]9 小时)。较大的肿瘤(16mm)被有效地消融(100%),无复发超过 90 天。所有治愈的大鼠在长达 12 个月的时间内都拒绝了再次挑战的肿瘤。在双肿瘤模型中,局部大肿瘤(16mm)的治疗也通过适应性免疫激活治愈了未经治疗的肿瘤(4-6mm)。这是我们首次证明局部用我们的 PTX 前药治疗可产生全身抗肿瘤作用。需要进一步研究以了解机制和最佳条件,以实现可转化为临床应用的全身抗肿瘤作用。

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