Lokerse Wouter J M, Bolkestein Michiel, Ten Hagen Timo L M, de Jong Marion, Eggermont Alexander M M, Grüll Holger, Koning Gerben A
1. Laboratory Experimental Surgical Oncology, Section Surgical Oncology, Department of Surgery, Erasmus MC, Rotterdam, The Netherlands.
2. Departments of Nuclear Medicine and Radiology, Erasmus MC, Rotterdam, the Netherlands.
Theranostics. 2016 Jun 24;6(10):1717-31. doi: 10.7150/thno.14960. eCollection 2016.
Doxorubicin (Dox) loaded thermosensitive liposomes (TSLs) have shown promising results for hyperthermia-induced local drug delivery to solid tumors. Typically, the tumor is heated to hyperthermic temperatures (41-42 °C), which induced intravascular drug release from TSLs within the tumor tissue leading to high local drug concentrations (1-step delivery protocol). Next to providing a trigger for drug release, hyperthermia (HT) has been shown to be cytotoxic to tumor tissue, to enhance chemosensitivity and to increase particle extravasation from the vasculature into the tumor interstitial space. The latter can be exploited for a 2-step delivery protocol, where HT is applied prior to i.v. TSL injection to enhance tumor uptake, and after 4 hours waiting time for a second time to induce drug release. In this study, we compare the 1- and 2-step delivery protocols and investigate which factors are of importance for a therapeutic response. In murine B16 melanoma and BFS-1 sarcoma cell lines, HT induced an enhanced Dox uptake in 2D and 3D models, resulting in enhanced chemosensitivity. In vivo, therapeutic efficacy studies were performed for both tumor models, showing a therapeutic response for only the 1-step delivery protocol. SPECT/CT imaging allowed quantification of the liposomal accumulation in both tumor models at physiological temperatures and after a HT treatment. A simple two compartment model was used to derive respective rates for liposomal uptake, washout and retention, showing that the B16 model has a twofold higher liposomal uptake compared to the BFS-1 tumor. HT increases uptake and retention of liposomes in both tumors models by the same factor of 1.66 maintaining the absolute differences between the two models. Histology showed that HT induced apoptosis, blood vessel integrity and interstitial structures are important factors for TSL accumulation in the investigated tumor types. However, modeling data indicated that the intraliposomal Dox fraction did not reach therapeutic relevant concentrations in the tumor tissue in a 2-step delivery protocol due to the leaking of the drug from its liposomal carrier providing an explanation for the observed lack of efficacy.
载有多柔比星(Dox)的热敏脂质体(TSLs)在热诱导局部药物递送至实体瘤方面已显示出有前景的结果。通常,将肿瘤加热至热疗温度(41 - 42°C),这会诱导肿瘤组织内TSLs的血管内药物释放,从而导致高局部药物浓度(一步给药方案)。除了为药物释放提供触发因素外,热疗(HT)已被证明对肿瘤组织具有细胞毒性,可增强化学敏感性,并增加颗粒从血管系统外渗到肿瘤间质空间。后者可用于两步给药方案,即在静脉注射TSL之前应用HT以增强肿瘤摄取,并在等待4小时后再次应用以诱导药物释放。在本研究中,我们比较了一步和两步给药方案,并研究哪些因素对治疗反应至关重要。在小鼠B16黑色素瘤和BFS - 1肉瘤细胞系中,HT在二维和三维模型中诱导了增强的多柔比星摄取,从而导致增强的化学敏感性。在体内,对两种肿瘤模型都进行了治疗效果研究,结果表明仅一步给药方案有治疗反应。SPECT/CT成像允许在生理温度和HT治疗后对两种肿瘤模型中的脂质体积累进行定量。使用一个简单的双室模型来推导脂质体摄取、洗脱和保留的各自速率,结果表明B16模型的脂质体摄取比BFS - 1肿瘤高两倍。HT使两种肿瘤模型中脂质体的摄取和保留增加相同的1.66倍,保持了两种模型之间的绝对差异。组织学显示,HT诱导的细胞凋亡、血管完整性和间质结构是所研究肿瘤类型中TSL积累的重要因素。然而,建模数据表明,在两步给药方案中,由于药物从其脂质体载体中泄漏,肿瘤组织中的脂质体内多柔比星部分未达到治疗相关浓度,这为观察到的疗效缺乏提供了解释。
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