超声敏感纳米颗粒联合聚焦超声在胰腺癌移植瘤模型中的抑瘤作用。
Tumor suppression effect of ultrasound-sensitive nanoparticles with focused ultrasound in a pancreas cancer xenograft model.
机构信息
Department of Radiology, Seoul National University Hospital, Seoul, Republic of Korea.
Department of Radiology, Seoul National University College of Medicine, 103 Daehak-Ro, Jongno-Gu, Seoul, Republic of Korea, 03080.
出版信息
Eur Radiol Exp. 2024 Mar 20;8(1):39. doi: 10.1186/s41747-024-00436-2.
BACKGROUND
We investigated the tumor suppression effect of an ultrasound-sensitive doxorubicin-loaded liposome-based nanoparticle, IMP301, to enhance the synergistic effect with focused ultrasound (FUS) in an animal model of pancreatic cancer.
METHODS
Thirty nude mice with xenografts of PANC-1 human pancreatic cancer cells were randomly and prospectively allocated to 6 different groups (5 per group) each for Study-1 (dose-response test) and Study-2 (synergistic effect test). Study-1 consisted of control, gemcitabine, Doxil with FUS, and three different doses of IMP301 (2, 4, 6 mg/kg) with FUS groups. Study-2 consisted of control, FUS only, gemcitabine, Doxil with FUS, and IMP301 (4 mg/kg) with or without FUS groups. Differences in tumor volume and growth rate were evaluated by one-way ANOVA and Student-Newman-Keuls test.
RESULTS
In Study-1, 4 mg/kg or greater IMP301 with FUS groups showed lower tumor growth rates of 14 ± 4 mm/day (mean ± standard deviation) or less, compared to the control, gemcitabine, and Doxil with FUS groups with rates exceeding 28 ± 5 (p < 0.050). The addition of FUS in Study-2 decreased the tumor growth rate in the IMP301-treated groups from 36 ± 17 to 9 ± 6, which was lower than the control, FUS only, gemcitabine, and Doxil with FUS groups (p < 0.050).
CONCLUSIONS
IMP301 combined with FUS exhibited higher tumor growth suppression compared to the use of a conventional drug alone or the combination with FUS. The present study showed the potential of IMP301 to enhance the synergistic effect with FUS for the treatment of pancreatic cancer.
RELEVANCE STATEMENT
This article aims to evaluate the synergistic effect of FUS and ultrasound-responsive liposomal drug in tumor growth suppression by using xenograft mouse model of pancreatic ductal adenocarcinoma. FUS-induced ultrasound-sensitive drug release may be a potential noninvasive repeatable treatment option for patients with locally advanced or unresectable pancreatic cancer.
KEY POINTS
• Modification of conventional drugs combined with FUS would maximize tumor suppression. • IMP301 with FUS had higher tumor suppression effect compared to conventional chemotherapy. • This image-guided drug delivery would enhance therapeutic effects of systemic chemotherapy.
背景
我们研究了一种超声敏感的载多柔比星脂质体纳米颗粒 IMP301 的肿瘤抑制作用,以增强其在胰腺癌动物模型中与聚焦超声(FUS)的协同作用。
方法
将 30 只荷人胰腺癌细胞 PANC-1 移植瘤的裸鼠随机、前瞻性地分为 6 组(每组 5 只),分别进行研究-1(剂量反应试验)和研究-2(协同作用试验)。研究-1 包括对照组、吉西他滨、载多柔比星的 Doxil 与 FUS 以及 FUS 组的三种不同剂量的 IMP301(2、4、6mg/kg)。研究-2 包括对照组、仅 FUS、吉西他滨、载多柔比星的 Doxil 与 FUS 以及有无 FUS 的 IMP301(4mg/kg)组。通过单向方差分析和 Student-Newman-Keuls 检验评估肿瘤体积和生长率的差异。
结果
在研究-1 中,与对照组、吉西他滨组和载多柔比星的 Doxil 与 FUS 组相比,FUS 组的 IMP301 剂量为 4mg/kg 或更高时,肿瘤生长率更低,为 14±4mm/天(均值±标准差)或更低(p<0.050)。在研究-2 中加入 FUS 后,IMP301 治疗组的肿瘤生长率从 36±17 降低至 9±6,低于对照组、仅 FUS、吉西他滨和载多柔比星的 Doxil 与 FUS 组(p<0.050)。
结论
与单独使用常规药物或联合 FUS 相比,IMP301 联合 FUS 表现出更高的肿瘤生长抑制作用。本研究表明,IMP301 有潜力增强 FUS 的协同作用,用于治疗胰腺癌。
重要性陈述
本文旨在通过使用胰腺导管腺癌的异种移植鼠模型来评估 FUS 和超声响应性脂质体药物联合在肿瘤生长抑制方面的协同作用。FUS 诱导的超声敏感药物释放可能是一种有前途的非侵入性、可重复的治疗选择,适用于局部晚期或不可切除的胰腺癌患者。
关键点
对常规药物进行修饰并联合 FUS 将最大限度地提高肿瘤抑制作用。
IMP301 联合 FUS 比常规化疗具有更高的肿瘤抑制效果。
这种图像引导的药物输送将增强全身化疗的治疗效果。
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