MR Molecular Image Guided Treatment of Pancreatic Cancer with Targeted ECO/miR-200c Nanoparticles in Immunocompetent Mouse Tumor Models.

IF 3.5 3区 医学 Q2 CHEMISTRY, MULTIDISCIPLINARY
Pharmaceutical Research Pub Date : 2024-09-01 Epub Date: 2024-08-28 DOI:10.1007/s11095-024-03762-7
Victoria Laney, Ryan Hall, Xueer Yuan, Emma Hampson, Augusta Halle, Grace Yeung, Kristen-Weber Bonk, Suneel Apte, Jordan Winter, Ruth Keri, Zheng-Rong Lu
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引用次数: 0

Abstract

Objective: Pancreatic ductal adenocarcinoma (PDAC) is characterized by desmoplasia due to increased deposition of extracellular matrix (ECM) proteins. This work investigates the efficacy of targeted ECO/miR-200c nanoparticles (ELNP) on ECM remodeling in PDAC and tumor proliferation with MR molecular imaging (MRMI) with MT218 in immunocompetent mouse models.

Methods: The miR-200c mediated regulation of EMT markers was measured in PDAC cells in vitro. Wild-type mice bearing mutated KRAS-driven KPC subcutaneous or orthotopic tumors were dosed weekly with RGD-ELNP/miR-200c at 1 mg-RNA/kg for a total of 4 doses. We utilized MT218-MRMI to non-invasively monitor the alteration of tumor ECM EDN-FN levels by miR-200c and tumor response to the treatment. The changes were also validated by posthumous histopathology.

Results: Transfection of PDAC cells with ELNP/miR-200c downregulated the expression of FN1 and EDB-FN and some mesenchymal markers, inhibiting 3D spheroid formation and migration of KPC PDAC cells. RGD-ELNP/miR-200c treatment resulted in significant signal reduction in the MT218 enhanced MRMI images of both subcutaneous and orthotopic KPC tumors compared to those prior to treatment and treated with a non-specific control. MT218-MRMI results were suggestive of EDB-FN downregulation in tumors, which was later confirmed by immunohistochemistry. Tumor growth in subcutaneous tumors was significantly attenuated with RGD-ELNP/miR-200c and was an observed trend in orthotopic tumors. Substantial necrosis and remodeling were observed in both models treated with RGD-ELNP/miR-200c based on H&E staining.

Conclusion: These results demonstrate the feasibility of RGD-ELNP/miR-200c in modulating PDAC ECM and restraining tumor growth and the utility of MT218-MRMI for non-invasively monitoring miR-200c efficacy.

Abstract Image

在免疫功能健全的小鼠肿瘤模型中用靶向 ECO/miR-200c 纳米粒子在磁共振分子影像引导下治疗胰腺癌
目的:胰腺导管腺癌(PDAC)的特点是由于细胞外基质(ECM)蛋白沉积增加而导致脱钙化。这项工作研究了靶向 ECO/miR-200c 纳米粒子(ELNP)对 PDAC 中 ECM 重塑的疗效,以及在免疫功能正常的小鼠模型中使用 MT218 进行磁共振分子成像(MRMI)对肿瘤增殖的影响:方法:在体外检测 PDAC 细胞中 miR-200c 介导的 EMT 标记调控。对携带突变 KRAS 驱动的 KPC 皮下或原位肿瘤的野生型小鼠每周注射 1 mg-RNA/kg 的 RGD-ELNP/miR-200c,共注射 4 次。我们利用 MT218-MRMI 非侵入性监测 miR-200c 对肿瘤 ECM EDN-FN 水平的改变以及肿瘤对治疗的反应。这些变化也得到了死后组织病理学的验证:结果:用ELNP/miR-200c转染PDAC细胞可降低FN1和EDB-FN以及一些间质标记物的表达,抑制KPC PDAC细胞的三维球形形成和迁移。与治疗前和使用非特异性对照组相比,RGD-ELNP/miR-200c 治疗导致皮下和正位 KPC 肿瘤的 MT218 增强 MRMI 图像信号显著降低。MT218-MRMI结果表明肿瘤中的EDB-FN出现了下调,随后免疫组化证实了这一点。RGD-ELNP/miR-200c能显著抑制皮下肿瘤的生长,而且在正位肿瘤中也能观察到这一趋势。根据 H&E 染色结果,在使用 RGD-ELNP/miR-200c 治疗的两种模型中均观察到大量坏死和重塑:这些结果证明了 RGD-ELNP/miR-200c 在调节 PDAC ECM 和抑制肿瘤生长方面的可行性,以及 MT218-MRMI 在无创监测 miR-200c 疗效方面的实用性。
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来源期刊
Pharmaceutical Research
Pharmaceutical Research 医学-化学综合
CiteScore
6.60
自引率
5.40%
发文量
276
审稿时长
3.4 months
期刊介绍: Pharmaceutical Research, an official journal of the American Association of Pharmaceutical Scientists, is committed to publishing novel research that is mechanism-based, hypothesis-driven and addresses significant issues in drug discovery, development and regulation. Current areas of interest include, but are not limited to: -(pre)formulation engineering and processing- computational biopharmaceutics- drug delivery and targeting- molecular biopharmaceutics and drug disposition (including cellular and molecular pharmacology)- pharmacokinetics, pharmacodynamics and pharmacogenetics. Research may involve nonclinical and clinical studies, and utilize both in vitro and in vivo approaches. Studies on small drug molecules, pharmaceutical solid materials (including biomaterials, polymers and nanoparticles) biotechnology products (including genes, peptides, proteins and vaccines), and genetically engineered cells are welcome.
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