依沃福酰胺经动脉给予的低氧激活疗法在肝癌中的临床前获益

Preclinical Benefit of Hypoxia-Activated Intra-arterial Therapy with Evofosfamide in Liver Cancer.

作者信息

Duran Rafael, Mirpour Sahar, Pekurovsky Vasily, Ganapathy-Kanniappan Shanmugasundaram, Brayton Cory F, Cornish Toby C, Gorodetski Boris, Reyes Juvenal, Chapiro Julius, Schernthaner Rüdiger E, Frangakis Constantine, Lin MingDe, Sun Jessica D, Hart Charles P, Geschwind Jean-François

机构信息

Russell H. Morgan Department of Radiology and Radiological Science, Division of Vascular and Interventional Radiology, The Johns Hopkins Hospital, Baltimore, Maryland.

Department of Radiology and Biomedical Imaging, Yale University School of Medicine, New Haven, Connecticut.

出版信息

Clin Cancer Res. 2017 Jan 15;23(2):536-548. doi: 10.1158/1078-0432.CCR-16-0725. Epub 2016 Jul 20.

DOI:10.1158/1078-0432.CCR-16-0725

PMID:27440271

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5241187/

Abstract

PURPOSE

To evaluate safety and characterize anticancer efficacy of hepatic hypoxia-activated intra-arterial therapy (HAIAT) with evofosfamide in a rabbit model.

EXPERIMENTAL DESIGN

VX2-tumor-bearing rabbits were assigned to 4 intra-arterial therapy (IAT) groups (n = 7/group): (i) saline (control); (ii) evofosfamide (Evo); (iii) doxorubicin-lipiodol emulsion followed by embolization with 100-300 μm beads (conventional, cTACE); or (iv) cTACE and evofosfamide (cTACE + Evo). Blood samples were collected pre-IAT and 1, 2, 7, and 14 days post-IAT. A semiquantitative scoring system assessed hepatocellular damage. Tumor volumes were segmented on multidetector CT (baseline, 7/14 days post-IAT). Pathologic tumor necrosis was quantified using manual segmentation on whole-slide images. Hypoxic fraction (HF) and compartment (HC) were determined by pimonidazole staining. Tumor DNA damage, apoptosis, cell proliferation, endogenous hypoxia, and metabolism were quantified (γ-H2AX, Annexin V, caspase-3, Ki-67, HIF1α, VEGF, GAPDH, MCT4, and LDH).

RESULTS

cTACE + Evo showed a similar profile of liver enzymes elevation and pathologic scores compared with cTACE. Neither hematologic nor renal toxicity were observed. Animals treated with cTACE + Evo demonstrated smaller tumor volumes, lower tumor growth rates, and higher necrotic fractions compared with cTACE. cTACE + Evo resulted in a marked reduction in the HF and HC. Correlation was observed between decreases in HF or HC and tumor necrosis. cTACE + Evo promoted antitumor effects as evidenced by increased expression of γ-H2AX, apoptotic biomarkers, and decreased cell proliferation. Increased HIF1α/VEGF expression and tumor glycolysis supported HAIAT.

CONCLUSIONS

HAIAT achieved a promising step towards the locoregional targeting of tumor hypoxia. The favorable toxicity profile and enhanced anticancer effects of evofosfamide in combination with cTACE pave the way towards clinical trials in patients with liver cancer. Clin Cancer Res; 23(2); 536-48. ©2016 AACR.

摘要

目的

在兔模型中评估依沃福司他进行肝缺氧激活动脉内治疗（HAIAT）的安全性并表征其抗癌疗效。

实验设计

将荷VX2肿瘤的兔分为4个动脉内治疗（IAT）组（每组n = 7）：（i）生理盐水（对照组）；（ii）依沃福司他（Evo）；（iii）阿霉素-碘油乳剂，随后用100 - 300μm微球栓塞（传统经动脉化疗栓塞，cTACE）；或（iv）cTACE联合依沃福司他（cTACE + Evo）。在IAT前以及IAT后1、2、7和14天采集血样。采用半定量评分系统评估肝细胞损伤。在多排CT上对肿瘤体积进行分割（基线，IAT后7/14天）。使用全玻片图像上的手动分割对病理性肿瘤坏死进行定量。通过匹莫硝唑染色确定缺氧分数（HF）和缺氧区室（HC）。对肿瘤DNA损伤、凋亡、细胞增殖、内源性缺氧和代谢进行定量分析（γ-H2AX、膜联蛋白V、半胱天冬酶-3、Ki-67、HIF1α、VEGF、GAPDH、MCT4和LDH）。

结果

与cTACE相比，cTACE + Evo显示出相似的肝酶升高情况和病理评分。未观察到血液学或肾毒性。与cTACE相比，接受cTACE + Evo治疗的动物肿瘤体积更小、肿瘤生长速率更低且坏死分数更高。cTACE + Evo导致HF和HC显著降低。观察到HF或HC降低与肿瘤坏死之间存在相关性。cTACE + Evo促进了抗肿瘤作用，表现为γ-H2AX表达增加、凋亡生物标志物增加以及细胞增殖减少。HIF1α/VEGF表达增加和肿瘤糖酵解支持了HAIAT。

结论

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/be20/5241187/a7f29b0d7446/nihms-805214-f0001.jpg

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依沃福酰胺经动脉给予的低氧激活疗法在肝癌中的临床前获益

Preclinical Benefit of Hypoxia-Activated Intra-arterial Therapy with Evofosfamide in Liver Cancer.

作者信息

机构信息

出版信息

PURPOSE

EXPERIMENTAL DESIGN

RESULTS

CONCLUSIONS

目的

实验设计

结果

结论

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