Idarubicin-Loaded ONCOZENE Drug-Eluting Bead Chemoembolization in a Rabbit Liver Tumor Model: Investigating Safety, Therapeutic Efficacy, and Effects on Tumor Microenvironment

医学 离体 有效扩散系数 磁共振成像 核医学 去甲柔比星 病理 肝损伤 肝肿瘤 内科学 体内 肝细胞癌 放射科 化疗 生物 生物技术 完全缓解
作者
Tabea Borde,Fabian M. Laage Gaupp,Jean-François Geschwind,Lynn Jeanette Savic,Milena Miszczuk,Irvin Rexha,Lucas Christoph Adam,John J. Walsh,Steffen Huber,James S. Duncan,Dana C. Peters,Albert J. Sinusas,Todd Schlachter,Bernhard Gebauer,Fahmeed Hyder,Daniel Coman,Johanna M. M. van Breugel,Julius Chapiro
出处
期刊:Journal of Vascular and Interventional Radiology [Elsevier]
卷期号:31 (10): 1706-1716.e1 被引量:9
标识
DOI:10.1016/j.jvir.2020.04.010
摘要

Purpose To investigate toxicity, efficacy, and microenvironmental effects of idarubicin-loaded 40-μm and 100-μm drug-eluting embolic (DEE) transarterial chemoembolization in a rabbit liver tumor model. Materials and Methods Twelve male New Zealand White rabbits with orthotopically implanted VX2 liver tumors were assigned to DEE chemoembolization with 40-μm (n = 5) or 100-μm (n = 4) ONCOZENE microspheres or no treatment (control; n = 3). At 24–72 hours postprocedurally, multiparametric magnetic resonance (MR) imaging including dynamic contrast-enhanced (DCE), diffusion-weighted imaging (DWI), and biosensor imaging of redundant deviation in shifts (BIRDS) was performed to assess extracellular pH (pHe), followed by immediate euthanasia. Laboratory parameters and histopathologic ex vivo analysis included fluorescence confocal microscopy and immunohistochemistry. Results DCE MR imaging demonstrated a similar degree of devascularization of embolized tumors for both microsphere sizes (mean arterial enhancement, 8% ± 12 vs 36% ± 51 in controls; P = .07). Similarly, DWI showed postprocedural increases in diffusion across the entire lesion (apparent diffusion coefficient, 1.89 × 10−3 mm2/s ± 0.18 vs 2.34 × 10−3 mm2/s ± 0.18 in liver; P = .002). BIRDS demonstrated profound tumor acidosis at baseline (mean pHe, 6.79 ± 0.08 in tumor vs 7.13 ± 0.08 in liver; P = .02) and after chemoembolization (6.8 ± 0.06 in tumor vs 7.1 ± 0.04 in liver; P = .007). Laboratory and ex vivo analyses showed central tumor core penetration and greater increase in liver enzymes for 40-μm vs 100-μm microspheres. Inhibition of cell proliferation, intratumoral hypoxia, and limited idarubicin elution were equally observed with both sphere sizes. Conclusions Noninvasive multiparametric MR imaging visualized chemoembolic effects in tumor and tumor microenvironment following DEE chemoembolization. Devascularization, increased hypoxia, coagulative necrosis, tumor acidosis, and limited idarubicin elution suggest ischemia as the predominant therapeutic mechanism. Substantial size-dependent differences indicate greater toxicity with the smaller microsphere diameter.
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