Development of a rabbit human glioblastoma model for testing of endovascular selective intra-arterial infusion (ESIA) of novel stem cell-based therapeutics

医学 血管性 颈内动脉 间充质干细胞 免疫组织化学 病理 U87型 干细胞 磁共振成像 地塞米松 胶质母细胞瘤 泌尿科 核医学 放射科 癌症研究 生物 遗传学
作者
Peter Kan,Visish M. Srinivasan,Joy Gumin,Roberto Garcia,Stephen Chen,Jeremiah N. Johnson,Dalis E Collins,Melissa Chen,Daniel Ledbetter,Jason T. Huse,Zean Aaron Evan Luna,Ariadna Robledo,Viren Vasandani,A. Venketeshwer Rao,Sanjay K. Singh,Elizabeth J. Shpall,Juàn Fueyo,Candelaria Gómez-Manzano,Frederick F. Lang
出处
期刊:Neuro-oncology [Oxford University Press]
卷期号:26 (1): 127-136 被引量:3
标识
DOI:10.1093/neuonc/noad152
摘要

Abstract Background Endovascular selective intra-arterial (ESIA) infusion of cellular oncotherapeutics is a rapidly evolving strategy for treating glioblastoma. Evaluation of ESIA infusion requires a unique animal model. Our goal was to create a rabbit human GBM model to test IA infusions of cellular therapies and to test its usefulness by employing clinical-grade microcatheters and infusion methods to deliver mesenchymal stem cells loaded with an oncolytic adenovirus, Delta-24-RGD (MSC-D24). Methods Rabbits were immunosuppressed with mycophenolate mofetil, dexamethasone, and tacrolimus. They underwent stereotactic xenoimplantation of human GBM cell lines (U87, MDA-GSC-17, and MDA-GSC-8-11) into the right frontal lobe. Tumor formation was confirmed on magnetic resonance imaging, histologic, and immunohistochemistry analysis. Selective microcatheter infusion of MSC-D24 was performed via the ipsilateral internal carotid artery to assess model utility and the efficacy and safety of this approach. Results Twenty-five rabbits were implanted (18 with U87, 2 MDA-GSC-17, and 5 MDA-GSC-8-11). Tumors formed in 68% of rabbits (77.8% for U87, 50.0% for MDA-GSC-17, and 40.0% for MDA-GSC-8-11). On MRI, the tumors were hyperintense on T2-weighted image with variable enhancement (evidence of blood brain barrier breakdown). Histologically, tumors showed phenotypic traits of human GBM including varying levels of vascularity. ESIA infusion into the distal internal carotid artery of 2 ml of MSCs-D24 (107 cells) was safe in the model. Examination of post infusion specimens documented that MSCs-D24 homed to the implanted tumor at 24 hours. Conclusions The intracranial immunosuppressed rabbit human GBM model allows testing of ESIA infusion of novel therapeutics (eg, MSC-D24) in a clinically relevant fashion.
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