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A preclinical model for predicting drug response in soft-tissue sarcoma with targeted AAVP molecular imaging

机译:靶向AAVP分子成像预测软组织肉瘤药物反应的临床前模型

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摘要

Human sarcomas are rare but diverse malignant tumors derived from mesenchymal tissue. Clinical response to therapy is currently determined by the modified World Health Organization (WHO) criteria or the Response Evaluation Criteria in Solid Tumors (RECIST), but these standards correlate poorly with sarcoma patient outcome. We introduced ligand-directed particles with elements of AAV and phage (AAVP) to enable integration of tumor targeting to molecular imaging. We report drug-response monitoring and prediction in a nude rat model of human sarcoma by AAVP imaging. As a proof-of-concept, we imaged Herpes simplex thymidine kinase in a clinic-ready setting with PET to show that one can a priori predict tumor response to a systemic cytotoxic. Given the target expression in patient-derived sarcomas, this platform may be translated in clinical applications. Sarcoma-specific ligands and promoters may ultimately lead to an imaging transcriptome.
机译:人肉瘤是罕见的,但起源于间质组织的多种恶性肿瘤。目前对治疗的临床反应是由修改后的世界卫生组织(WHO)标准或实体瘤反应评估标准(RECIST)确定的,但这些标准与肉瘤患者预后的相关性很差。我们引入了具有AAV和噬菌体(AAVP)元素的配体导向颗粒,以使肿瘤靶向整合到分子成像中。我们通过AAVP成像报告人类肉瘤的裸鼠模型中的药物反应监测和预测。作为概念验证,我们在临床准备就绪的环境中用PET对单纯疱疹胸苷激酶进行了成像,以显示可以先验地预测肿瘤对全身细胞毒性的反应。给定患者源性肉瘤中的靶表达,该平台可以在临床应用中翻译。肉瘤特异性配体和启动子可能最终导致成像转录组。

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