Micellar Formulation of Talazoparib and Buparlisib for Enhanced DNA Damage in Breast Cancer Chemoradiotherapy

体内 乳腺癌 放射增敏剂 放射治疗 癌症研究 放化疗 DNA损伤 癌症 肿瘤科 药理学 材料科学 医学 内科学 生物 DNA 生物技术 遗传学
作者
Allison N. DuRoss,Megan J. Neufeld,Madeleine R. Landry,Justin G. Rosch,Colin T. Eaton,Gaurav Sahay,Charles R. Thomas,Conroy Sun
出处
期刊:ACS Applied Materials & Interfaces [American Chemical Society]
卷期号:11 (13): 12342-12356 被引量:19
标识
DOI:10.1021/acsami.9b02408
摘要

Chemoradiation is an effective combined modality therapeutic approach that utilizes principles of spatial cooperation to combat the adaptability associated with cancer and to potentially expand the therapeutic window. Optimal therapeutic efficacy requires intelligent selection and refinement of radiosynergistic pharmaceutical agents, enhanced delivery methods, and temporal consideration. Here, a monodisperse sub-20 nm mixed poloxamer micelle (MPM) system was developed to deliver hydrophobic drugs intravenously, in tandem with ionizing radiation. This report demonstrates in vitro synergy and enhanced radiosensitivity when two molecularly targeted DNA repair inhibitors, talazoparib and buparlisib, are encapsulated and combined with radiation in a 4T1 murine breast cancer model. Evaluation of in vivo biodistribution and toxicity exhibited no reduction in particle accumulation upon radiation and a lack of both acute and chronic toxicities. In vivo efficacy studies suggested the promise of combining talazoparib, buparlisib, and radiation to enhance survival and control tumor growth. Tissue analysis suggests enhanced DNA damage leading to apoptosis, thus increasing efficacy. These findings highlight the challenges associated with utilizing clinically relevant inclusion criteria and treatment protocols because complete tumor regression and extended survival were masked by an aggressively metastasizing model. As with clinical treatment regimens, the findings here establish a need for further optimization of this multimodal platform.
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