Low-dose X-ray radiotherapy–radiodynamic therapy via nanoscale metal–organic frameworks enhances checkpoint blockade immunotherapy

被引:0
|
作者
Kuangda Lu
Chunbai He
Nining Guo
Christina Chan
Kaiyuan Ni
Guangxu Lan
Haidong Tang
Charles Pelizzari
Yang-Xin Fu
Michael T. Spiotto
Ralph R. Weichselbaum
Wenbin Lin
机构
[1] The University of Chicago,Department of Chemistry
[2] The University of Chicago,The Ludwig Center for Metastasis Research
[3] The University of Chicago,Department of Radiation and Cellular Oncology
[4] University of Texas Southwestern Medical Center,Department of Pathology
来源
Nature Biomedical Engineering | 2018年 / 2卷
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摘要
Checkpoint blockade immunotherapy relies on energized cytotoxic T cells attacking tumour tissue systemically. However, for many cancers, the reliance on T cell infiltration leads to low response rates. Conversely, radiotherapy has served as a powerful therapy for local tumours over the past 100 years, yet is rarely sufficient to cause systemic tumour rejection. Here, we describe a treatment strategy that combines nanoscale metal–organic framework (nMOF)-enabled radiotherapy–radiodynamic therapy with checkpoint blockade immunotherapy for both local and systemic tumour elimination. In mouse models of breast and colorectal cancer, intratumorally injected nMOFs treated with low doses of X-ray irradiation led to the eradication of local tumours and, when loaded with an inhibitor of the immune checkpoint molecule indoleamine 2,3-dioxygenase, the irradiated nMOFs led to consistent abscopal responses that rejected distal tumours. By combining the advantages of local radiotherapy and systemic tumour rejection via synergistic X-ray-induced in situ vaccination and indoleamine 2,3-dioxygenase inhibition, nMOFs may overcome some of the limitations of checkpoint blockade in cancer treatment.
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页码:600 / 610
页数:10
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