Active targeting of chemotherapy to disseminated tumors using nanoparticle-carrying T cells

癌症研究 体内 体内分布 离体 淋巴瘤 医学 归巢(生物学) 药理学 化学 药物输送 免疫学 生物 生态学 生物技术 有机化学
作者
Bruce Huang,Wuhbet Abraham,Yiran Zheng,Sandra C. Bustamante López,Samantha S. Luo,Darrell J. Irvine
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science (AAAS)]
卷期号:7 (291) 被引量:238
标识
DOI:10.1126/scitranslmed.aaa5447
摘要

Tumor cells disseminate into compartments that are poorly accessible from circulation, which necessitates high doses of systemic chemotherapy. However, the effectiveness of many drugs, such as the potent topoisomerase I poison SN-38, is hampered by poor pharmacokinetics. To deliver SN-38 to lymphoma tumors in vivo, we took advantage of the fact that healthy lymphocytes can be programmed to phenocopy the biodistribution of the tumor cells. In a murine model of disseminated lymphoma, we expanded autologous polyclonal T cells ex vivo under conditions that retained homing receptors mirroring lymphoma cells, and functionalized these T cells to carry SN-38-loaded nanocapsules on their surfaces. Nanocapsule-functionalized T cells were resistant to SN-38 but mediated efficient killing of lymphoma cells in vitro. Upon adoptive transfer into tumor-bearing mice, these T cells served as active vectors to deliver the chemotherapeutic into tumor-bearing lymphoid organs. Cell-mediated delivery concentrated SN-38 in lymph nodes at levels 90-fold greater than free drug systemically administered at 10-fold higher doses. The live T cell delivery approach reduced tumor burden significantly after 2 weeks of treatment and enhanced survival under conditions where free SN-38 and SN-38-loaded nanocapsules alone were ineffective. These results suggest that tissue-homing lymphocytes can serve as specific targeting agents to deliver nanoparticles into sites difficult to access from the circulation, and thus improve the therapeutic index of chemotherapeutic drugs with unfavorable pharmacokinetics.
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