| Literature DB >> 31074257 |
Gyu Seong Heo1, Yongfeng Zhao2, Deborah Sultan1, Xiaohui Zhang1, Lisa Detering1, Hannah P Luehmann1, Xiangyu Zhang3, Richen Li1, Ankur Choksi4, Savannah Sharp5, Sidney Levingston1, Tina Primeau3, David E Reichert1, Guorong Sun1, Babak Razani3, Shunqiang Li3, Katherine N Weilbaecher3, Farrokh Dehdashti1, Karen L Wooley6, Yongjian Liu1.
Abstract
Nanoparticles have been widely used for preclinical cancer imaging. However, their successful clinical translation is largely hampered by potential toxicity, unsatisfactory detection of malignancy at early stages, inaccurate diagnosis of tumor biomarkers, and histology for imaging-guided treatment. Herein, a targeted copper nanocluster (CuNC) is reported with high potential to address these challenges for future translation. Its ultrasmall structure enables efficient renal/bowel clearance, minimized off-target effects in nontargeted organs, and low nonspecific tumor retention. The pH-dependent in vivo dissolution of CuNCs affords minimal toxicity and potentially selective drug delivery to tumors. The intrinsic radiolabeling through the direct addition of 64Cu to CuNC (64Cu-CuNCs-FC131) synthesis offers high specific activity for sensitive and accurate detection of CXCR4 via FC131-directed targeting in novel triple negative breast cancer (TNBC) patient-derived xenograft mouse models and human TNBC tissues. In summary, this study not only reveals the potential of CXCR4-targeted 64Cu-CuNCs for TNBC imaging in clinical settings, but also provides a useful strategy to design and assess the translational potential of nanoparticles for cancer theranostics.Entities:
Keywords: CXCR4; breast cancer; copper nanocluster; positron emission tomography; translation
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Year: 2019 PMID: 31074257 DOI: 10.1021/acsami.8b22752
Source DB: PubMed Journal: ACS Appl Mater Interfaces ISSN: 1944-8244 Impact factor: 9.229