<i>In Vivo</i> Albumin Traps Photosensitizer Monomers from Self-Assembled Phthalocyanine Nanovesicles: A Facile and Switchable Theranostic Approach

Xingshu Li(Ewha Womans University), Sungsook Yu(Yonsei University), Yoonji Lee(Ewha Womans University), Tianyang Guo(Ewha Womans University), Nahyun Kwon(Ewha Womans University), Dayoung Lee(Ewha Womans University), Su Cheong Yeom(Seoul National University), Yejin Cho(Yonsei University), Gyoungmi Kim(Ewha Womans University), Jian‐Dong Huang(Fuzhou University), Sun Choi(Ewha Womans University), Ki Taek Nam(Yonsei University), Juyoung Yoon(Ewha Womans University)
Journal of the American Chemical Society
December 19, 2018
Cited by 222Open Access
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Abstract

Albumin is a promising candidate as a biomarker for potential disease diagnostics and has been extensively used as a drug delivery carrier for decades. In these two directions, many albumin-detecting probes and exogenous albumin-based nanocomposite delivery systems have been developed. However, there are only a few cases demonstrating the specific interactions of exogenous probes with albumin in vivo, and nanocomposite delivery systems usually suffer from tedious fabrication processes and potential toxicity of the complexes. Herein, we demonstrate a facile "one-for-all" switchable nanotheranostic (NanoPcS) for both albumin detection and cancer treatment. In particular, the in vivo specific binding between albumin and PcS, arising from the disassembly of injected NanoPcS, is confirmed using an inducible transgenic mouse system. Fluorescence imaging and antitumor tests on different tumor models suggest that NanoPcS has superior tumor-targeting ability and the potential for time-modulated, activatable photodynamic therapy.


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