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Multiarm Nanoconjugates for Cancer Cell-Targeted Delivery of Photosensitizers

  • Yan Zhao
    Yan Zhao
    Department of Cancer Biology and Comprehensive Cancer Center, Wake Forest University School of Medicine, Winston-Salem, North Carolina 27157, United States
    National Pharmaceutical Engineering Research Center, China State Institute of Pharmaceutical Industry, Shanghai 201203, China
    More by Yan Zhao
  • Fang Li
    Fang Li
    Department of Cancer Biology and Comprehensive Cancer Center, Wake Forest University School of Medicine, Winston-Salem, North Carolina 27157, United States
    School of Pharmacy, Jiangsu Vocational College of Medicine, Yancheng 224005, China
    More by Fang Li
  • Chengqiong Mao
    Chengqiong Mao
    Department of Cancer Biology and Comprehensive Cancer Center, Wake Forest University School of Medicine, Winston-Salem, North Carolina 27157, United States
  • , and 
  • Xin Ming*
    Xin Ming
    Department of Cancer Biology and Comprehensive Cancer Center, Wake Forest University School of Medicine, Winston-Salem, North Carolina 27157, United States
    *E-mail: [email protected]. Phone: 1-336-716-8440.
    More by Xin Ming
Cite this: Mol. Pharmaceutics 2018, 15, 7, 2559–2569
Publication Date (Web):May 16, 2018
https://doi.org/10.1021/acs.molpharmaceut.8b00088
Copyright © 2018 American Chemical Society
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Abstract

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Photodynamic therapy, a procedure that uses a photosensitizer to enable light therapy selectively at diseased sites, remains underutilized in oncological clinic. To further improve its cancer selectivity, we developed a polymeric nanosystem by conjugating a photosensitizer IRDye 700DX (IR700) and cancer targeting RGD peptide to 8-arm polyethylene glycol (PEG). The resulting nanoconjugates (RGD-8PEG-IR700) exhibited a hydrodynamic size of 6.6 nm with narrow distribution of size. The targeted nanoconjugates showed significantly higher intracellular uptake of IR700 in integrin αvβ3-expressing A375 and SKOV3 cells when compared with nontargeted control 8PEG-IR700, and an excess amount of RGD peptides could abolish this enhancement, indicating a receptor-mediated uptake mechanism for the targeted polymer conjugates. Phototoxicity studies indicated that RGD-8PEG-IR700 produced massive cell killing in A375 cells after photoirradiation with an IC50 value of 57.8 nM for IR700. In contrast, free IR700 and the control 8PEG-IR700 conjugates did not produce any phototoxicity at the concentrations up to 1 μM IR700. Upon photoirradiation, the RGD-8PEG-IR700 could produce sufficient singlet oxygen in the cells and induced cell apoptosis. The studies with three-dimensional tumor spheroids showed that they penetrated tumor spheroids deeply and produced strong phototoxicity. Thus, we conclude that the polymer nanoconjugates may provide a promising delivery system for targeted photodynamic therapy of cancers due to their small size, cancer cell specificity, and minimal side effects.

Cited By


This article is cited by 3 publications.

  1. Xubin Suo, Brittany N. Eldridge, Han Zhang, Chengqiong Mao, Yuanzeng Min, Yao Sun, Ravi Singh, Xin Ming. P-Glycoprotein-Targeted Photothermal Therapy of Drug-Resistant Cancer Cells Using Antibody-Conjugated Carbon Nanotubes. ACS Applied Materials & Interfaces 2018, 10 (39) , 33464-33473. https://doi.org/10.1021/acsami.8b11974
  2. Xiaobao Zhao, Jingxing Si, Dongsheng Huang, Ke Li, Ying Xin, Meihua Sui. Application of star poly(ethylene glycol) derivatives in drug delivery and controlled release. Journal of Controlled Release 2020, 323 , 565-577. https://doi.org/10.1016/j.jconrel.2020.04.039
  3. Chengqiong Mao, Yan Zhao, Fang Li, Zibo Li, Shaomin Tian, Waldemar Debinski, Xin Ming. P-glycoprotein targeted and near-infrared light-guided depletion of chemoresistant tumors. Journal of Controlled Release 2018, 286 , 289-300. https://doi.org/10.1016/j.jconrel.2018.08.005

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