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Biodegradable nanocomplex from hyaluronic acid and arginine based poly(ester amide)s as the delivery vehicles for improved photodynamic therapy of multidrug resistant tumor cells: An in vitro study of the performance of chlorin e6 photosensitizer
Author(s) -
Ji Ying,
Zhao Jihui,
Chu ChihChang
Publication year - 2017
Publication title -
journal of biomedical materials research part a
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.849
H-Index - 150
eISSN - 1552-4965
pISSN - 1549-3296
DOI - 10.1002/jbm.a.35982
Subject(s) - photodynamic therapy , hyaluronic acid , biophysics , nanocarriers , in vitro , singlet oxygen , endocytosis , materials science , cd44 , cytotoxicity , multiple drug resistance , tumor microenvironment , intracellular , doxorubicin , biochemistry , cancer research , drug delivery , chemistry , cell , nanotechnology , tumor cells , biology , oxygen , organic chemistry , genetics , antibiotics , chemotherapy
Photodynamic therapy (PDT), which enables the localized therapeutic effect by light irradiation, provides an alternative and complementary modality for the treatment of tumor. However, the aggregation of photosensitizers in acidic microenvironment of tumor and the non‐targeted distribution of photosensitizers in normal tissues significantly affect the PDT efficiency. In this study, we developed a biodegradable nanocomplex HA‐Arg‐PEA from hyaluronic acid (HA) and arginine based poly(ester amide)s (Arg‐PEA) as the nanocarrier for chlorin e6 (Ce6). HA enhanced the tumor‐specific endocytosis mediated by the overexpression of CD44 receptor. Arg‐PEA not only provide electrostatic interaction with HA to form self‐assembled nanostructure, but also improve the monomerization of Ce6 at physiological pH as well as mildly acidic pH. The biodegradable characteristic of HA‐Arg‐PEA nanocomplex enabled the intracellular delivery of Ce6, in which its release and generation of singlet oxygen can be accelerated by enzymatic degradation of the carrier. The in vitro PDT efficiency of Ce6‐loaded HA‐Arg‐PEA nanocomplex was examined in CD44 positive MDA‐MB‐435/MDR multidrug resistant melanoma cells. CD44‐mediated uptake of Ce6‐loaded HA‐Arg‐PEA nanocomplex significantly improved Ce6 level in MDA‐MB‐435/MDR cells within short incubation time, and the PDT efficiency in inhibiting multidrug resistant tumor cells was also enhanced at higher Ce6 concentrations. © 2017 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 105A: 1487–1499, 2017.