Intracellular drug release nanosystems

被引:212
作者
Meng, Fenghua
Cheng, Ru
Deng, Chao
Zhong, Zhiyuan [1 ]
机构
[1] Soochow Univ, Biomed Polymers Lab, Dept Polymer Sci & Engn, Coll Chem Chem Engn & Mat Sci, Suzhou 215123, Peoples R China
来源
MATERIALS TODAY | 2012年 / 15卷 / 10期
基金
中国国家自然科学基金;
关键词
NONVIRAL GENE TRANSFECTION; CROSS-LINKED MICELLES; CANCER-THERAPY; PROTEIN DELIVERY; BLOCK-COPOLYMER; RESPONSIVE NANOPARTICLES; BIODEGRADABLE MICELLES; TRIGGERED RELEASE; DIBLOCK COPOLYMER; LYSOSOMAL-ENZYMES;
D O I
10.1016/S1369-7021(12)70195-5
中图分类号
T [工业技术];
学科分类号
08 ;
摘要
In order to elicit therapeutic effects, many drugs including small molecule anticancer drugs, proteins, siRNA, and DNA have to be delivered and released into the specific cellular compartments typically the cytoplasm or nucleus of target cells. Intracellular environment-responsive nanosystems that exhibit good extracellular stability while rapidly releasing drugs inside cancer cells have been actively pursued for effective cancer therapy. Here, we highlight novel designs of smart nanosystems that release drugs in response to an intracellular biological signal of cancer cells such as acidic pH in endo/lysosomal compartments, enzymes in lysosomes, and redox potential in cytoplasm and the cell nucleus.
引用
收藏
页码:436 / 442
页数:7
相关论文
共 86 条
  • [1] Drug delivery systems: Entering the mainstream
    Allen, TM
    Cullis, PR
    [J]. SCIENCE, 2004, 303 (5665) : 1818 - 1822
  • [2] Enzyme-triggered nanomedicine: Drug release strategies in cancer therapy (Invited Review)
    Andresen, Thomas L.
    Thompson, David H.
    Kaasgaard, Thomas
    [J]. MOLECULAR MEMBRANE BIOLOGY, 2010, 27 (07) : 353 - 363
  • [3] Enzymatic reduction of disulfide bonds in lysosomes: Characterization of a Gamma-interferon-inducible lysosomal thiol reductase (GILT)
    Arunachalam, B
    Phan, UT
    Geuze, HJ
    Cresswell, P
    [J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2000, 97 (02) : 745 - 750
  • [4] Acetal-derivatized dextran:: An acid-responsive biodegradable material for therapeutic applications
    Bachelder, Eric M.
    Beaudette, Tristan T.
    Broaders, Kyle E.
    Dashe, Jesse
    Frechet, Jean M. J.
    [J]. JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 2008, 130 (32) : 10494 - +
  • [5] Glutathione-mediated shedding of PEG layers based on disulfide-linked catiomers for DNA delivery
    Cai, Xiao-Jun
    Dong, Hai-Qing
    Xia, Wen-Juan
    Wen, Hui-Yun
    Li, Xue-Quan
    Yu, Jin-Hai
    Li, Yong-Yong
    Shi, Dong-Lu
    [J]. JOURNAL OF MATERIALS CHEMISTRY, 2011, 21 (38) : 14639 - 14645
  • [6] PEG-SS-PPS: Reduction-sensitive disulfide block copolymer vesicles for intracellular drug delivery
    Cerritelli, Simona
    Velluto, Diana
    Hubbell, Jeffrey A.
    [J]. BIOMACROMOLECULES, 2007, 8 (06) : 1966 - 1972
  • [7] pH-Sensitive degradable polymersomes for triggered release of anticancer drugs: A comparative study with micelles
    Chen, Wei
    Meng, Fenghua
    Cheng, Ru
    Zhong, Zhiyuan
    [J]. JOURNAL OF CONTROLLED RELEASE, 2010, 142 (01) : 40 - 46
  • [8] Versatile Synthesis of Functional Biodegradable Polymers by Combining Ring-Opening Polymerization and Postpolymerization Modification via Michael-Type Addition Reaction
    Chen, Wei
    Yang, Huicui
    Wang, Rong
    Cheng, Ru
    Meng, Fenghua
    Wei, Wenxiang
    Zhong, Zhiyuan
    [J]. MACROMOLECULES, 2010, 43 (01) : 201 - 207
  • [9] pH-Responsive Biodegradable Micelles Based on Acid-Labile Polycarbonate Hydrophobe: Synthesis and Triggered Drug Release
    Chen, Wei
    Meng, Fenghua
    Li, Feng
    Ji, Shun-Jun
    Zhong, Zhiyuan
    [J]. BIOMACROMOLECULES, 2009, 10 (07) : 1727 - 1735
  • [10] Reduction and temperature dual-responsive crosslinked polymersomes for targeted intracellular protein delivery
    Cheng, Ru
    Meng, Fenghua
    Ma, Shoubao
    Xu, Haifei
    Liu, Haiyan
    Jing, Xiabin
    Zhong, Zhiyuan
    [J]. JOURNAL OF MATERIALS CHEMISTRY, 2011, 21 (47) : 19013 - 19020
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