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Bioorthogonal Pretargeting Strategy for Anchoring Activatable Photosensitizers on Plasma Membranes for Effective Photodynamic Therapy.

Abstract
Developing novel activatable photosensitizers with excellent plasma membrane targeting ability is urgently needed for smart photodynamic therapy (PDT). Herein, a tumor acidity-activatable photosensitizer combined with a two-step bioorthogonal pretargeting strategy to anchor photosensitizers on the plasma membrane for effective PDT is developed. Briefly, artificial receptors are first anchored on the cell plasma membrane using cell-labeling agents (Az-NPs) via the enhanced permeability and retention effect to achieve the tumor cell labeling. Then, pH-sensitive nanoparticles (S-NPs) modified with dibenzocyclooctyne (DBCO) and chlorin e6 (Ce6) accumulate in tumor tissue and disassemble upon protonation of their tertiary amines in response to the acidic tumor environment, exposing the contained DBCO and Ce6. The selective, highly specific click reactions between DBCO and azide groups enable Ce6 to be anchored on the tumor cell surface. Upon laser irradiation, the cell membrane is severely damaged by the cytotoxic reactive oxygen species, resulting in remarkable cellular apoptosis. Taken together, the membrane-localized PDT by our bioorthogonal pretargeting strategy to anchor activatable photosensitizers on the plasma membrane provides a simple but effective method for enhancing the therapeutic efficacy of photosensitizers in anticancer therapy.
AuthorsRuili Wei, Yansong Dong, Yalan Tu, Shiwei Luo, Xinrui Pang, Wanli Zhang, Wang Yao, Wenjie Tang, Huikang Yang, Xinhua Wei, Xinqing Jiang, Youyong Yuan, Ruimeng Yang
JournalACS applied materials & interfaces (ACS Appl Mater Interfaces) Vol. 13 Issue 12 Pg. 14004-14014 (Mar 31 2021) ISSN: 1944-8252 [Electronic] United States
PMID33728894 (Publication Type: Journal Article)
Chemical References
  • Chlorophyllides
  • Cyclooctanes
  • Photosensitizing Agents
  • Porphyrins
  • Receptors, Artificial
  • phytochlorin
Topics
  • Animals
  • Cell Line, Tumor
  • Cell Membrane (metabolism)
  • Chlorophyllides
  • Cyclooctanes (administration & dosage, pharmacokinetics, therapeutic use)
  • Drug Delivery Systems
  • Humans
  • Mice
  • Nanoparticles (administration & dosage, therapeutic use)
  • Neoplasms (drug therapy, metabolism)
  • Photochemotherapy
  • Photosensitizing Agents (administration & dosage, pharmacokinetics, therapeutic use)
  • Porphyrins (administration & dosage, pharmacokinetics, therapeutic use)
  • Receptors, Artificial (metabolism)

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