articleCancer ResearchJul 1, 2006BRONZE OA

Antibody Targeting of Long-Circulating Lipidic Nanoparticles Does Not Increase Tumor Localization but Does Increase Internalization in Animal Models

California Pacific Medical Center · University of California, San Francisco

PubMed
Indexed incrossrefpubmed

Abstract

We describe evidence for a novel mechanism of monoclonal antibody (MAb)-directed nanoparticle (immunoliposome) targeting to solid tumors in vivo. Long-circulating immunoliposomes targeted to HER2 (ErbB2, Neu) were prepared by the conjugation of anti-HER2 MAb fragments (Fab' or single chain Fv) to liposome-grafted polyethylene glycol chains. MAb fragment conjugation did not affect the biodistribution or long-circulating properties of i.v.-administered liposomes. However, antibody-directed targeting also did not increase the tumor localization of immunoliposomes, as both targeted and nontargeted liposomes achieved similarly high levels (7-8% injected dose/g tumor tissue) of tumor tissue accumulation in…

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Authors

9

Topics & keywords

Keywords
  • Internalization
  • Liposome
  • Endocytosis
  • Drug delivery
  • Monoclonal antibody
  • In vivo
  • Cancer cell
  • Targeted drug delivery
UN Sustainable Development Goals
  • Good health and well-being
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