4.7 Article

A Bacteria Deriving Peptide Modified Dendrigraft Poly-L-lysines (DGL) Self-Assembling Nanoplatform for Targeted Gene Delivery

Journal

MOLECULAR PHARMACEUTICS
Volume 11, Issue 10, Pages 3330-3341

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/mp500084s

Keywords

brain-targeted; tumor-targeted; gene delivery; laminin receptor; nanoparticles

Funding

  1. National Basic Research Program of China (973 Program) [2013CB932500]
  2. National Natural Science Foundation of China [81373355]
  3. Program for New Century Excellent Talents in University

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Achieving effective gene therapy for glioma depends on gene delivery systems. The gene delivery system should be able to cross the blood brain-barrier (BBB) and further target glioma at its early stage. Active brain tumor targeted delivery can be achieved using the Trojan horse technology, which involves either endogenous ligands or extraneous substances that can recognize and bind to specific receptors in target sites. This method facilitates receptor-mediated endocytosis to cross the BBB and enter into glioma cells. Dendrigraft poly-L-lysines (DGLs), which are novel nonviral gene vectors, are conjugated to a peptide (sequence: EPRNEEK) derived from Streptococcus pneumonia, a pathogen causing meningitis. This process yields peptide-modified nanoparticles (NPs) after DNA loading. Cellular uptake and in vivo imaging results indicate that EPRNEEK peptide-modified NPs have a better brain tumor targeted effect compared with a pentapeptide derived from endogenous laminin after intravenous injection. The mechanism of this effect is further explored in the present study. Besides, EPRNEEK peptide-modified NPs also exhibited a prolonged median survival time. In conclusion, the EPRNEEK peptide-modified DGL NPs exhibit potential as a nonviral platform for efficient, noninvasive, and safe brain glioma dual-targeted gene delivery.

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