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Flow arrest intra-arterial delivery of small TAT-decorated and neutral micelles to gliomas

  • Juliane Nguyen
  • , Shaolie S. Hossain
  • , Johann R.N. Cooke
  • , Jason A. Ellis
  • , Michael B. Deci
  • , Charles W. Emala
  • , Jeffrey N. Bruce
  • , Irving J. Bigio
  • , Robert M. Straubinger
  • , Shailendra Joshi
  • SUNY Buffalo
  • University of Texas at Austin
  • Texas Heart Institute
  • Columbia University
  • Boston University

Research output: Contribution to journalArticlepeer-review

18 Scopus citations

Abstract

The cell-penetrating trans-activator of transcription (TAT) is a cationic peptide derived from human immunodeficiency virus-1. It has been used to facilitate macromolecule delivery to various cell types. This cationic peptide is capable of crossing the blood–brain barrier and therefore might be useful for enhancing the delivery of drugs that target brain tumors. Here we test the efficiency with which relatively small (20 nm) micelles can be delivered by an intra-arterial route specifically to gliomas. Utilizing the well-established method of flow-arrest intra-arterial injection we compared the degree of brain tumor deposition of cationic TAT-decorated micelles versus neutral micelles. Our in vivo and post-mortem analyses confirm glioma-specific deposition of both TAT-decorated and neutral micelles. Increased tumor deposition conferred by the positive charge on the TAT-decorated micelles was modest. Computational modeling suggested a decreased relevance of particle charge at the small sizes tested but not for larger particles. We conclude that continued optimization of micelles may represent a viable strategy for targeting brain tumors after intra-arterial injection. Particle size and charge are important to consider during the directed development of nanoparticles for intra-arterial delivery to brain tumors.

Original languageEnglish
Pages (from-to)77-85
Number of pages9
JournalJournal of Neuro-Oncology
Volume133
Issue number1
DOIs
StatePublished - May 1 2017

Keywords

  • Adjuvant therapy
  • Blood–brain barrier
  • Brain tumor
  • Chemotherapy
  • Drug delivery
  • Glioblastoma

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