Blood-brainbarrier disruption dictates nanoparticle accumulation following experimental brain injury

Vimala N Bharadwaj; Rachel K Rowe; Jordan Harrison; Chen Wu; Trent R Anderson; Jonathan Lifshitz; P David Adelson; Vikram D Kodibagkar; Sarah E Stabenfeldt

doi:10.1016/j.nano.2018.06.004

Blood-brainbarrier disruption dictates nanoparticle accumulation following experimental brain injury

Nanomedicine. 2018 Oct;14(7):2155-2166. doi: 10.1016/j.nano.2018.06.004. Epub 2018 Jun 19.

Authors

Vimala N Bharadwaj¹, Rachel K Rowe², Jordan Harrison³, Chen Wu⁴, Trent R Anderson⁵, Jonathan Lifshitz⁶, P David Adelson⁷, Vikram D Kodibagkar¹, Sarah E Stabenfeldt⁸

Affiliations

¹ School of Biological and Health Systems Engineering, Arizona State University, Tempe, AZ.
² Department of Child Health, University of Arizona, College of Medicine, Phoenix, AZ; BARROW Neurological Institute at Phoenix Children's Hospital, Phoenix, AZ; Phoenix Veteran Affairs Healthcare System, Phoenix, AZ.
³ Interdisciplinary Graduate Program in Neuroscience, Arizona State University, Tempe, AZ.
⁴ Department of Child Health, University of Arizona, College of Medicine, Phoenix, AZ.
⁵ Basic Medical Sciences, University of Arizona, College of Medicine, Phoenix, AZ.
⁶ Department of Child Health, University of Arizona, College of Medicine, Phoenix, AZ; BARROW Neurological Institute at Phoenix Children's Hospital, Phoenix, AZ; Phoenix Veteran Affairs Healthcare System, Phoenix, AZ; Interdisciplinary Graduate Program in Neuroscience, Arizona State University, Tempe, AZ.
⁷ Department of Child Health, University of Arizona, College of Medicine, Phoenix, AZ; BARROW Neurological Institute at Phoenix Children's Hospital, Phoenix, AZ.
⁸ School of Biological and Health Systems Engineering, Arizona State University, Tempe, AZ. Electronic address: sarah.stabenfeldt@asu.edu.

Abstract

Clinically, traumatic brain injury (TBI) results in complex heterogeneous pathology that cannot be recapitulated in single pre-clinical animal model. Therefore, we focused on evaluating utility of nanoparticle (NP)-based therapeutics following three diffuse-TBI models: mildclosed-head injury (mCHI), repetitive-mCHI and midline-fluid percussion injury (FPI). We hypothesized that NP accumulation after diffuse TBI correlates directly with blood-brainbarrier permeability. Mice received PEGylated-NP cocktail (20-500 nm) (intravenously) after single- or repetitive-(1 impact/day, 5 consecutive days) CHI (immediately) and midline-FPI (1 h, 3 h and 6 h). NPs circulated for 1 h before perfusion/brain extraction. NP accumulation was analyzed using fluorescent microscopy in brain regions vulnerable to neuropathology. Minimal/no NP accumulation after mCHI/RmCHI was observed. In contrast, midlineFPI resulted in significant peak accumulation of up to 500 nm NP at 3 h post-injury compared to sham, 1 h, and 6 h groups in the cortex. Therefore, our study provides the groundwork for feasibility of NP-delivery based on NPinjection time and NPsize after mCHI/RmCHI and midline-FPI.

Keywords: Blood-brain barrier; Drug delivery; Fluid percussion injury; Mild closed head injury; Nanoparticles; Optimal therapeutic window; Pharmacodynamics; Traumatic brain injury.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Blood-Brain Barrier / drug effects
Blood-Brain Barrier / pathology*
Brain Injuries / metabolism*
Brain Injuries / pathology
Cell Membrane Permeability / drug effects*
Disease Models, Animal*
Male
Mice
Mice, Inbred C57BL
Nanoparticles / administration & dosage
Nanoparticles / chemistry
Nanoparticles / metabolism*

Grants and funding

DP2 HD084067/HD/NICHD NIH HHS/United States