Oxidized Activated Charcoal Nanozymes: Synthesis, and Optimization for In Vitro and In Vivo Bioactivity for Traumatic Brain Injury

Author:

McHugh Emily A.1,Liopo Anton V.2ORCID,Mendoza Kimberly1,Robertson Claudia S.3,Wu Gang4,Wang Zhe1,Chen Weiyin1,Beckham Jacob L.1,Derry Paul J.25ORCID,Kent Thomas A.126ORCID,Tour James M.1789

Affiliation:

1. Department of Chemistry Rice University 6100 Main Street Houston TX 77005 USA

2. Institute of Biosciences and Technology Texas A&M Health Science Center 2121 W. Holcombe Street Houston TX 77030 USA

3. Department of Neurosurgery Baylor College of Medicine Houston TX 77030 USA

4. Hematology, Internal Medicine University of Texas McGovern Medical School—Houston Houston TX 77030 USA

5. EnMed School of Engineering Medicine Texas A&M University 1020 W. Holcombe Blvd Houston TX 77030 USA

6. Stanley H. Appel Department of Neurology and Research Institute Houston Methodist Hospital Houston TX 77030 USA

7. Smalley‐Curl Institute Rice University 6100 Main Street Houston TX 77005 USA

8. Department of Materials Science and NanoEngineering Rice University 6100 Main Street Houston TX 77005 USA

9. NanoCarbon Center and the Welch Institute for Advanced Materials Rice University 6100 Main Street Houston TX 77005 USA

Abstract

AbstractCarbon‐based superoxide dismutase (SOD) mimetic nanozymes have recently been employed as promising antioxidant nanotherapeutics due to their distinct properties. The structural features responsible for the efficacy of these nanomaterials as antioxidants are, however, poorly understood. Here, the process–structure–property–performance properties of coconut‐derived oxidized activated charcoal (cOAC) nano‐SOD mimetics are studied by analyzing how modifications to the nanomaterial's synthesis impact the size, as well as the elemental and electrochemical properties of the particles. These properties are then correlated to the in vitro antioxidant bioactivity of poly(ethylene glycol)‐functionalized cOACs (PEG‐cOAC). Chemical oxidative treatment methods that afford smaller, more homogeneous cOAC nanoparticles with higher levels of quinone functionalization show enhanced protection against oxidative damage in bEnd.3 murine endothelioma cells. In an in vivo rat model of mild traumatic brain injury (mTBI) and oxidative vascular injury, PEG‐cOACs restore cerebral perfusion rapidly to the same extent as the former nanotube‐derived PEG‐hydrophilic carbon clusters (PEG‐HCCs) with a single intravenous injection. These findings provide a deeper understanding of how carbon nanozyme syntheses can be tailored for improved antioxidant bioactivity, and set the stage for translation of medical applications.

Funder

National Institutes of Health

Welch Foundation

Publisher

Wiley

Subject

Mechanical Engineering,Mechanics of Materials,General Materials Science

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