Injectable Nanoparticles Could Protect Injuries from Oxidative Stress
Author: Rice University - Contact: rice.edu
Published: 2015/02/11
Topic: Nanomedicine and Nanotechnology (Publications Database)
Page Content: Synopsis Introduction Main Item
Synopsis: Injectable nanoparticles that could protect an injured person from further damage due to oxidative stress have proven effective in tests.
Introduction
Scientists at Rice University, Baylor College of Medicine and the University of Texas Health Science Center at Houston (UTHealth) Medical School designed methods to validate their 2012 discovery that combined polyethylene glycol-hydrophilic carbon clusters - known as PEG-HCCs - could quickly stem the process of over-oxidation that can cause damage in the minutes and hours after an injury.
Main Item
The tests revealed a single nanoparticle can quickly catalyze the neutralization of thousands of damaging reactive oxygen species molecules that are over-expressed by the body's cells in response to an injury and turn the molecules into oxygen. These reactive species can damage cells and cause mutations, but PEG-HCCs appear to have an enormous capacity to turn them into less-reactive substances.
The researchers hope an injection of PEG-HCCs as soon as possible after an injury, such as traumatic brain injury or stroke, can mitigate further brain damage by restoring normal oxygen levels to the brain's sensitive circulatory system.
The results were reported today in the Proceedings of the National Academy of Sciences.
"Effectively, they bring the level of reactive oxygen species back to normal almost instantly," said Rice chemist James Tour. "This could be a useful tool for emergency responders who need to quickly stabilize an accident or heart attack victim or to treat soldiers in the field of battle." Tour led the new study with neurologist Thomas Kent of Baylor College of Medicine and biochemist Ah-Lim Tsai of UTHealth.
PEG-HCCs are about 3 nanometers wide and 30 to 40 nanometers long and contain from 2,000 to 5,000 carbon atoms. In tests, an individual PEG-HCC nanoparticle can catalyze the conversion of 20,000 to a million reactive oxygen species molecules per second into molecular oxygen, which damaged tissues need, and hydrogen peroxide while quenching reactive intermediates.
Tour and Kent led the earlier research that determined an infusion of nontoxic PEG-HCCs may quickly stabilize blood flow in the brain and protect against reactive oxygen species molecules over-expressed by cells during a medical trauma, especially when accompanied by massive blood loss.
Their research targeted traumatic brain injuries, after which cells release an excessive amount of the reactive oxygen species known as a superoxide into the blood. These toxic free radicals are molecules with one unpaired electron that the immune system uses to kill invading microorganisms. In small concentrations, they contribute to a cell's normal energy regulation. Generally, they are kept in check by superoxide dismutase, an enzyme that neutralizes superoxides.
But even mild traumas can release enough superoxides to overwhelm the brain's natural defenses. In turn, superoxides can form such other reactive oxygen species as peroxynitrite that cause further damage.
"The current research shows PEG-HCCs work catalytically, extremely rapidly and with an enormous capacity to neutralize thousands upon thousands of the deleterious molecules, particularly superoxide and hydroxyl radicals that destroy normal tissue when left unregulated," Tour said.
"This will be important not only in traumatic brain injury and stroke treatment, but for many acute injuries of any organ or tissue and in medical procedures such as organ transplantation," he said. "Anytime tissue is stressed and thereby oxygen-starved, superoxide can form to further attack the surrounding good tissue."
The researchers used an electron paramagnetic resonance spectroscopy technique that gets direct structure and rate information for superoxide radicals by counting unpaired electrons in the presence or absence of PEG-HCC antioxidants. Another test with an oxygen-sensing electrode, peroxidase and a red dye confirmed the particles' ability to catalyze superoxide conversion.
"In sharp contrast to the well-known superoxide dismutase, PEG-HCC is not a protein and does not have metal to serve the catalytic role," Tsai said. "The efficient catalytic turnover could be due to its more 'planar,' highly conjugated carbon core."
The tests showed the number of superoxides consumed far surpassed the number of possible PEG-HCC bonding sites. The researchers found the particles have no effect on important nitric oxides that keep blood vessels dilated and aid neurotransmission and cell protection, nor was the efficiency sensitive to pH changes.
"PEG-HCCs have enormous capacity to convert superoxide to oxygen and the ability to quench reactive intermediates while not affecting nitric oxide molecules that are beneficial in normal amounts," Kent said. "So they hold a unique place in our potential armamentarium against a range of diseases that involve loss of oxygen and damaging levels of free radicals."
The study also determined PEG-HCCs remain stable, as batches up to 3 months old performed as good as new.
Graduate student Errol Samuel and alumna Daniela Marcano, both of Rice, and Vladimir Berka, a senior research scientist at UTHealth, are lead authors of the study. Co-authors are Rice alumnus Austin Potter; alumnus Brittany Bitner and associate professor Robia Pautler of Baylor College of Medicine; instructor Gang Wu of UTHealth and Roderic Fabian of Baylor College of Medicine and the Michael E. DeBakey Veterans Affairs Medical Center.
Kent is a professor of neurology and director of stroke research and education at Baylor College of Medicine and chief of neurology and a member of the Center for Translational Research on Inflammatory Diseases at the DeBakey Center. Tour is the T.T. and W.F. Chao Chair in Chemistry as well as a professor of materials science and nano-engineering and of computer science and a member of Rice's Richard E. Smalley Institute for Nanoscale Science and Technology. Tsai is a professor of hematology at UTHealth and adjunct professor of biochemistry and cell biology at Rice.
The Mission Connect Mild Traumatic Brain Injury Consortium from the Department of Defense and the National Institutes of Health, the Alliance for Nano-Health and UTHealth supported the research.
Read the abstract at www.pnas.org/cgi/doi/10.1073/pnas.1417047112
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