Widely used iron nanoparticles exhibit toxic effects on neuronal cells. |
Researchers at UC San Diego have discovered that iron-containing nanoparticles being tested for use in several biomedical applications can be toxic to nerve cells and interfere with the formation of their signal-transmitting extensions.
In their studies, the UCSD researchers used PC12 cells, a line derived from a rat pheochromocytoma. Nerve growth factor prompts PC12 cells to express a variety of neuron-specific genes and generate thin sprout-like cellular extensions called neurites, which are hundreds of times longer than the width of the cell, or up to several millimeters in length. These properties of PC12 cells have made them useful for studying the neurobiological and neurochemical properties of nerve cells.
Jin's group had initially investigated the nanoparticles for use in in vitro studies as a possible way to manipulate nerve cells remotely with magnetic force. Eventually they had hoped to conduct in vivo experiments, using nanoparticles-laden nerve cells to bridge regions of damaged neurons. However, when they added nerve growth factor to nanoparticle-laden cells in culture flasks, they observed toxic dose-dependent effects: some cells died, and many of the survivors exhibited a diminished ability to produce neurites.
In their experiments, PC12 cells that had not been exposed to magnetic nanoparticles generated three neurites in response to nerve growth factor. However, exposure to a low concentration of iron oxide nanoparticles resulted in the production of fewer than three neurites per cell in response to growth factor addition. A 10-fold increase in the concentration of nanoparticles led to the production of two neurites per cell, and a 10-fold increase of that concentration resulted in only one neurite per cell. Additionally, neurites produced in response to the growth factor in the presence of iron oxide nanoparticles were less well formed and also showed abnormal morphology and neurobiological characteristics.
The researchers also studied long protein polymers inside the PC12 cells that make up the cytoskeletal structure. They found that iron oxide nanoparticles resulted in fewer and less organized microtubules and microfilaments, protein polymers involved in cell motility and cell shape.
"It's worth noting that neither iron oxide nanoparticles alone, nor the coating material alone are overtly toxic, but combining the two to create water-soluble nanoparticles has a completely different effect," said Pisanic, who carried out the studies as a part of a Ph.D. thesis project at UCSD.
Iron oxide nanoparticles are considered promising because they are maneuverable by remote magnetic fields, and can be coated with various marker molecules to make them stick selectively to tumors and other targets within the body. The particles can also be made to carry anti-cancer drugs or radioactive materials directly to a tumor. Magnetic nanoparticles designed to attach to cancerous tissue can also be made to heat up by using a remote, alternating magnetic field, thereby selectively killing cancer cells in a process called magnetic hyperthermia.
Many researchers throughout the world are also studying the use of iron-containing nanoparticles in gene therapy, magnetic resonance imaging (MRI), and other medically important applications. While studies have focused primarily on the many potential uses of nanoparticles, Jin said more attention should be paid to their safety. "Our experience leads us to conclude that any analysis of the biocompatibility of nanoparticles should include not just a toxicological study of the component parts," said Pisanic, "but also an examination of the total structure as a whole." ###
Contact: Rex Graham ragraham@ucsd.edu 858-822-3075 University of California - San Diego
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