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Stem cells used to successfully regenerate damage in corticospinal injury

For first time, researchers show functional benefit in animal model of key motor control system

Date:
March 28, 2016
Source:
University of California - San Diego
Summary:
Researchers have successfully directed stem cell-derived neurons to regenerate lost tissue in damaged corticospinal tracts of rats, resulting in functional benefit, a new article reports.
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Writing in the March 28, 2016 issue of Nature Medicine, researchers at University of California, San Diego School of Medicine and Veterans Affairs San Diego Healthcare System, with colleagues in Japan and Wisconsin, report that they have successfully directed stem cell-derived neurons to regenerate lost tissue in damaged corticospinal tracts of rats, resulting in functional benefit.

"The corticospinal projection is the most important motor system in humans," said senior study author Mark Tuszynski, MD, PhD, professor in the UC San Diego School of Medicine Department of Neurosciences and director of the UC San Diego Translational Neuroscience Institute. "It has not been successfully regenerated before. Many have tried, many have failed -- including us, in previous efforts."

"The new thing here was that we used neural stem cells for the first time to determine whether they, unlike any other cell type tested, would support regeneration. And to our surprise, they did."

Specifically, the researchers grafted multipotent neural progenitor cells into sites of spinal cord injury in rats. The stem cells were directed to specifically develop as a spinal cord, and they did so robustly, forming functional synapses that improved forelimb movements in the rats. The feat upends an existing belief that corticospinal neurons lacked internal mechanisms needed for regeneration.

Previous studies have reported functional recovery in rats following various therapies for spinal cord injury, but none had involved regeneration of corticospinal axons. In humans, the corticospinal tract extends from the cerebral cortex in the upper brain down into the spinal cord.

"We humans use corticospinal axons for voluntary movement," said Tuszynski. "In the absence of regeneration of this system in previous studies, I was doubtful that most therapies taken to humans would improve function. Now that we can regenerate the most important motor system for humans, I think that the potential for translation is more promising."

Nonetheless, the road to testing and treatment in people remains long and uncertain.

"There is more work to do prior to moving to humans," Tuszynski said. We must establish long-term safety and long-term functional benefit in animals. We must devise methods for transferring this technology to humans in larger animal models. And we must identify the best type of human neural stem cell to bring to the clinic."


Story Source:

Materials provided by University of California - San Diego. Original written by Scott LaFee. Note: Content may be edited for style and length.


Journal Reference:

  1. Ken Kadoya, Paul Lu, Kenny Nguyen, Corinne Lee-Kubli, Hiromi Kumamaru, Lin Yao, Joshua Knackert, Gunnar Poplawski, Jennifer N Dulin, Hans Strobl, Yoshio Takashima, Jeremy Biane, James Conner, Su-Chun Zhang, Mark H Tuszynski. Spinal cord reconstitution with homologous neural grafts enables robust corticospinal regeneration. Nature Medicine, 2016; DOI: 10.1038/nm.4066

Cite This Page:

University of California - San Diego. "Stem cells used to successfully regenerate damage in corticospinal injury." ScienceDaily. ScienceDaily, 28 March 2016. <www.sciencedaily.com/releases/2016/03/160328114619.htm>.
University of California - San Diego. (2016, March 28). Stem cells used to successfully regenerate damage in corticospinal injury. ScienceDaily. Retrieved November 13, 2024 from www.sciencedaily.com/releases/2016/03/160328114619.htm
University of California - San Diego. "Stem cells used to successfully regenerate damage in corticospinal injury." ScienceDaily. www.sciencedaily.com/releases/2016/03/160328114619.htm (accessed November 13, 2024).

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