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Journal Article

Citation

Shapiro LA. Cell Transplant. 2016; ePub(ePub): ePub.

Copyright

(Copyright © 2016, Cognizant Communication)

DOI

10.3727/096368916X693491

PMID

27772540

Abstract

Traumatic brain injury (TBI) is a devastating disorder, causing negative outcomes in millions of people each year. Despite the alarming numbers of brain injuries, and the long-term detrimental outcomes that can be associate with TBI, treatment options are lacking. Extensive investigation is underway, in hopes of identifying effective treatment strategies. Among the most state-of-the-art strategies is cell replacement therapy. TBI is a seemingly good candidate for cell replacement studies, because there is often neuron loss. However, translation of this therapy has not yet been successful. It is possible that a better understanding of endogenous neurogenic mechanisms after TBI could lead to more efficacious study designs using exogenous cell replacement strategies. Therefore, this study was designed to examine the number and migration of immature neurons at 1 and 7 days after a fluid percussion TBI. The results show that the number of immature neurons increases from by 7 days after an FPI, and there is ectopic migration of DCX+ immature neurons into the hilar region of the dentate gyrus. The results add important data to the understanding of the endogenous neurogenic niche after TBI. Follow-up studies are needed to better understand the functional significance of elevated neurogenesis and aberrant migration into the hilus.


Language: en

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