Over-expression of p73β results in apoptotic death of post-mitotic hNT neurons

The p53-related p73 protein is an important mediator of apoptosis, development and tumorigenesis. Previously, we showed that over-expression of the p73β isoform induced apoptosis in proliferating neuronal cells; however, the study did not address the effect of p73 in post-mitotic neurons. To address...

Full description

Saved in:
Bibliographic Details
Published in:Journal of the neurological sciences 2006-01, Vol.240 (1), p.1-6
Main Authors: Jiang, Yuying, Lo, Warren, Akhmametyeva, Elena M., Chang, Long-Sheng
Format: Article
Language:English
Subjects:
Apoptosis
Bax
Biological and medical sciences
Development. Senescence. Regeneration. Transplantation
Fundamental and applied biological sciences. Psychology
Injuries of the nervous system and the skull. Diseases due to physical agents
Medical sciences
Neurology
p57 Kip2
p73
Post-mitotic hNT neurons
Recombinant adenovirus
Traumas. Diseases due to physical agents
Vertebrates: nervous system and sense organs
Citations: Items that this one cites
Items that cite this one
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:The p53-related p73 protein is an important mediator of apoptosis, development and tumorigenesis. Previously, we showed that over-expression of the p73β isoform induced apoptosis in proliferating neuronal cells; however, the study did not address the effect of p73 in post-mitotic neurons. To address this question, we used post-mitotic hNT neurons, which have been used as a model of human central nervous system neurons. We found that over-expression of p73β in hNT neurons resulted in apoptosis and an increase in the expression of p57 Kip2 and Bax, but no increase in p53 expression. These results suggest that apoptosis of post-mitotic neurons induced by p73β may involve these mediators. Understanding the regulation of p73 expression will be important for understanding the development of the nervous system and may have implications for the treatment of neurological diseases.
ISSN:0022-510X
1878-5883
DOI:10.1016/j.jns.2005.08.012