Healia

Medical Journals

Shut-down of Translation, a Global Neuronal Stress Response: Mechanisms and Pathological Relevance.

Authors:
  • Paschen Wulf
  • Proud Christopher G
  • Mies Günter

From: Multidisciplinary Neuroprotection Laboratories, Department of Anesthesiology, Duke University Medical Center, Durham, NC 27710, USA. wulf.paschen@duke.edu

Current pharmaceutical design

  • Publish Date: 2007
  • ISSN: 1873-4286
  • Volume: 13
  • Issue: 18
  • Pages: 1887-902
  • Medium: Internet
  • Language: English
  • Citation (JAMA): Paschen Wulf, Proud Christopher G, Mies Günter, et al. Shut-down of Translation, a Global Neuronal Stress Response: Mechanisms and Pathological Relevance.. Curr. Pharm. Des. 2007;13:1887-902

Abstract

Shut-down of translation is a global stress response required to block synthesis of proteins that cannot be correctly folded and thereby reduce the work load of the folding machinery, a primary target of the pathological process triggered by severe forms of stress. The short-term control of protein synthesis involves alterations in the activity of initiation factors mediated through changes in their phosphorylation states, the alpha subunit of eukaryotic initiation factor 2 being a key player in this process. While the stress-induced shut-down of translation is viewed as a protective response, the inability of vulnerable cells to restore protein synthesis after being exposed to a severe form of stress is a pathological process because it blocks the translation of messages coding for protective proteins required for restoration of function. In models of cerebral ischemia, prolonged suppression of protein synthesis is therefore always associated with extensive cell death. Endoplasmic reticulum (ER) dysfunction has been identified as the mechanism underlying ischemia-induced suppression of protein synthesis. GADD34 is a protein that plays a pivotal role in the recovery of cells from shut-down of translation induced by ER stress. After transient ischemia, a rise in GADD34 protein levels has been found in resistant but not in vulnerable cells. Knowledge of the mechanisms activated in resistant cells to restore protein synthesis after severe stress will help open up new avenues for therapeutic strategies to combat various disorders of the brain associated with impairment of the translational machinery.

Mesh Headings (Keywords): Animals, Antigens, Differentiation, Cell Cycle Proteins, Cell Death, Endoplasmic Reticulum, Eukaryotic Initiation Factors, Humans, Ischemic Attack, Transient, Neurons, Phosphorylation, Protein Biosynthesis, Protein Folding, RNA, Messenger, Stress

Check for Full Text / PubMed Unique Identifier (PMID): 17584115

This abstract is part of PubMed, a service of the U.S. National Library of Medicine. PubMed includes more than 17 million citations from MEDLINE and other life science journals for biomedical articles. See Copyright and Disclaimers.

Linked medical terms appearing on this page are added by Healia to help readers find more information and are not part of the original PubMed document.

The data herein was last updated on July 8th, 2008 and may not reflect the most current and accurate data available from NLM.

Advertisements

About | Privacy Policy | Business Solutions | Advertise | Contact | Add Healia to your site

©2012. Healia / Meredith Corporation  

Use of this site constitutes acceptance of our Terms of Service and Privacy Policy. All content on this Web site, including medical opinion and any other health-related information, is for informational purposes only and should not be used for a specific diagnosis or individual treatment plan for any situation. Use of this site and the information contained herein does not create a doctor-patient relationship. Always seek the direct advice of your doctor in connection with any questions or issues you may have regarding your own health or the health of others.