Literature DB >> 18627434

Translation arrest and ribonomics in post-ischemic brain: layers and layers of players.

Donald J DeGracia1, Jill T Jamison, Jeffrey J Szymanski, Monique K Lewis.   

Abstract

A persistent translation arrest (TA) correlates precisely with the selective vulnerability of post-ischemic neurons. Mechanisms of post-ischemic TA that have been assessed include ribosome biochemistry, the link between TA and stress responses, and the inactivation of translational components via sequestration in subcellular structures. Each of these approaches provides a perspective on post-ischemic TA. Here, we develop the notion that mRNA regulation via RNA-binding proteins, or ribonomics, also contributes to post-ischemic TA. We describe the ribonomic network, or structures involved in mRNA regulation, including nuclear foci, polysomes, stress granules, embryonic lethal abnormal vision/Hu granules, processing bodies, exosomes, and RNA granules. Transcriptional, ribonomic, and ribosomal regulation together provide multiple layers mediating cell reprogramming. Stress gene induction via the heat-shock response, immediate early genes, and endoplasmic reticulum stress represents significant reprogramming of post-ischemic neurons. We present a model of post-ischemic TA in ischemia-resistant neurons that incorporates ribonomic considerations. In this model, selective translation of stress-induced mRNAs contributes to translation recovery. This model provides a basis to study dysfunctional stress responses in vulnerable neurons, with a key focus on the inability of vulnerable neurons to selectively translate stress-induced mRNAs. We suggest a ribonomic approach will shed new light on the roles of mRNA regulation in persistent TA in vulnerable post-ischemic neurons.

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Year:  2008        PMID: 18627434      PMCID: PMC2574835          DOI: 10.1111/j.1471-4159.2008.05561.x

Source DB:  PubMed          Journal:  J Neurochem        ISSN: 0022-3042            Impact factor:   5.372


  96 in total

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Authors:  Muriel Brengues; Daniela Teixeira; Roy Parker
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6.  An Hsp70-like protein in the ER: identity with the 78 kd glucose-regulated protein and immunoglobulin heavy chain binding protein.

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8.  Co-translational protein aggregation after transient cerebral ischemia.

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  26 in total

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2.  Reaction of small heat-shock proteins to different kinds of cellular stress in cultured rat hippocampal neurons.

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Review 6.  Heterogeneity in the penumbra.

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9.  mRNA redistribution during permanent focal cerebral ischemia.

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10.  HuR function and translational state analysis following global brain ischemia and reperfusion.

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