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Influence of Stochastic Gene Expression on the Cell Survival Rheostat after Traumatic Brain Injury

Experimental evidence suggests that random, spontaneous (stochastic) fluctuations in gene expression have important biological consequences, including determination of cell fate and phenotypic variation within isogenic populations. We propose that fluctuations in gene expression represent a valuable...

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Autores principales: Rojo, Daniel R., Prough, Donald S., Falduto, Michael T., Boone, Deborah R., Micci, Maria-Adelaide, Kahrig, Kristen M., Crookshanks, Jeanna M., Jimenez, Arnaldo, Uchida, Tatsuo, Cowart, Jeremy C., Hawkins, Bridget E., Avila, Marcela, DeWitt, Douglas S., Hellmich, Helen L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3154935/
https://www.ncbi.nlm.nih.gov/pubmed/21853077
http://dx.doi.org/10.1371/journal.pone.0023111
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author Rojo, Daniel R.
Prough, Donald S.
Falduto, Michael T.
Boone, Deborah R.
Micci, Maria-Adelaide
Kahrig, Kristen M.
Crookshanks, Jeanna M.
Jimenez, Arnaldo
Uchida, Tatsuo
Cowart, Jeremy C.
Hawkins, Bridget E.
Avila, Marcela
DeWitt, Douglas S.
Hellmich, Helen L.
author_facet Rojo, Daniel R.
Prough, Donald S.
Falduto, Michael T.
Boone, Deborah R.
Micci, Maria-Adelaide
Kahrig, Kristen M.
Crookshanks, Jeanna M.
Jimenez, Arnaldo
Uchida, Tatsuo
Cowart, Jeremy C.
Hawkins, Bridget E.
Avila, Marcela
DeWitt, Douglas S.
Hellmich, Helen L.
author_sort Rojo, Daniel R.
collection PubMed
description Experimental evidence suggests that random, spontaneous (stochastic) fluctuations in gene expression have important biological consequences, including determination of cell fate and phenotypic variation within isogenic populations. We propose that fluctuations in gene expression represent a valuable tool to explore therapeutic strategies for patients who have suffered traumatic brain injury (TBI), for which there is no effective drug therapy. We have studied the effects of TBI on the hippocampus because TBI survivors commonly suffer cognitive problems that are associated with hippocampal damage. In our previous studies we separated dying and surviving hippocampal neurons by laser capture microdissection and observed unexplainable variations in post-TBI gene expression, even though dying and surviving neurons were adjacent and morphologically identical. We hypothesized that, in hippocampal neurons that subsequently are subjected to TBI, randomly increased pre-TBI expression of genes that are associated with neuroprotection predisposes neurons to survival; conversely, randomly decreased expression of these genes predisposes neurons to death. Thus, to identify genes that are associated with endogenous neuroprotection, we performed a comparative, high-resolution transcriptome analysis of dying and surviving hippocampal neurons in rats subjected to TBI. We found that surviving hippocampal neurons express a distinct molecular signature — increased expression of networks of genes that are associated with regeneration, cellular reprogramming, development, and synaptic plasticity. In dying neurons we found decreased expression of genes in those networks. Based on these data, we propose a hypothetical model in which hippocampal neuronal survival is determined by a rheostat that adds injury-induced genomic signals to expression of pro-survival genes, which pre-TBI varies randomly and spontaneously from neuron to neuron. We suggest that pharmacotherapeutic strategies that co-activate multiple survival signals and enhance self-repair mechanisms have the potential to shift the cell survival rheostat to favor survival and therefore improve functional outcome after TBI.
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spelling pubmed-31549352011-08-18 Influence of Stochastic Gene Expression on the Cell Survival Rheostat after Traumatic Brain Injury Rojo, Daniel R. Prough, Donald S. Falduto, Michael T. Boone, Deborah R. Micci, Maria-Adelaide Kahrig, Kristen M. Crookshanks, Jeanna M. Jimenez, Arnaldo Uchida, Tatsuo Cowart, Jeremy C. Hawkins, Bridget E. Avila, Marcela DeWitt, Douglas S. Hellmich, Helen L. PLoS One Research Article Experimental evidence suggests that random, spontaneous (stochastic) fluctuations in gene expression have important biological consequences, including determination of cell fate and phenotypic variation within isogenic populations. We propose that fluctuations in gene expression represent a valuable tool to explore therapeutic strategies for patients who have suffered traumatic brain injury (TBI), for which there is no effective drug therapy. We have studied the effects of TBI on the hippocampus because TBI survivors commonly suffer cognitive problems that are associated with hippocampal damage. In our previous studies we separated dying and surviving hippocampal neurons by laser capture microdissection and observed unexplainable variations in post-TBI gene expression, even though dying and surviving neurons were adjacent and morphologically identical. We hypothesized that, in hippocampal neurons that subsequently are subjected to TBI, randomly increased pre-TBI expression of genes that are associated with neuroprotection predisposes neurons to survival; conversely, randomly decreased expression of these genes predisposes neurons to death. Thus, to identify genes that are associated with endogenous neuroprotection, we performed a comparative, high-resolution transcriptome analysis of dying and surviving hippocampal neurons in rats subjected to TBI. We found that surviving hippocampal neurons express a distinct molecular signature — increased expression of networks of genes that are associated with regeneration, cellular reprogramming, development, and synaptic plasticity. In dying neurons we found decreased expression of genes in those networks. Based on these data, we propose a hypothetical model in which hippocampal neuronal survival is determined by a rheostat that adds injury-induced genomic signals to expression of pro-survival genes, which pre-TBI varies randomly and spontaneously from neuron to neuron. We suggest that pharmacotherapeutic strategies that co-activate multiple survival signals and enhance self-repair mechanisms have the potential to shift the cell survival rheostat to favor survival and therefore improve functional outcome after TBI. Public Library of Science 2011-08-11 /pmc/articles/PMC3154935/ /pubmed/21853077 http://dx.doi.org/10.1371/journal.pone.0023111 Text en Rojo et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Rojo, Daniel R.
Prough, Donald S.
Falduto, Michael T.
Boone, Deborah R.
Micci, Maria-Adelaide
Kahrig, Kristen M.
Crookshanks, Jeanna M.
Jimenez, Arnaldo
Uchida, Tatsuo
Cowart, Jeremy C.
Hawkins, Bridget E.
Avila, Marcela
DeWitt, Douglas S.
Hellmich, Helen L.
Influence of Stochastic Gene Expression on the Cell Survival Rheostat after Traumatic Brain Injury
title Influence of Stochastic Gene Expression on the Cell Survival Rheostat after Traumatic Brain Injury
title_full Influence of Stochastic Gene Expression on the Cell Survival Rheostat after Traumatic Brain Injury
title_fullStr Influence of Stochastic Gene Expression on the Cell Survival Rheostat after Traumatic Brain Injury
title_full_unstemmed Influence of Stochastic Gene Expression on the Cell Survival Rheostat after Traumatic Brain Injury
title_short Influence of Stochastic Gene Expression on the Cell Survival Rheostat after Traumatic Brain Injury
title_sort influence of stochastic gene expression on the cell survival rheostat after traumatic brain injury
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3154935/
https://www.ncbi.nlm.nih.gov/pubmed/21853077
http://dx.doi.org/10.1371/journal.pone.0023111
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