Neuron-Specific mRNA Complexity Responses during Hippocampal Apoptosis after Traumatic Brain Injury

doi:10.1523/JNEUROSCI.5051-03.2004

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The Journal of Neuroscience, March 24, 2004, 24(12):2866-2876; doi:10.1523/JNEUROSCI.5051-03.2004

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Neurobiology of Disease
Neuron-Specific mRNA Complexity Responses during Hippocampal Apoptosis after Traumatic Brain Injury
Paolo G. Marciano,¹ Julia Brettschneider,⁶ Elisabetta Manduchi,⁴ Jason E. Davis,³ Scott Eastman,⁷ Ramesh Raghupathi,³ Kathryn E. Saatman,³ Terence P. Speed,⁶ Christian J. Stoeckert, Jr,⁴ James H. Eberwine,²^* and Tracy K. McIntosh³^,5^*
Departments of ¹Neuroscience, ²Pharmacology, and ³Neurosurgery and ⁴Center for Bioinformatics, University of Pennsylvania, Philadelphia, Pennsylvania 19104, ⁵Veterans Administration Medical Center, Philadelphia, Pennsylvania 19104, ⁶Department of Statistics, University of California, Berkeley, California 94720, and ⁷Incyte Genomics, Fremont, California 94304

In an effort to understand the complexity of genomic responseswithin selectively vulnerable regions after experimental braininjury, we examined whether single apoptotic neurons from boththe CA3 and dentate differed from those in an uninjured brain.The mRNA from individual active caspase 3(+)/terminal deoxynucleotidyltransferase-mediated biotinylated UTP nick end labeling [TUNEL(–)]and active caspase 3(+)/TUNEL(+) pyramidal and granule neuronsin brain-injured mice were amplified and compared with thosefrom nonlabeled neurons in uninjured brains. Gene analysis revealedthat overall expression of mRNAs increased with activation ofcaspase 3 and decreased to below uninjured levels with TUNELreactivity. Cell type specificity of the apoptotic responsewas observed with both regionally distinct expression of mRNAsand differences in those mRNAs that were maximally regulated.Immunohistochemical analysis for two of the most highly differentiallyexpressed genes (prion and Sos2) demonstrated a correlationbetween the observed differential gene expression after traumaticbrain injury and corresponding protein translation.

Key words: apoptosis; traumatic brain injury; hippocampus; CA3; dentate; single-cell amplification; microarray; cell death; differential expression; real-time quantitative PCR

Received Nov 13, 2003; revised January 27, 2004; accepted January 29, 2004.

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