Age and Sex Differences in Brain Gene Expression in Neonatal Rats

D. Torbati; B. R. Totapally; A. Raszynski; J. Osborne; L. van Zyl; S. Kalomiris; J. Wolfsdorf

doi:10.1055/s-0028-1105923

Neuropediatrics, Table of Contents

Neuropediatrics 2008; 39(4): 219-225
DOI: 10.1055/s-0028-1105923

Original Article

Age and Sex Differences in Brain Gene Expression in Neonatal Rats

D. Torbati¹ , B. R. Totapally¹ , A. Raszynski¹ , J. Osborne² , L. van Zyl³ , S. Kalomiris¹ , J. Wolfsdorf¹

¹Division of Critical Care Medicine, Miami Children's Hospital, Miami, FL, USA
²North Carolina State University, Department of Statistics, Raleigh, NC, USA
³ArrayXpress, Raleigh, NC, USA

Abstract

Gene expression in the central nervous system is highly region-specific. We tested the hypothesis that certain developmental biomarkers could be detected in the whole brain or in cortical, subcortical or cerebellar structures. Brain gene expressions of male and female rats at birth, 3 days, and 10 days of age were measured by microarray technique (≈10 K genes; n=9/category). We found 53 significantly up-regulated and 8 down-regulated genes at 10 days of age, relative to birth and 3 days of age. The whole brain, however, showed no significant sex differences in gene expression patterns up to 10 days of age. Ten genes with the highest up-regulation, and 5 down-regulated genes were further confirmed by quantitative real-time PCR (Q-PCR), using the whole brain, cortices, subcortical structures, and cerebellum. The Q-PCR confirmed genes are known to be involved in neuronal differentiation, axonal myelination and growth, neurotransmission and glycolytic pathways. With a few exceptions, the expression levels of Q-PCR confirmed genes were significantly different in the whole brain, compared to other regions. In a separate study, we tested the potential utility of the Q-PCR confirmed genes, as whole brain biomarkers, after a six-hour exposure to hyperoxia (>98% oxygen breathing) in 10 days old rats. This relatively mild oxidative challenge created a 3.5-fold increase in the expression of T-cell receptor β Variable 8.3b, known to have regulatory function during development. We suggest that genes displaying significant expression in the whole brain, regardless of their origin, could be used to screen normal brain development in neonatal rat models of experimental neurology.

Key words

brain development - gene expression - gene profiling - microarrays - neonatal rats

Full Text

References

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Correspondence

Prof. D. TorbatiPhD

Division of Critical Care Medicine

Miami Children's Hospital

Miami

FL 33155

USA

Phone: +1/305/663 85 26

Fax: +1/305/663 05 30

Email: Dan.Torbati@MCH.Com