The effects of globin on microarray-based gene expression analysis of mouse blood

被引:0
|
作者
Mary E. Winn
Matthew A. Zapala
Iiris Hovatta
Victoria B. Risbrough
Elizabeth Lillie
Nicholas J. Schork
机构
[1] University of California at San Diego,Graduate Program in Biomedical Sciences, Department of Medicine
[2] The Scripps Research Institute,Scripps Genomic Medicine, Department of Molecular & Experimental Medicine, and The Scripps Translational Science Institute
[3] University of California at San Diego,Department of Radiology
[4] University of Helsinki,Research Program of Molecular Neurology and Department of Medical Genetics
[5] National Institute for Health and Welfare,Department of Mental Health and Substance Abuse Services
[6] University of California at San Diego,Department of Psychiatry
[7] Center of Excellence for Stress and Mental Health,undefined
[8] Veteran’s Affairs,undefined
来源
Mammalian Genome | 2010年 / 21卷
关键词
Mouse Blood; Tissue Gene Expression; Blood Gene Expression; Globin mRNA; Globin Reduction;
D O I
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中图分类号
学科分类号
摘要
The use of mouse blood as a model for human blood is often considered in the development of clinically relevant, gene expression-based disease biomarkers. However, the ability to derive biologically meaningful insights from microarray-based gene expression patterns in mouse whole blood, as in human whole blood, is hindered by high levels of globin mRNA. In order to characterize the effects of globin reduction on gene expression of peripheral mouse blood, we performed gene set enrichment analysis on genes identified as expressed in blood via microarray-based genome-wide transcriptome analysis. Depletion of globin mRNA enhanced the quality of microarray data as shown by improved gene expression detection and increased sensitivity. Compared to genes expressed in whole blood, genes detected as expressed in blood following globin reduction were enriched for low abundance transcripts implicated in many biological pathways, including development, g-protein signaling, and immune response. Broadly, globin reduction resulted in improved detection of expressed genes that serve as molecular binding proteins and enzymes in cellular metabolism, intracellular transport/localization, transcription, and translation, as well as genes that potentially could act as biomarkers for diseases such as schizophrenia. These significantly enriched pathways overlap considerably with those identified in globin-reduced human blood suggesting that globin-reduced mouse blood gene expression studies may be useful for identifying genes relevant to human disease. Overall, the results of this investigation provide a better understanding of the impact of reducing globin transcripts in mouse blood and highlight the potential of microarray-based, globin-reduced, mouse blood gene expression studies in biomarker development.
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页码:268 / 275
页数:7
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