Microarray analysis of lipopolysaccharide-treated human neutrophils

doi:10.1152/ajplung.00094.2002

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Microarray analysis of lipopolysaccharide-treated human neutrophils

Kenneth C. Malcolm¹, Patrick G. Arndt¹^,², Elizabeth J. Manos³, David A. Jones³, and G. Scott Worthen¹^,²

¹ Department of Medicine, National Jewish Medical and Research Center, Denver 80206; ² University of Colorado Health Sciences Center, Denver, Colorado 80262; and ³ The Huntsman Cancer Institute, University of Utah, Salt Lake City, Utah 84112

Neutrophils respond to infection by degranulation, release of reactive oxygen intermediates, and secretion of chemokines andcytokines; however, activation of neutrophil transcriptional machineryhas been little appreciated. Recent findings suggest that geneexpression may represent an additional neutrophil function afterexposure to lipopolysaccharide (LPS). We performed microarraygene expression analysis of 4,608 mostly nonredundant genes onLPS-stimulated human neutrophils. Analysis of three donors indicatedsome variability but also a high degree of reproducibility ingene expression. Twenty-eight verifiable, distinct genes wereinduced by 4 h of LPS treatment, and 13 genes were repressed.Genes other than cytokines and chemokines are regulated; interestingly,genes involved in cell growth regulation and survival, transcriptionalregulation, and interferon response are among those induced, whereasgenes involved in cytoskeletal regulation are predominantly repressed.In addition, we identified monocyte chemoattractant protein-1as a novel LPS-regulated chemokine in neutrophils. Included inthese lists are five clones with no defined function. These datasuggest molecular mechanisms by which neutrophils respond to infectionand indicate that the transcriptional potential of neutrophilsis greater than previouslythought.

cellular activation; gene regulation; Toll-like receptor; host defense

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