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Molecular Cancer Research 6, 175-185, February 1, 2008. doi: 10.1158/1541-7786.MCR-07-0391
© 2008 American Association for Cancer Research

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Angiogenesis, Metastasis, and the Cellular Microenvironment

Transcriptome of Hypoxic Immature Dendritic Cells: Modulation of Chemokine/Receptor Expression

Annamaria Ricciardi1, Angela Rita Elia2,3, Paola Cappello2,3, Maura Puppo1, Cristina Vanni1, Paolo Fardin1, Alessandra Eva1, David Munroe4, Xiaolin Wu4, Mirella Giovarelli2,3 and Luigi Varesio1

1 Laboratory of Molecular Biology, Giannina Gaslini Institute, Genoa, Italy; 2 Center for Experimental Research and Medical Studies, San Giovanni Battista Hospital; 3 Department of Medicine and Experimental Oncology, University of Turin, Turin, Italy; and 4 Laboratory of Molecular Technology, Science Applications International Corporation-Frederick, Inc., National Cancer Institute-Frederick, Frederick, Maryland

Requests for reprints: Annamaria Ricciardi, Istituto Giannina Gaslini, Largo Gaslini 5, 16147 Genova Quarto, Italy. Phone: 39-010-5636633; Fax: 39-010-3733346. E-mail: annamariaricciardi{at}ospedale-gaslini.ge.it

Hypoxia is a condition of low oxygen tension occurring in inflammatory tissues. Dendritic cells (DC) are professional antigen-presenting cells whose differentiation, migration, and activities are intrinsically linked to the microenvironment. DCs will home and migrate through pathologic tissues before reaching their final destination in the lymph node. We studied the differentiation of human monocytes into immature DCs (iDCs) in a hypoxic microenvironment. We generated iDC in vitro under normoxic (iDCs) or hypoxic (Hi-DCs) conditions and examined the hypoxia-responsive element in the promoter, gene expression, and biochemical KEGG pathways. Hi-DCs had an interesting phenotype represented by up-regulation of genes associated with cell movement/migration. In addition, the Hi-DC cytokine/receptor pathway showed a dichotomy between down-regulated chemokines and up-regulated chemokine receptor mRNA expression. We showed that CCR3, CX3CR1, and CCR2 are hypoxia-inducible genes and that CCL18, CCL23, CCL26, CCL24, and CCL14 are inhibited by hypoxia. A strong chemotactic response to CCR2 and CXCR4 agonists distinguished Hi-DCs from iDCs at a functional level. The hypoxic microenvironment promotes the differentiation of Hi-DCs, which differs from iDCs for gene expression profile and function. The most prominent characteristic of Hi-DCs is the expression of a mobility/migratory rather than inflammatory phenotype. We speculate that Hi-DCs have the tendency to leave the hypoxic tissue and follow the chemokine gradient toward normoxic areas where they can mature and contribute to the inflammatory process. (Mol Cancer Res 2008;6(2):175–85)







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Cancer Research Clinical Cancer Research
Cancer Epidemiology Biomarkers & Prevention Molecular Cancer Therapeutics
Molecular Cancer Research Cancer Prevention Research
Cancer Prevention Journals Portal Cancer Reviews Online
Annual Meeting Education Book Meeting Abstracts Online
Copyright © 2008 by the American Association for Cancer Research.