IRF4 promotes cutaneous dendritic cell migration to lymph nodes during homeostasis and inflammation

Migration of resident dendritic cells (DC) from the skin to local lymph nodes (LN) triggers T cell-mediated immune responses during cutaneous infection, autoimmune disease, and vaccination. In this study, we investigated whether the development and migration of skin-resident DC were regulated by IFN...

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Published inThe Journal of immunology (1950) Vol. 189; no. 7; pp. 3368 - 3377
Main Authors Bajaña, Sandra, Roach, Kimberly, Turner, Sean, Paul, Jinny, Kovats, Susan
Format Journal Article
LanguageEnglish
Published United States 01.10.2012
Subjects
Animals
CD11b Antigen - biosynthesis
Cell Movement - immunology
Cells, Cultured
Dendritic Cells - cytology
Dendritic Cells - immunology
Dendritic Cells - pathology
Female
Homeostasis - immunology
Inflammation Mediators - metabolism
Inflammation Mediators - physiology
Interferon Regulatory Factors - deficiency
Interferon Regulatory Factors - genetics
Interferon Regulatory Factors - physiology
Lymph Nodes - cytology
Lymph Nodes - immunology
Lymph Nodes - pathology
Male
Mice
Mice, Inbred C57BL
Mice, Knockout
Skin - cytology
Skin - immunology
Skin - pathology
Spleen - cytology
Spleen - immunology
Spleen - pathology
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Summary:Migration of resident dendritic cells (DC) from the skin to local lymph nodes (LN) triggers T cell-mediated immune responses during cutaneous infection, autoimmune disease, and vaccination. In this study, we investigated whether the development and migration of skin-resident DC were regulated by IFN regulatory factor 4 (IRF4), a transcription factor that is required for the development of CD11b(+) splenic DC. We found that the skin of naive IRF4(-/-) mice contained normal numbers of epidermal Langerhans cells (eLC) and increased numbers of CD11b(+) and CD103(+) dermal DC (dDC) populations, indicating that tissue DC development and skin residency is not disrupted by IRF4 deficiency. In contrast, numbers of migratory eLC and CD11b(+) dDC were significantly reduced in the cutaneous LN of IRF4(-/-) mice, suggesting a defect in constitutive migration from the dermis during homeostasis. Upon induction of skin inflammation, CD11b(+) dDC in IRF4(-/-) mice did not express the chemokine receptor CCR7 and failed to migrate to cutaneous LN, whereas the migration of eLC was only mildly impaired. Thus, although dispensable for their development, IRF4 is crucial for the CCR7-mediated migration of CD11b(+) dDC, a predominant population in murine and human skin that plays a vital role in normal and pathogenic cutaneous immunity.
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ISSN:0022-1767
1550-6606
DOI:10.4049/jimmunol.1102613