Autocrine IL-10 partially prevents differentiation of neonatal dendritic epidermal leukocytes into Langerhans cells

Souyet Chang-Rodriguez ^*, Rupert Ecker , Georg Stingl ^*, and Adelheid Elbe-Bürger ^*^@

*Department of Dermatology, Division of Immunology, Allergy and Infectious Diseases, Medical University of Vienna, Austria; and Competence Center for Bio Molecular Therapeutics, Vienna, Austria

^@ To whom correspondence should be addressed. E-mail: adelheid.elbe-buerger{at}meduniwien.ac.at.

Abstract

To test whether reduced immune responsiveness in early lifemay be related to the immaturity of neonatal antigen-presentingcells, we comparatively assessed the phenotypic and functionalcharacteristics of dendritic epidermal leukocytes (DEL) andepidermal Langerhans cells (LC) in newborn (NB) and adult mice,respectively. We report that purified, 3-day-cultured DEL donot acquire the morphology and phenotype typical of LC and aresignificantly weaker stimulators of naive, allogeneic CD4⁺ andCD8⁺ T cells than LC. Freshly isolated DEL are twice as efficientas LC in the uptake of fluorescein isothiocyanate-conjugatedtracers but are not able to present these to antigen-specificT cell hybridomas. To clarify the underlying cause, cytokineexpression of NB and adult epidermal cells (EC) was examined.We found that DEL express considerable amounts of interleukin(IL)-10, that IL-10 in NB EC supernatants partially inhibitsLC maturation, and that DEL-enriched EC from IL-10^-/- mice inducestronger primary T cell responses compared with those from IL-10^+/+mice. We conclude that IL-10 is one of the factors preventingmaturation and differentiation of DEL into immunocompetent LCin intrauterine life and is at least partly responsible forthe poor immune responsiveness of neonates.

Key Words: antigen presentation/processing • cytokines • cytokine receptors • dendritic cells • skin

Article

Autocrine IL-10 partially prevents differentiation of neonatal dendritic epidermal leukocytes into Langerhans cells