Journal home > Archive > Table of Contents > Article > Abstract

Journal home Advance online publication Current issue Archive Press releases Supplements Focuses Guide to authors Online submission For referees Free online issue Contact the journal Subscribe Advertising work@npg Reprints and permissions About this site For librarians   NPG Resources Nature Nature Reviews Nature Immunology Nature Cell Biology Nature Genetics news@nature.com Nature Conferences Dissect Medicine NPG Subject areas Biotechnology Cancer Chemistry Clinical Medicine Dentistry Development Drug Discovery Earth Sciences Evolution & Ecology Genetics Immunology Materials Science Medical Research Microbiology Molecular Cell Biology Neuroscience Pharmacology Physics Browse all publications Article Nature Medicine  9, 744 - 749 (2003) Published online: 12 May 2003; | doi:10.1038/nm872 Prostaglandin E2−EP4 signaling initiates skin immune responses by promoting migration and maturation of Langerhans cells Kenji Kabashima1, 2, Daiji Sakata1, Miyako Nagamachi1, 2, Yoshiki Miyachi2, Kayo Inaba3 & Shuh Narumiya1 1  Department of Pharmacology, Kyoto University Faculty of Medicine, Kyoto 606-8501, Japan. 2  Department of Dermatology, Kyoto University Faculty of Medicine, Kyoto 606-8501, Japan. 3  Department of Animal Development and Physiology, Graduate School of Biostudies, Kyoto University, Kyoto 606-8502, Japan. Correspondence should be addressed to Shuh Narumiya snaru@mfour.med.kyoto-u.ac.jpAntigen-specific immune responses in the skin are initiated by antigen uptake into Langerhans cells and the subsequent migration of these cells to draining lymph nodes. Although prostaglandin E2 (PGE2) is produced substantially in skin exposed to antigen, its role remains unclear. Here we show that although Langerhans cells express all four PGE receptor subtypes, their migration to regional lymph nodes was decreased only in EP4-deficient (Ptger4-/-) mice and in wild-type mice treated with an EP4 antagonist. An EP4 agonist promoted the migration of Langerhans cells, increased their expression of costimulatory molecules and enhanced their ability to stimulate T cells in the mixed lymphocyte reaction in vitro. Contact hypersensitivity to antigen was impaired in Ptger4-/- mice and in wild-type mice treated with the EP4 antagonist during sensitization. PGE2-EP4 signaling thus facilitates initiation of skin immune responses by promoting the migration and maturation of Langerhans cells.  Top Abstract Previous | Next Table of contents Full text Download PDF Send to a friend Open Innovation Challenges Methods of Modeling Adaptation in Populations Deadline: Dec 30 2009 Reward: $15,000 USD The analysis of adaptation with a population is a frequently encountered computational modeling scen... Novel Approaches to Protecting Maize from Insect Damage Deadline: Nov 29 2009 Reward: $20,000 USD The Seeker is looking for novel approaches to protecting maize from insect damage. This Challenge re... More Challenges Powered by: nature jobs Manager / Sr. Manager - Business Development (Custom Synthesis) Syngene International Bangalore, Karnataka 560099 India Leadership Fellowships University of Oxford Oxford United Kingdom More science jobs Post a job for free Figures & Tables Export citation Search buyers guide:   ADVERTISEMENT

ISSN: 1078-8956 EISSN: 1546-170X Journal home | Advance online publication | Current issue | Archive | Press releases | Supplements | Focuses | For authors | Online submission | For referees | Free online issue | About the journal | Contact the journal | Subscribe | Advertising | work@npg | Reprints and permissions | About this site | For librarians

©2003 Nature Publishing Group | Privacy policy