Mast cell maturation is driven via a group III phospholipase A2-prostaglandin D2–DP1 receptor paracrine axis

Yoshitaka Taketomi,Kei Yamamoto,Masataka Nakamura,Kenji Kabashima,Momoko Kawana,Makoto Arita,Noriko Ueno,Hiroyasu Sato,Chisei Ra,Kazutaka Ikeda,Kikuko Watanabe,Kosuke Aritake,Shuh Narumiya,Mariko Sakanaka,Hiroyuki Hirai,Ryo Taguchi,Satoshi Tanaka,Makoto Murakami,Takao Shimizu,Naotomo Kambe,Takehiko Yokomizo,Yoshihiro Urade,Yasumasa Nishito,Yukihiko Sugimoto,Kazushi Morimoto,Satoshi Nakamizo,Yoshimichi Okayama,Shuntaro Hara,Remi Murase,Motonao Nakamura,Masanori Nakamura,Tatsuhiro Kojima ,Michael H Gelb

doi:10.1038/ni.2586

Abstract

Microenvironment-based alterations in phenotypes of mast cells influence the susceptibility to anaphylaxis, yet the mechanisms underlying proper maturation of mast cells toward an anaphylaxis-sensitive phenotype are incompletely understood. Here we report that PLA2G3, a mammalian homolog of anaphylactic bee venom phospholipase A2, regulates this process. PLA2G3 secreted from mast cells is coupled with fibroblastic lipocalin-type PGD2 synthase (L-PGDS) to provide PGD2, which facilitates mast-cell maturation via PGD2 receptor DP1. Mice lacking PLA2G3, L-PGDS or DP1, mast cell-deficient mice reconstituted with PLA2G3-null or DP1-null mast cells, or mast cells cultured with L-PGDS-ablated fibroblasts exhibited impaired maturation and anaphylaxis of mast cells. Thus, we describe a lipid-driven PLA2G3-L-PGDS-DP1 loop that drives mast cell maturation.

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