Lipid-orchestrated paracrine circuit coordinates mast cell maturation and anaphylaxis through functional interaction with fibroblasts

Yoshitaka Taketomi; Takayoshi Higashi; Kuniyuki Kano; Yoshimi Miki; Chika Mochizuki; Shota Toyoshima; Yoshimichi Okayama; Yasumasa Nishito; Susumu Nakae; Satoshi Tanaka; Suzumi M. Tokuoka; Yoshiya Oda; Shigeyuki Shichino; Satoshi Ueha; Kouji Matsushima; Noriyuki Akahoshi; Satoshi Ishii; Jerold Chun; Junken Aoki; Makoto Murakami

doi:10.1016/j.immuni.2024.06.012

Lipid-orchestrated paracrine circuit coordinates mast cell maturation and anaphylaxis through functional interaction with fibroblasts

Yoshitaka Taketomi, Takayoshi Higashi, Kuniyuki Kano, Yoshimi Miki, Chika Mochizuki, Shota Toyoshima, Yoshimichi Okayama, Yasumasa Nishito, Susumu Nakae, Satoshi Tanaka, Suzumi M. Tokuoka, Yoshiya Oda, Shigeyuki Shichino, Satoshi Ueha, Kouji Matsushima, Noriyuki Akahoshi, Satoshi Ishii, Jerold Chun, Junken Aoki, Makoto Murakami

Research Institute for Biomedical Sciences

Research output: Contribution to journal › Article › peer-review

3 Citations (Scopus)

Abstract

Interaction of mast cells (MCs) with fibroblasts is essential for MC maturation within tissue microenvironments, although the underlying mechanism is incompletely understood. Through a phenotypic screening of >30 mouse lines deficient in lipid-related genes, we found that deletion of the lysophosphatidic acid (LPA) receptor LPA₁, like that of the phospholipase PLA2G3, the prostaglandin D₂ (PGD₂) synthase L-PGDS, or the PGD₂ receptor DP1, impairs MC maturation and thereby anaphylaxis. Mechanistically, MC-secreted PLA2G3 acts on extracellular vesicles (EVs) to supply lysophospholipids, which are converted by fibroblast-derived autotaxin (ATX) to LPA. Fibroblast LPA₁ then integrates multiple pathways required for MC maturation by facilitating integrin-mediated MC-fibroblast adhesion, IL-33-ST2 signaling, L-PGDS-driven PGD₂ generation, and feedforward ATX-LPA₁ amplification. Defective MC maturation resulting from PLA2G3 deficiency is restored by supplementation with LPA₁ agonists or PLA2G3-modified EVs. Thus, the lipid-orchestrated paracrine circuit involving PLA2G3-driven lysophospholipid, eicosanoid, integrin, and cytokine signaling fine-tunes MC-fibroblast communication, ensuring MC maturation.

Original language	English
Pages (from-to)	1828-1847.e11
Journal	Immunity
Volume	57
Issue number	8
DOIs	https://doi.org/10.1016/j.immuni.2024.06.012
Publication status	Published - 13 Aug 2024

Keywords

anaphylaxis
fibroblast
lipid mediator
lysophosphatidic acid
mast cell
phospholipase A
prostaglandin

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10.1016/j.immuni.2024.06.012

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Taketomi, Y., Higashi, T., Kano, K., Miki, Y., Mochizuki, C., Toyoshima, S., Okayama, Y., Nishito, Y., Nakae, S., Tanaka, S., Tokuoka, S. M., Oda, Y., Shichino, S., Ueha, S., Matsushima, K., Akahoshi, N., Ishii, S., Chun, J., Aoki, J., & Murakami, M. (2024). Lipid-orchestrated paracrine circuit coordinates mast cell maturation and anaphylaxis through functional interaction with fibroblasts. Immunity, 57(8), 1828-1847.e11. https://doi.org/10.1016/j.immuni.2024.06.012

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title = "Lipid-orchestrated paracrine circuit coordinates mast cell maturation and anaphylaxis through functional interaction with fibroblasts",

abstract = "Interaction of mast cells (MCs) with fibroblasts is essential for MC maturation within tissue microenvironments, although the underlying mechanism is incompletely understood. Through a phenotypic screening of >30 mouse lines deficient in lipid-related genes, we found that deletion of the lysophosphatidic acid (LPA) receptor LPA1, like that of the phospholipase PLA2G3, the prostaglandin D2 (PGD2) synthase L-PGDS, or the PGD2 receptor DP1, impairs MC maturation and thereby anaphylaxis. Mechanistically, MC-secreted PLA2G3 acts on extracellular vesicles (EVs) to supply lysophospholipids, which are converted by fibroblast-derived autotaxin (ATX) to LPA. Fibroblast LPA1 then integrates multiple pathways required for MC maturation by facilitating integrin-mediated MC-fibroblast adhesion, IL-33-ST2 signaling, L-PGDS-driven PGD2 generation, and feedforward ATX-LPA1 amplification. Defective MC maturation resulting from PLA2G3 deficiency is restored by supplementation with LPA1 agonists or PLA2G3-modified EVs. Thus, the lipid-orchestrated paracrine circuit involving PLA2G3-driven lysophospholipid, eicosanoid, integrin, and cytokine signaling fine-tunes MC-fibroblast communication, ensuring MC maturation.",

keywords = "anaphylaxis, fibroblast, lipid mediator, lysophosphatidic acid, mast cell, phospholipase A, prostaglandin",

author = "Yoshitaka Taketomi and Takayoshi Higashi and Kuniyuki Kano and Yoshimi Miki and Chika Mochizuki and Shota Toyoshima and Yoshimichi Okayama and Yasumasa Nishito and Susumu Nakae and Satoshi Tanaka and Tokuoka, {Suzumi M.} and Yoshiya Oda and Shigeyuki Shichino and Satoshi Ueha and Kouji Matsushima and Noriyuki Akahoshi and Satoshi Ishii and Jerold Chun and Junken Aoki and Makoto Murakami",

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doi = "10.1016/j.immuni.2024.06.012",

language = "English",

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Taketomi, Y, Higashi, T, Kano, K, Miki, Y, Mochizuki, C, Toyoshima, S, Okayama, Y, Nishito, Y, Nakae, S, Tanaka, S, Tokuoka, SM, Oda, Y, Shichino, S , Ueha, S , Matsushima, K, Akahoshi, N, Ishii, S, Chun, J, Aoki, J & Murakami, M 2024, 'Lipid-orchestrated paracrine circuit coordinates mast cell maturation and anaphylaxis through functional interaction with fibroblasts', Immunity, vol. 57, no. 8, pp. 1828-1847.e11. https://doi.org/10.1016/j.immuni.2024.06.012

TY - JOUR

T1 - Lipid-orchestrated paracrine circuit coordinates mast cell maturation and anaphylaxis through functional interaction with fibroblasts

AU - Taketomi, Yoshitaka

AU - Higashi, Takayoshi

AU - Kano, Kuniyuki

AU - Miki, Yoshimi

AU - Mochizuki, Chika

AU - Toyoshima, Shota

AU - Okayama, Yoshimichi

AU - Nishito, Yasumasa

AU - Nakae, Susumu

AU - Tanaka, Satoshi

AU - Tokuoka, Suzumi M.

AU - Oda, Yoshiya

AU - Shichino, Shigeyuki

AU - Ueha, Satoshi

AU - Matsushima, Kouji

AU - Akahoshi, Noriyuki

AU - Ishii, Satoshi

AU - Chun, Jerold

AU - Aoki, Junken

AU - Murakami, Makoto

PY - 2024/8/13

Y1 - 2024/8/13

N2 - Interaction of mast cells (MCs) with fibroblasts is essential for MC maturation within tissue microenvironments, although the underlying mechanism is incompletely understood. Through a phenotypic screening of >30 mouse lines deficient in lipid-related genes, we found that deletion of the lysophosphatidic acid (LPA) receptor LPA1, like that of the phospholipase PLA2G3, the prostaglandin D2 (PGD2) synthase L-PGDS, or the PGD2 receptor DP1, impairs MC maturation and thereby anaphylaxis. Mechanistically, MC-secreted PLA2G3 acts on extracellular vesicles (EVs) to supply lysophospholipids, which are converted by fibroblast-derived autotaxin (ATX) to LPA. Fibroblast LPA1 then integrates multiple pathways required for MC maturation by facilitating integrin-mediated MC-fibroblast adhesion, IL-33-ST2 signaling, L-PGDS-driven PGD2 generation, and feedforward ATX-LPA1 amplification. Defective MC maturation resulting from PLA2G3 deficiency is restored by supplementation with LPA1 agonists or PLA2G3-modified EVs. Thus, the lipid-orchestrated paracrine circuit involving PLA2G3-driven lysophospholipid, eicosanoid, integrin, and cytokine signaling fine-tunes MC-fibroblast communication, ensuring MC maturation.

AB - Interaction of mast cells (MCs) with fibroblasts is essential for MC maturation within tissue microenvironments, although the underlying mechanism is incompletely understood. Through a phenotypic screening of >30 mouse lines deficient in lipid-related genes, we found that deletion of the lysophosphatidic acid (LPA) receptor LPA1, like that of the phospholipase PLA2G3, the prostaglandin D2 (PGD2) synthase L-PGDS, or the PGD2 receptor DP1, impairs MC maturation and thereby anaphylaxis. Mechanistically, MC-secreted PLA2G3 acts on extracellular vesicles (EVs) to supply lysophospholipids, which are converted by fibroblast-derived autotaxin (ATX) to LPA. Fibroblast LPA1 then integrates multiple pathways required for MC maturation by facilitating integrin-mediated MC-fibroblast adhesion, IL-33-ST2 signaling, L-PGDS-driven PGD2 generation, and feedforward ATX-LPA1 amplification. Defective MC maturation resulting from PLA2G3 deficiency is restored by supplementation with LPA1 agonists or PLA2G3-modified EVs. Thus, the lipid-orchestrated paracrine circuit involving PLA2G3-driven lysophospholipid, eicosanoid, integrin, and cytokine signaling fine-tunes MC-fibroblast communication, ensuring MC maturation.

KW - anaphylaxis

KW - fibroblast

KW - lipid mediator

KW - lysophosphatidic acid

KW - mast cell

KW - phospholipase A

KW - prostaglandin

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U2 - 10.1016/j.immuni.2024.06.012

DO - 10.1016/j.immuni.2024.06.012

M3 - Article

C2 - 39002541

AN - SCOPUS:85198582121

SN - 1074-7613

VL - 57

SP - 1828-1847.e11

JO - Immunity

JF - Immunity

IS - 8

ER -

Lipid-orchestrated paracrine circuit coordinates mast cell maturation and anaphylaxis through functional interaction with fibroblasts

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