Summary of ssbd-repos-000395

Name
URL
DOI

Title
Lung inflammation and fibrosis images of CD45-deficient mice
Description

Group 2 innate lymphoid cells (ILC2s) are critical for the immune response against parasite infection and tissue homeostasis and involved in the pathogenesis of allergy and inflammatory diseases. Although multiple molecules positively regulating ILC2 development and activation have been extensively investigated, the factors limiting their population size and response remain poorly studied. Here, we found that CD45, a membrane-bound tyrosine phosphatase essential for T-cell development, negatively regulated ILC2s in a cell-intrinsic manner. ILC2s in CD45-deficient mice exhibited enhanced proliferation and maturation in the bone marrow and hyperactivated phenotypes in the lung with high glycolytic capacity. Furthermore, CD45 signaling suppressed the type 2 inflammatory response by lung ILC2s and alleviated airway inflammation and pulmonary fibrosis. Finally, the interaction with galectin-9 influenced CD45 signaling in ILC2s. These results demonstrate that CD45 is a cell-intrinsic negative regulator of ILC2s and prevents lung inflammation and fibrosis via ILC2s.

Submited Date
2024-09-17
Release Date
2024-11-28
Updated Date
-
License
Funding information
-
File formats
TIF
Data size
114.6 MB

Organism
Mus musculus
Strain
C57BL/6
Cell Line
-
Genes
Ptprc
Proteins
CD45

GO Molecular Function (MF)
-
GO Biological Process (BP)
Inflammation
GO Cellular Component (CC)
-
Study Type
Inflammation
Imaging Methods
bright-field microscopy

Method Summary

See details in Cui, et. al. (2023) Proc Natl Acad Sci U S A.

Related paper(s)

Guangwei Cui, Akihiro Shimba, Jianshi Jin, Nozomi Hojo, Takuma Asahi, Shinya Abe, Aki Ejima, Shinri Okada, Keizo Ohira, Ryoma Kato, Shizue Tani-Ichi, Ryo Yamada, Takashi Ebihara, Katsuyuki Shiroguchi, Koichi Ikuta (2023) CD45 alleviates airway inflammation and lung fibrosis by limiting expansion and activation of ILC2s., Proceedings of the National Academy of Sciences of the United States of America, Volume 120, Number 36, pp. e2215941120

Published in 2023 Sep 5 (Electronic publication in Aug. 28, 2023, midnight )

(Abstract) Group 2 innate lymphoid cells (ILC2s) are critical for the immune response against parasite infection and tissue homeostasis and involved in the pathogenesis of allergy and inflammatory diseases. Although multiple molecules positively regulating ILC2 development and activation have been extensively investigated, the factors limiting their population size and response remain poorly studied. Here, we found that CD45, a membrane-bound tyrosine phosphatase essential for T cell development, negatively regulated ILC2s in a cell-intrinsic manner. ILC2s in CD45-deficient mice exhibited enhanced proliferation and maturation in the bone marrow and hyperactivated phenotypes in the lung with high glycolytic capacity. Furthermore, CD45 signaling suppressed the type 2 inflammatory response by lung ILC2s and alleviated airway inflammation and pulmonary fibrosis. Finally, the interaction with galectin-9 influenced CD45 signaling in ILC2s. These results demonstrate that CD45 is a cell-intrinsic negative regulator of ILC2s and prevents lung inflammation and fibrosis via ILC2s.

Contact(s)
Guangwei Cui
Organization(s)
Kyoto University , Department of Virus Research, Institute for Life and Medical Sciences , Laboratory of Immune Regulation
Image Data Contributors
Koichi Ikuta
Quantitative Data Contributors

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