Your search keyword '"Asao, Atsuko"' showing total 7 results

1. The adaptor TRAF5 limits the differentiation of inflammatory CD4+ T cells by antagonizing signaling via the receptor for IL-6.

Author

Nagashima, Hiroyuki, Okuyama, Yuko, Asao, Atsuko, Kawabe, Takeshi, Yamaki, Satoshi, Nakano, Hiroyasu, Croft, Michael, Ishii, Naoto, and So, Takanori

Subjects

*T cell differentiation, *ADAPTOR proteins, *CD4 antigen, *INTERLEUKIN-6, *TUMOR necrosis factor receptors, *T helper cells, *STAT proteins

Abstract

The physiological functions of members of the tumor-necrosis factor (TNF) receptor (TNFR)-associated factor (TRAF) family in T cell immunity are not well understood. We found that in the presence of interleukin 6 (IL-6), naive TRAF5-deficient CD4+ T cells showed an enhanced ability to differentiate into the TH17 subset of helper T cells. Accordingly, TH17 cell-associated experimental autoimmune encephalomyelitis (EAE) was greatly exaggerated in Traf5−/− mice. Although it is normally linked with TNFR signaling pathways, TRAF5 constitutively associated with a cytoplasmic region in the signal-transducing receptor gp130 that overlaps with the binding site for the transcription activator STAT3 and suppressed the recruitment and activation of STAT3 in response to IL-6. Our results identify TRAF5 as a negative regulator of the IL-6 receptor signaling pathway that limits the induction of proinflammatory CD4+ T cells that require IL-6 for their development. [ABSTRACT FROM AUTHOR]

Published

2014

2. Fatty acid‐binding protein 3 controls contact hypersensitivity through regulating skin dermal Vγ4+ γ/δ T cell in a murine model.

Author

Kobayashi, Shuhei, Phung, Hai The, Kagawa, Yoshiteru, Miyazaki, Hirofumi, Takahashi, Yu, Asao, Atsuko, Maruyama, Takashi, Yoshimura, Akihiko, Ishii, Naoto, and Owada, Yuji

Subjects

*FATTY acid-binding proteins, *CONTACT dermatitis, *T cells, *UNSATURATED fatty acids, *SKIN inflammation

Abstract

Background: Fatty acid‐binding protein 3 (FABP3) is a cytosolic carrier protein of polyunsaturated fatty acids (PUFAs) and regulates cellular metabolism. However, the physiological functions of FABP3 in immune cells and how FABP3 regulates inflammatory responses remain unclear. Methods: Contact hypersensitivity (CHS) induced by 2,4‐dinitrofluorobenzene (DNFB) and fluorescein isothiocyanate was applied to the skin wild‐type and Fabp3−/− mice. Skin inflammation was assessed using FACS, histological, and qPCR analyses. The development of γ/δ T cells was evaluated by a co‐culture system with OP9/Dll1 cells in the presence or absence of transgene of FABP3. Results: Fabp3‐deficient mice exhibit a more severe phenotype of contact hypersensitivity (CHS) accompanied by infiltration of IL‐17‐producing Vγ4+ γ/δ T cells that critically control skin inflammation. In Fabp3−/− mice, we found a larger proportion of Vγ4+ γ/δ T cells in the skin, even though the percentage of total γ/δ T cells did not change at steady state. Similarly, juvenile Fabp3−/− mice also contained a higher amount of Vγ4+ γ/δ T cells not only in the skin but in the thymus when compared with wild‐type mice. Furthermore, thymic double‐negative (DN) cells expressed FABP3, and FABP3 negatively regulates the development of Vγ4+ γ/δ T cells in the thymus. Conclusions: These findings suggest that FABP3 functions as a negative regulator of skin inflammation through limiting pathogenic Vγ4+ γ/δ T‐cell generation in the thymus. [ABSTRACT FROM AUTHOR]

Published

2021

3. GITR controls intestinal inflammation by suppressing IL‐15‐dependent NK cell activity.

Author

Sakurai, Tsuyoshi, Okuyama, Yuko, Kobayashi, Shuhei, Phung, Hai The, Asao, Atsuko, Kawabe, Takeshi, Ndhlovu, Lishomwa C., Riccardi, Carlo, Kudo, Hironori, Wada, Motoshi, Nio, Masaki, So, Takanori, and Ishii, Naoto

Abstract

Glucocorticoid‐induced TNFR family related gene (GITR) is a member of the TNFR superfamily that is expressed on cells of the immune system. Although the protective and pathogenic roles of GITR in T cell immunity are well characterized, the role of GITR in innate immunity in the intestinal tissues has not been well clarified. In this study, using a dextran sulfate sodium (DSS)‐induced colitis model in mice, we found that GITR‐deficiency rendered mice more susceptible to acute intestinal inflammation and that a significantly higher number of activated natural killer (NK) cells was accumulated in the colonic lamina propria of Gitr−/− mice as compared to wild‐type mice. Additionally, Rag2−/−Gitr−/− mice, which lack T cells but have NK cells, also displayed more severe colonic inflammation than Rag2−/− mice. In contrast, an anti‐GITR agonistic antibody significantly alleviated colitis in Rag2−/− mice. Engagement of GITR inhibited IL‐15‐mediated activating signaling events in NK cells, which include cell activation and proliferation, and production of cytokines and cytotoxic granules. Taken together, our results provide the first evidence that GITR negatively controls intestinal inflammation through NK cell functions. [ABSTRACT FROM AUTHOR]

Published

2020

4. IQ motif-containing GTPase-activating protein 1 is essential for the optimal maintenance of lung ILC2s.

Author

Tayama, Shunichi, Okuyama, Yuko, Phung, Hai The, Asao, Atsuko, Kobayashi, Shuhei, Musha, Tomomi, Machiyama, Tomoaki, Sakurai, Tsuyoshi, Zhang, Chengming, Ushio-Fukai, Masuko, Kawabe, Takeshi, So, Takanori, and Ishii, Naoto

Subjects

*GTPASE-activating protein, *INNATE lymphoid cells, *SCAFFOLD proteins, *LUNGS, *APOPTOSIS

Abstract

Group 2 innate lymphoid cells (ILC2s) play critical roles in type 2 immunity and are crucial for pathogenesis of various types of inflammatory disease. IQ motif-containing GTPase-activating protein 1 (IQGAP1) is a ubiquitously expressed scaffold protein that is involved in multiple cellular functions such as cell survival and trafficking. While the roles for IQGAP1 in T and B lymphocytes have been uncovered, the physiological significance of IQGAP1 in innate lymphocytes remains to be elucidated. In the current study, we demonstrate that using bone marrow chimeras, the deficiency of IQGAP1 caused an impaired survival of lung ILC2s in a cell-intrinsic manner and that Iqgap1 −/− mice displayed decreased accumulation of ILC2s after administration of papain and thereby reduced the pathology of the disease. Moreover, Iqgap1 −/− ILC2s showed a significantly enhanced apoptosis as compared to wild-type ILC2s under both steady-state and inflammatory conditions. Together these results identify for the first time that IQGAP1 is essential for homeostasis of ILC2s in the lung. [ABSTRACT FROM AUTHOR]

Published

2020

5. TNF receptor associated factor 5 controls oncostatin M-mediated lung inflammation.

Author

Machiyama, Tomoaki, So, Takanori, Okuyama, Yuko, Kobayashi, Shuhei, Phung, Hai The, Asao, Atsuko, Harigae, Hideo, and Ishii, Naoto

Subjects

*TUMOR necrosis factor receptors, *ONCOSTATIN M, *PNEUMONIA, *PULMONARY fibrosis, *ENDOTHELIAL cells

Abstract

Oncostatin M (OSM) is involved in pathogenesis of several human inflammatory diseases including lung inflammation and fibrosis. Although accumulating evidence indicates that OSM mediates lung inflammation, the precise mechanism for OSM on lung inflammation still remains unclear. In this study, we found that OSM receptor was abundantly expressed on endothelial and stromal/fibroblast cells in the lung of mice. In vitro stimulation with OSM upregulated vascular cell adhesion molecule-1 (VCAM-1), which promotes eosinophil infiltration in the lung tissues, on freshly-isolated lung stromal/fibroblast cells from wild-type mice. However, these cells from TNF receptor associated factor 5 (TRAF5)-deficient mice failed to show the increase in VCAM-1 expression after OSM stimulation. Furthermore, Traf5 −/− mice showed markedly attenuated lung inflammation in terms of eosinophil infiltration upon intranasal administration with OSM as compared to wild-type mice. These results indicate that TRAF5 is crucially involved in OSM-mediated lung inflammation probably by inducing lung stromal/fibroblast cell activation. [ABSTRACT FROM AUTHOR]

Published

2018

6. Gene Therapy Model of X-linked Severe Combined Immunodeficiency Using a Modified Foamy Virus Vector.

Author

Horino, Satoshi, Uchiyama, Toru, So, Takanori, Nagashima, Hiroyuki, Sun, Shu-lan, Sato, Miki, Asao, Atsuko, Haji, Yoichi, Sasahara, Yoji, Candotti, Fabio, Tsuchiya, Shigeru, Kure, Shigeo, Sugamura, Kazuo, and Ishii, Naoto

Subjects

*IMMUNOLOGICAL deficiency syndrome treatment, *GENE therapy, *FOAMY viruses, *MICROBIAL mutation, *CYTOKINE receptors, *KILLER cells, *HUMAN genetics

Abstract

X-linked severe combined immunodeficiency (SCID-X1) is an inherited genetic immunodeficiency associated with mutations in the common cytokine receptor γ chain (γc) gene, and characterized by a complete defect of T and natural killer (NK) cells. Gene therapy for SCID-X1 using conventional retroviral (RV) vectors carrying the γc gene results in the successful reconstitution of T cell immunity. However, the high incidence of vector-mediated T cell leukemia, caused by vector insertion near or within cancer-related genes has been a serious problem. In this study, we established a gene therapy model of mouse SCID-X1 using a modified foamy virus (FV) vector expressing human γc. Analysis of vector integration in a human T cell line demonstrated that the FV vector integration sites were significantly less likely to be located within or near transcriptional start sites than RV vector integration sites. To evaluate the therapeutic efficacy, bone marrow cells from γc-knockout (γc-KO) mice were infected with the FV vector and transplanted into γc-KO mice. Transplantation of the FV-treated cells resulted in the successful reconstitution of functionally active T and B cells. These data suggest that FV vectors can be effective and may be safer than conventional RV vectors for gene therapy for SCID-X1. [ABSTRACT FROM AUTHOR]

Published

2013

7. Germ-Free Conditions Modulate Host Purine Metabolism, Exacerbating Adenine-Induced Kidney Damage.

Author

Mishima, Eikan, Ichijo, Mariko, Kawabe, Takeshi, Kikuchi, Koichi, Akiyama, Yukako, Toyohara, Takafumi, Suzuki, Takehiro, Suzuki, Chitose, Asao, Atsuko, Ishii, Naoto, Fukuda, Shinji, and Abe, Takaaki

Subjects

*ADENINE, *KIDNEYS, *METABOLISM

Abstract

Alterations in microbiota are known to affect kidney disease conditions. We have previously shown that germ-free conditions exacerbated adenine-induced kidney damage in mice; however, the mechanism by which this occurs has not been elucidated. To explore this mechanism, we examined the influence of germ-free conditions on purine metabolism and renal immune responses involved in the kidney damage. Germ-free mice showed higher expression levels of purine-metabolizing enzymes such as xanthine dehydrogenase, which converts adenine to a nephrotoxic byproduct 2,8-dihydroxyadenine (2,8-DHA). The germ-free mice also showed increased urinary excretion of allantoin, indicating enhanced purine metabolism. Metabolome analysis demonstrated marked differences in the purine metabolite levels in the feces of germ-free mice and mice with microbiota. Furthermore, unlike the germ-free condition, antibiotic treatment did not increase the expression of purine-metabolizing enzymes or exacerbate adenine-induced kidney damage. Considering renal immune responses, the germ-free mice displayed an absence of renal IL-17A expression. However, the adenine-induced kidney damage in wild-type mice was comparable to that in IL-17A-deficient mice, suggesting that IL-17A does not play a major role in the disease condition. Our results suggest that the enhanced host purine metabolism in the germ-free mice potentially promotes the conversion of the administered adenine into 2,8-DHA, resulting in exacerbated kidney damage. This further suggests a role of the microbiota in regulating host purine metabolism. [ABSTRACT FROM AUTHOR]

Published

2020