Your search keyword '"Mao, Kairui"' showing total 39 results

1. Lymphatic-localized Treg-mregDC crosstalk limits antigen trafficking and restrains anti-tumor immunity

Author

You, Siyuan, Li, Shuqin, Zeng, Lingsu, Song, Jinsheng, Li, Zifeng, Li, Weiyun, Ni, Hengxiao, Xiao, Xu, Deng, Wenbo, Li, Hongye, Lin, Wenbo, Liang, Chenyu, Zheng, Yanfei, Cheng, Shih-Chin, Xiao, Nengming, Tong, Mengsha, Yu, Rongshan, Huang, Jialiang, Huang, Hongling, Xu, Hongzhi, Han, Jiahuai, Ren, Jianlin, and Mao, Kairui

Published

2024

2. The transcription factor Zeb1 controls homeostasis and function of type 1 conventional dendritic cells

Author

Wang, Yan, Zhang, Quan, He, Tingting, Wang, Yechen, Lu, Tianqi, Wang, Zengge, Wang, Yiyi, Lin, Shen, Yang, Kang, Wang, Xinming, Xie, Jun, Zhou, Ying, Hong, Yazhen, Liu, Wen-Hsien, Mao, Kairui, Cheng, Shih-Chin, Chen, Xin, Li, Qiyuan, and Xiao, Nengming

Published

2023

3. The glycolysis/HIF-1α axis defines the inflammatory role of IL-4-primed macrophages

Author

Dang, Buyun, Gao, Qingxiang, Zhang, Lishan, Zhang, Jia, Cai, Hanyi, Zhu, Yanhui, Zhong, Qiumei, Liu, Junqiao, Niu, Yujia, Mao, Kairui, Xiao, Nengming, Liu, Wen-Hsien, Lin, Shu-hai, Huang, Jialiang, Huang, Stanley Ching-Cheng, Ho, Ping-Chih, and Cheng, Shih-Chin

Published

2023

4. B cell residency but not T cell–independent IgA switching in the gut requires innate lymphoid cells

Author

Zheng, Mingzhu, Mao, Kairui, Fang, Difeng, Li, Dan, Lyu, Jun, Peng, Dingkang, Chen, Xi, Cannon, Nikki, Hu, Gangqing, Han, Jiajia, Zhao, Keji, Chen, Wanjun, and Zhu, Jinfang

Published

2021

5. S1P-dependent interorgan trafficking of group 2 innate lymphoid cells supports host defense

Author

Huang, Yuefeng, Mao, Kairui, Chen, Xi, Sun, Ming-an, Kawabe, Takeshi, Li, Weizhe, Usher, Nicholas, Zhu, Jinfang, Urban, Joseph F., Paul, William E., and Germain, Ronald N.

Published

2018

6. Transcription factor TCF-1 regulates the functions, but not the development, of lymphoid tissue inducer subsets in different tissues

Author

Zheng, Mingzhu, primary, Yao, Chen, additional, Ren, Gang, additional, Mao, Kairui, additional, Chung, Hyunwoo, additional, Chen, Xi, additional, Hu, Gangqing, additional, Wang, Lei, additional, Luan, Xuemei, additional, Fang, Difeng, additional, Li, Dan, additional, Zhong, Chao, additional, Lu, Xiaoxiao, additional, Cannon, Nikki, additional, Zhang, Mingxu, additional, Bhandoola, Avinash, additional, Zhao, Keji, additional, O’Shea, John J., additional, and Zhu, Jinfang, additional

Published

2023

7. The transcription factor Zeb1 controls homeostasis and function of type 1 conventional dendritic cells

Author

Wang, Yan, primary, zhang, quan, additional, He, Tingting, additional, Wang, Yechen, additional, Lu, Tianqi, additional, Wang, Zengge, additional, Lin, Shen, additional, Yang, Kang, additional, Wang, Xinming, additional, Xie, Jun, additional, Zhou, Ying, additional, Hong, Yazhen, additional, Liu, Wen-Hsien, additional, Mao, Kairui, additional, Cheng, Shih-Chin, additional, Chen, Xin, additional, Li, Qiyuan, additional, and Xiao, Nengming, additional

Published

2023

8. The glycolysis/HIF-1α axis defines the inflammatory role of IL-4-primed 2 macrophages

Author

Cheng, Shih-Chin, primary, Dang, Buyun, additional, Zhang, Jia, additional, Gao, Qingxiang, additional, Zhong, Qiumei, additional, Zhang, Lishan, additional, Zhu, Yanhui, additional, Liu, Junqiao, additional, Niu, Yujia, additional, Xiao, Nengming, additional, Liu, Wen-Hsien, additional, Mao, Kairui, additional, Lin, Shu-hai, additional, Huang, Jialiang, additional, Huang, Stanley, additional, and Ho, Ping-Chih, additional

Published

2022

9. Type 2 Immune Response Plays A Critical Role in Trained Immunity

Author

Cheng, Shih-Chin, primary, Dang, Buyun, additional, Zhang, Jia, additional, Gao, Qingxiang, additional, Zhong, Qiumei, additional, Zhang, Lishan, additional, Zhu, Yanhui, additional, Liu, Junqiao, additional, Niu, Yujia, additional, Xiao, Nengming, additional, Liu, Wen-Hsien, additional, Mao, Kairui, additional, Lin, Shu-hai, additional, Huang, Jialiang, additional, Huang, Stanley, additional, and Ho, Ping-Chih, additional

Published

2022

10. The Glycolysis/HIF-1α Axis Defines the Inflammatory Role of IL-4-Primed Macrophages

Author

Dang, Buyun, primary, Gao, Qingxiang, additional, Zhang, Lishan, additional, Zhang, Jia, additional, Cai, Hanyi, additional, Zhu, Yanhui, additional, Zhong, Qiumei, additional, Liu, Junqiao, additional, Niu, Yujia, additional, Mao, Kairui, additional, Xiao, Nengming, additional, Liu, Wen-Hsien, additional, Lin, Shuhai, additional, Huang, Jialiang, additional, Huang, Stanley Ching-Cheng, additional, Ho, Ping-Chih, additional, and Cheng, Shih-Chin, additional

Published

2022

11. Innate and adaptive lymphocytes sequentially shape the gut microbiota and lipid metabolism

Author

Mao, Kairui, Baptista, Antonio P., Tamoutounour, Samira, Zhuang, Lenan, Bouladoux, Nicolas, Martins, Andrew J., Huang, Yuefeng, Gerner, Michael Y., Belkaid, Yasmine, and Germain, Ronald N.

Subjects

Lymphocytes -- Physiological aspects, Microbiota (Symbiotic organisms) -- Physiological aspects, Physiological research, Lipid metabolism -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

Author(s): Kairui Mao (corresponding author) [1]; Antonio P. Baptista [1]; Samira Tamoutounour [2]; Lenan Zhuang [3]; Nicolas Bouladoux [2]; Andrew J. Martins [4]; Yuefeng Huang [5]; Michael Y. Gerner [6]; [...]

Published

2018

12. Cellular localization of NLRP3 inflammasome

Author

Wang, Yan, Yang, Chen, Mao, Kairui, Chen, Shuzhen, Meng, Guangxun, and Sun, Bing

Published

2013

13. Correction: β-arrestin1 Is Critical for the Full Activation of NLRP3 and NLRC4 Inflammasomes

Author

Mao, Kairui, primary, Chen, Shuzhen, additional, Wang, Yan, additional, Zeng, Yan, additional, Ma, Yonglei, additional, Hu, Yu, additional, Zhang, Hong, additional, Sun, Shuhui, additional, Wu, Xiaodong, additional, Meng, Guangxun, additional, Pei, Gang, additional, and Sun, Bing, additional

Published

2020

14. B cell recruitment to the intestine critically depends on GATA3- and RORgt-mediated development of NKp46 negative innate lymphoid cells

Author

Zheng, Mingzhu, primary, Mao, Kairui, additional, Li, Dan, additional, Fang, Difeng, additional, Lyu, Jun, additional, and Zhu, Jinfang (Jeff), additional

Published

2019

15. T-bet expression is fine-tuned for balancing IFN-γ-producing Th1 and Tfh cell differentiation and IgG2a(c) production

Author

Fang, Difeng, primary, Zheng, Mingzhu, additional, Mao, Kairui, additional, Reiner, Steven L, additional, Sher, Alan, additional, and Zhu, Jinfang (Jeff), additional

Published

2019

16. Thinking differently about ILCs-Not just tissue resident and not just the same as CD4+ T-cell effectors

Author

Huang, Yuefeng, primary, Mao, Kairui, additional, and Germain, Ronald N., additional

Published

2018

17. Transient T-bet expression functionally specifies a distinct T follicular helper subset

Author

Fang, Difeng, primary, Cui, Kairong, additional, Mao, Kairui, additional, Hu, Gangqing, additional, Li, Rao, additional, Zheng, Mingzhu, additional, Riteau, Nicolas, additional, Reiner, Steven L., additional, Sher, Alan, additional, Zhao, Keji, additional, and Zhu, Jinfang, additional

Published

2018

18. Sequential activity of innate and adaptive lymphocytes supports non-inflammatory gut microbial commensalism

Author

Mao, Kairui, primary, Baptista, Antonio, additional, Bouladoux, Nicolas, additional, Martins, Andrew J, additional, Tamoutounour, Samira, additional, Davis, Jacquice, additional, Huang, Yuefeng, additional, Gerner, Michael Y., additional, Belkaid, Yasmine, additional, and Germain, Ronald N, additional

Published

2017

19. Inflammatory ILC2: An IL-25-activated circulating ILC population with a protective role during helminthic infection

Author

Huang, Yuefeng, primary, Mao, Kairui, additional, Chen, Xi, additional, Kawabe, Takeshi, additional, Li, Weizhe, additional, Zhu, Jinfang (Jeff), additional, Urban, Joseph F., additional, Germain, Ronald N, additional, and Paul, William E, additional

Published

2017

20. Group 3 innate lymphoid cells continuously require the transcription factor GATA-3 after commitment

Author

Zhong, Chao, primary, Cui, Kairong, additional, Wilhelm, Christoph, additional, Hu, Gangqing, additional, Mao, Kairui, additional, Belkaid, Yasmine, additional, Zhao, Keji, additional, and Zhu, Jinfang, additional

Published

2016

21. Erratum: Group 3 innate lymphoid cells continuously require the transcription factor GATA-3 after commitment

Author

Zhong, Chao, primary, Cui, Kairong, additional, Wilhelm, Christoph, additional, Hu, Gangqing, additional, Mao, Kairui, additional, Belkaid, Yasmine, additional, Zhao, Keji, additional, and Zhu, Jinfang, additional

Published

2016

22. Thinking differently about ILCs—Not just tissue resident and not just the same as CD4+ T‐cell effectors.

Author

Huang, Yuefeng, Mao, Kairui, and Germain, Ronald N.

Subjects

*TUMOR immunology, *CD4 antigen, *T cells, *TRANSCRIPTION factors, *CYTOKINES, *CELLULAR signal transduction, *TUMOR microenvironment, *PHYSIOLOGY

Abstract

Abstract: Innate lymphoid cells (ILCs) resemble adaptive T lymphocytes based on transcription factor expression, cytokine production, and their presumptive roles in immunity, but are activated for effector function through cytokine signaling and not antigen‐specific receptors. The prevailing view is that ILCs adapt to specific microenvironments during development and operate as tissue‐resident cells in co‐operation with antigen‐specific T cells to provide host protection and contribute to tissue maintenance. In particular, conventional models equate the activity of different ILC subsets with CD4+ effector T‐cell types based on corresponding transcription factor expression and a potential for comparable cytokine production. Based on recent data from our laboratory, we suggest that these views on tissue residence and parallel functioning to CD4+ T cells are too restrictive. Our findings show that ILC2s can be mobilized from the gut under inflammatory conditions and contribute to distal immunity in the lungs during infection, whereas gut‐resident ILC3s operate in a quite distinct manner from Th17 CD4+ effector cells in responding to commensal microbes, with important implications for control of metabolic homeostasis. In this review, we discuss the recent advances leading to these revised views of ILC inter‐organ trafficking and the distinct and complementary function of ILCs with respect to adaptive T cells in establishing and maintaining a physiologic host environment. [ABSTRACT FROM AUTHOR]

Published

2018

23. Group 3 innate lymphoid cells continuously require the transcription factor GATA-3 after commitment

Author

Zhong, Chao, primary, Cui, Kairong, additional, Wilhelm, Christoph, additional, Hu, Gangqing, additional, Mao, Kairui, additional, Belkaid, Yasmine, additional, Zhao, Keji, additional, and Zhu, Jinfang, additional

Published

2015

24. β-arrestin1 Is Critical for the Full Activation of NLRP3 and NLRC4 Inflammasomes

Author

Mao, Kairui, primary, Chen, Shuzhen, additional, Wang, Yan, additional, Zeng, Yan, additional, Ma, Yonglei, additional, Hu, Yu, additional, Zhang, Hong, additional, Sun, Shuhui, additional, Wu, Xiaodong, additional, Meng, Guangxun, additional, Pei, Gang, additional, and Sun, Bing, additional

Published

2015

25. Negative Regulation of Nmi on Virus-Triggered Type I IFN Production by Targeting IRF7

Author

Wang, Jie, primary, Yang, Bo, additional, Hu, Yu, additional, Zheng, Yuhan, additional, Zhou, Haiyan, additional, Wang, Yanming, additional, Ma, Yonglei, additional, Mao, Kairui, additional, Yang, Leilei, additional, Lin, Guomei, additional, Ji, Yongyong, additional, Wu, Xiaodong, additional, and Sun, Bing, additional

Published

2013

26. Nitric oxide suppresses NLRP3 inflammasome activation and protects against LPS-induced septic shock

Author

Mao, Kairui, primary, Chen, Shuzhen, additional, Chen, Mingkuan, additional, Ma, Yonglei, additional, Wang, Yan, additional, Huang, Bo, additional, He, Zhengyu, additional, Zeng, Yan, additional, Hu, Yu, additional, Sun, Shuhui, additional, Li, Jing, additional, Wu, Xiaodong, additional, Wang, Xiangrui, additional, Strober, Warren, additional, Chen, Chang, additional, Meng, Guangxun, additional, and Sun, Bing, additional

Published

2013

27. ECM1 controls TH2 cell egress from lymph nodes through re-expression of S1P1

Author

Li, Zhenhu, primary, Zhang, Yuan, additional, Liu, Zhiduo, additional, Wu, Xiaodong, additional, Zheng, Yuhan, additional, Tao, Zhiyun, additional, Mao, Kairui, additional, Wang, Jie, additional, Lin, Guomei, additional, Tian, Lin, additional, Ji, Yongyong, additional, Qin, Meiling, additional, Sun, Shuhui, additional, Zhu, Xueliang, additional, and Sun, Bing, additional

Published

2011

28. Tripartite-Motif Protein 30 Negatively Regulates NLRP3 Inflammasome Activation by Modulating Reactive Oxygen Species Production

Author

Hu, Yu, primary, Mao, Kairui, additional, Zeng, Yan, additional, Chen, Shuzhen, additional, Tao, Zhiyun, additional, Yang, Chen, additional, Sun, Shuhui, additional, Wu, Xiaodong, additional, Meng, Guangxun, additional, and Sun, Bing, additional

Published

2010

29. In Vivo Disruption of TGF-β Signaling by Smad7 in Airway Epithelium Alleviates Allergic Asthma but Aggravates Lung Carcinogenesis in Mouse

Author

Luo, Xiaolin, primary, Ding, Qiurong, additional, Wang, Min, additional, Li, Zhigang, additional, Mao, Kairui, additional, Sun, Bing, additional, Pan, Yi, additional, Wang, Zhenzhen, additional, Zang, Ying Qin, additional, and Chen, Yan, additional

Published

2010

30. Dec2 Promotes Th2 Cell Differentiation by Enhancing IL-2R Signaling

Author

Liu, Zhiduo, primary, Li, Zhenhu, additional, Mao, Kairui, additional, Zou, Jia, additional, Wang, Yuan, additional, Tao, Zhiyun, additional, Lin, Guomei, additional, Tian, Lin, additional, Ji, Yongyong, additional, Wu, Xiaodong, additional, Zhu, Xueliang, additional, Sun, Shuhui, additional, Chen, Weiguang, additional, Xiang, Charlie, additional, and Sun, Bing, additional

Published

2009

31. Trichosanthin functions as Th2-type adjuvant in induction of allergic airway inflammation

Author

Wang, Yuan, primary, Mao, Kairui, additional, Sun, Shuhui, additional, Lin, Guomei, additional, Wu, Xiaodong, additional, Yao, Gang, additional, and Sun, Bing, additional

Published

2009

32. Novel function of perforin in negatively regulating CD4+ T cell activation by affecting calcium signaling

Author

Bi, Enguang, primary, Huang, Chunjian, additional, Hu, Yu, additional, Wu, Xiaodong, additional, Deng, Weiwen, additional, Lin, Guomei, additional, Liu, Zhiduo, additional, Tian, Lin, additional, Sun, Shuhui, additional, Mao, Kairui, additional, Zou, Jia, additional, Zheng, Yuhan, additional, and Sun, Bing, additional

Published

2009

33. TRIM30α negatively regulates TLR-mediated NF-κB activation by targeting TAB2 and TAB3 for degradation

Author

Shi, Mude, primary, Deng, Weiwen, additional, Bi, Enguang, additional, Mao, Kairui, additional, Ji, Yongyong, additional, Lin, Guomei, additional, Wu, Xiaodong, additional, Tao, Zhiyun, additional, Li, Zhenhu, additional, Cai, Xinfen, additional, Sun, Shuhui, additional, Xiang, Charlie, additional, and Sun, Bing, additional

Published

2008

34. Group 3 innate lymphoid cells continuously require the transcription factor GATA-3 after commitment

Author

Zhong, Chao, Cui, Kairong, Wilhelm, Christoph, Hu, Gangqing, Mao, Kairui, Belkaid, Yasmine, Zhao, Keji, and Zhu, Jinfang

Abstract

The transcription factor GATA-3 is indispensable for the development of all innate lymphoid cells (ILCs) that express the interleukin 7 receptor α-chain (IL-7Rα). However, the function of low GATA-3 expression in committed group 3 ILCs (ILC3 cells) has not been identified. We found that GATA-3 regulated the homeostasis of ILC3 cells by controlling IL-7Rα expression. In addition, GATA-3 served a critical function in the development of the NKp46+ILC3 subset by regulating the balance between the transcription factors T-bet and RORγt. Among NKp46+ILC3 cells, although GATA-3 positively regulated genes specific to the NKp46+ILC3 subset, it negatively regulated genes specific to lymphoid tissue–inducer (LTi) or LTi-like ILC3 cells. Furthermore, GATA-3 was required for IL-22 production in both ILC3 subsets. Thus, despite its low expression, GATA-3 was critical for the homeostasis, development and function of ILC3 subsets.

Published

2016

35. ECM1 controls TH2 cell egress from lymph nodes through re-expression of S1P1.

Author

Li, Zhenhu, Zhang, Yuan, Liu, Zhiduo, Wu, Xiaodong, Zheng, Yuhan, Tao, Zhiyun, Mao, Kairui, Wang, Jie, Lin, Guomei, Tian, Lin, Ji, Yongyong, Qin, Meiling, Sun, Shuhui, Zhu, Xueliang, and Sun, Bing

Subjects

EXTRACELLULAR matrix proteins, TH2 cells, ALLERGIES, ASTHMA, AIRWAY (Anatomy), FUNCTIONAL analysis, LYMPH node diseases

Abstract

Type 2 helper T cells (TH2) are critically involved in allergies and asthma. Here we demonstrate that extracellular matrix protein-1 (ECM1) is highly and selectively expressed in TH2 cells. ECM1 deficiency caused impaired TH2 responses and reduced allergic airway inflammation in vivo. Functional analysis demonstrated that although the TH2 polarization of ECM1-deficient cells was unimpaired, these cells had a defect in migration and were retained in peripheral lymphoid organs. This was associated with reduced expression of KLF2 and S1P1. We also found that ECM1 could directly bind the interleukin-2 (IL-2) receptor to inhibit IL-2 signaling and activate S1P1 expression. Our data identify a previously unknown function of ECM1 in regulating TH2 cell migration through control of KLF2 and S1P1 expression. [ABSTRACT FROM AUTHOR]

Published

2011

36. ECM1 controls TH2 cell egress from lymph nodes through re-expression of S1P1.

Author

Li, Zhenhu, Zhang, Yuan, Liu, Zhiduo, Wu, Xiaodong, Zheng, Yuhan, Tao, Zhiyun, Mao, Kairui, Wang, Jie, Lin, Guomei, Tian, Lin, Ji, Yongyong, Qin, Meiling, Sun, Shuhui, Zhu, Xueliang, and Sun, Bing

Subjects

*EXTRACELLULAR matrix proteins, *TH2 cells, *ALLERGIES, *ASTHMA, *AIRWAY (Anatomy), *FUNCTIONAL analysis, *LYMPH node diseases

Abstract

Type 2 helper T cells (TH2) are critically involved in allergies and asthma. Here we demonstrate that extracellular matrix protein-1 (ECM1) is highly and selectively expressed in TH2 cells. ECM1 deficiency caused impaired TH2 responses and reduced allergic airway inflammation in vivo. Functional analysis demonstrated that although the TH2 polarization of ECM1-deficient cells was unimpaired, these cells had a defect in migration and were retained in peripheral lymphoid organs. This was associated with reduced expression of KLF2 and S1P1. We also found that ECM1 could directly bind the interleukin-2 (IL-2) receptor to inhibit IL-2 signaling and activate S1P1 expression. Our data identify a previously unknown function of ECM1 in regulating TH2 cell migration through control of KLF2 and S1P1 expression. [ABSTRACT FROM AUTHOR]

Published

2011

37. Progranulin-dependent repair function of Regulatory T cells drive bone fracture healing.

Author

Chen R, Zhang X, Li B, Tonetti MS, Yang Y, Li Y, Liu B, Qian S, Gu Y, Wang Q, Mao K, Cheng H, Lai H, and Shi J

Abstract

Local immunoinflammatory events instruct skeletal stem cells (SSCs) to repair/regenerate bone after injury, but mechanisms are incompletely understood. We hypothesized that specialized Regulatory T (Treg) cells are necessary for bone repair and interact directly with SSCs through organ-specific messages. Both in human patients with bone fracture and mouse model of bone injury, we identified a bone injury-responding Treg subpopulation with bone-repair capacity marked by CCR8. Local production of CCL1 induced a massive migration of CCR8+ Treg cells from periphery to the injury site. Depending on secretion of progranulin (PGRN), a protein encoded by the granulin (Grn) gene, CCR8+ Treg cells supported the accumulation and osteogenic differentiation of SSCs, and thereby bone repair. Mechanistically, we revealed that CCL1 enhanced expression level of basic leucine zipper ATF-like transcription factor (BATF) in CCR8+ Treg cells, which bound to Grn promoter and increased Grn translational output and then PGRN secretion. Together, our work provides a new perspective in osteoimmunology and highlights possible ways of manipulating Treg cell signaling to enhance bone repair and regeneration.

Published

2024

38. In vivo disruption of TGF-beta signaling by Smad7 in airway epithelium alleviates allergic asthma but aggravates lung carcinogenesis in mouse.

Author

Luo X, Ding Q, Wang M, Li Z, Mao K, Sun B, Pan Y, Wang Z, Zang YQ, and Chen Y

Subjects

Animals, Asthma chemically induced, Asthma therapy, Cytokines analysis, Disease Models, Animal, Genetic Therapy, Inflammation prevention & control, Lung Neoplasms chemically induced, Lung Neoplasms therapy, Mice, Mice, Transgenic, Ovalbumin, Smad7 Protein genetics, Th2 Cells, Transforming Growth Factor beta antagonists & inhibitors, Urethane, Asthma etiology, Lung Neoplasms etiology, Respiratory Mucosa metabolism, Signal Transduction drug effects, Smad7 Protein pharmacology, Transforming Growth Factor beta physiology

Abstract

Background: TGF-beta has been postulated to play an important role in the maintenance of epithelial homeostasis and the development of epithelium-derived cancers. However, most of previous studies are mainly focused on the function of TGF-beta in immune cells to the development of allergic asthma and how TGF-beta signaling in airway epithelium itself in allergic inflammation is largely unknown. Furthermore, the in vivo TGF-beta function specifically in the airway epithelium during lung cancer development has been largely elusive., Methodology/principal Findings: To evaluate the in vivo contribution of TGF-beta signaling in lung epithelium to the development of allergic disease and lung cancer, we generated a transgenic mouse model with Smad7, an intracellular inhibitor of TGF-beta signaling, constitutively expressed in mouse airway Clara cells using a mouse CC10 promoter. The mice were subjected to the development of OVA-induced allergic asthma and urethane-induced lung cancer. The Smad7 transgenic animals significantly protected from OVA-induced asthma, with reduced airway inflammation, airway mucus production, extracellular matrix deposition, and production of OVA-specific IgE. Further analysis of cytokine profiles in lung homogenates revealed that the Th2 cytokines including IL-4, IL-5 and IL-13, as well as other cytokines including IL-17, IL-1, IL-6, IP10, G-CSF, and GM-CSF were significantly reduced in the transgenic mice upon OVA induction. In contrast, the Smad7 transgenic animals had an increased incidence of lung carcinogenesis when subjected to urethane treatment., Conclusion/significance: These studies, therefore, demonstrate for the first time the in vivo function of TGF-beta signaling specifically in airway epithelium during the development of allergic asthma and lung cancer.

Published

2010

39. TRIM30 alpha negatively regulates TLR-mediated NF-kappa B activation by targeting TAB2 and TAB3 for degradation.

Author

Shi M, Deng W, Bi E, Mao K, Ji Y, Lin G, Wu X, Tao Z, Li Z, Cai X, Sun S, Xiang C, and Sun B

Subjects

Animals, Cell Line, Feedback, Physiological immunology, Female, HeLa Cells, Humans, Intracellular Signaling Peptides and Proteins metabolism, MAP Kinase Kinase Kinases metabolism, Mice, Mice, Inbred C57BL, Mice, Transgenic, NF-kappa B antagonists & inhibitors, Toll-Like Receptors agonists, Toll-Like Receptors antagonists & inhibitors, Adaptor Proteins, Signal Transducing metabolism, Intracellular Signaling Peptides and Proteins physiology, NF-kappa B metabolism, Toll-Like Receptors physiology

Abstract

Toll-like receptor (TLR) signaling is pivotal to innate and adaptive immune responses and must be tightly controlled. The mechanisms of TLR signaling have been the focus of extensive studies. Here we report that the tripartite-motif protein TRIM30alpha, a RING protein, was induced by TLR agonists and interacted with the TAB2-TAB3-TAK1 adaptor-kinase complex involved in the activation of transcription factor NF-kappaB. TRIM30alpha promoted the degradation of TAB2 and TAB3 and inhibited NF-kappaB activation induced by TLR signaling. In vivo studies showed that transfected or transgenic mice overexpressing TRIM30alpha were more resistant to endotoxic shock. Consistent with that, in vivo 'knockdown' of TRIM30alpha mRNA by small interfering RNA impaired lipopolysaccharide-induced tolerance. Finally, expression of TRIM30alpha depended on NF-kappaB activation. Our results collectively indicate that TRIM30alpha negatively regulates TLR-mediated NF-kappaB activation by targeting degradation of TAB2 and TAB3 by a 'feedback' mechanism.

Published

2008