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34 results on '"Herjan, Tomasz"'

1. IL-17A Recruits Rab35 to IL-17R to Mediate PKCα-Dependent Stress Fiber Formation and Airway Smooth Muscle Contractility

Author

Bulek, Katarzyna, Chen, Xing, Parron, Vandy, Sundaram, Aparna, Herjan, Tomasz, Ouyang, Suidong, Liu, Caini, Majors, Alana, Zepp, Jarod, Gao, Ji, Dongre, Ashok, Bodaszewska-Lubas, Malgorzata, Echard, Arnaud, Aronica, Mark, Carman, Julie, Garantziotis, Stavros, Sheppard, Dean, and Li, Xiaoxia

Subjects
Lung, Asthma, Aetiology, 2.1 Biological and endogenous factors, Respiratory, Animals, Interleukin-17, Mice, Mice, Knockout, Muscle Contraction, Muscle, Smooth, Protein Kinase C-alpha, Protein Kinase Inhibitors, Receptors, Interleukin-17, Stress Fibers, rab GTP-Binding Proteins, Immunology
Abstract

IL-17A is a critical proinflammatory cytokine for the pathogenesis of asthma including neutrophilic pulmonary inflammation and airway hyperresponsiveness. In this study, by cell type-specific deletion of IL-17R and adaptor Act1, we demonstrated that IL-17R/Act1 exerts a direct impact on the contraction of airway smooth muscle cells (ASMCs). Mechanistically, IL-17A induced the recruitment of Rab35 (a small monomeric GTPase) and DennD1C (guanine nucleotide exchange factor [GEF]) to the IL-17R/Act1 complex in ASMCs, resulting in activation of Rab35. Rab35 knockdown showed that IL-17A-induced Rab35 activation was essential for protein kinase Cα (PKCα) activation and phosphorylation of fascin at Ser39 in ASMCs, allowing F-actin to interact with myosin to form stress fibers and enhance the contraction induced by methacholine. PKCα inhibitor or Rab35 knockdown indeed substantially reduced IL-17A-induced stress fiber formation in ASMCs and attenuated IL-17A-enhanced, methacholine-induced contraction of airway smooth muscle. Taken together, these data indicate that IL-17A promotes airway smooth muscle contraction via direct recruitment of Rab35 to IL-17R, followed by PKCα activation and stress fiber formation.

Published
2019

3. IRAK2 directs stimulus-dependent nuclear export of inflammatory mRNAs

Author

Zhou, Hao, Bulek, Katarzyna, Li, Xiao, Herjan, Tomasz, Yu, Minjia, Qian, Wen, Wang, Han, Zhou, Gao, Chen, Xing, Yang, Hui, Hong, Lingzi, Zhao, Junjie, Qin, Luke, Fukuda, Koichi, Flotho, Annette, Gao, Ji, Dongre, Ashok, Carman, Julie A, Kang, Zizhen, Su, Bing, Kern, Timothy S, Smith, Jonathan D, Hamilton, Thomas A, Melchior, Frauke, Fox, Paul L, and Li, Xiaoxia

Subjects
Genetics, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, Active Transport, Cell Nucleus, Animals, Interleukin-1 Receptor-Associated Kinases, Lipopolysaccharides, Macrophages, Mice, Nucleocytoplasmic Transport Proteins, Phosphorylation, RNA, Messenger, RNA-Binding Proteins, Serine-Arginine Splicing Factors, Sumoylation, RNA export, cell biology, immunology, inflammation, mouse, nuclear translocation, sumoylation, toll-like receptor, Biochemistry and Cell Biology
Abstract

Expression of inflammatory genes is determined in part by post-transcriptional regulation of mRNA metabolism but how stimulus- and transcript-dependent nuclear export influence is poorly understood. Here, we report a novel pathway in which LPS/TLR4 engagement promotes nuclear localization of IRAK2 to facilitate nuclear export of a specific subset of inflammation-related mRNAs for translation in murine macrophages. IRAK2 kinase activity is required for LPS-induced RanBP2-mediated IRAK2 sumoylation and subsequent nuclear translocation. Array analysis showed that an SRSF1-binding motif is enriched in mRNAs dependent on IRAK2 for nuclear export. Nuclear IRAK2 phosphorylates SRSF1 to reduce its binding to target mRNAs, which promotes the RNA binding of the nuclear export adaptor ALYREF and nuclear export receptor Nxf1 loading for the export of the mRNAs. In summary, LPS activates a nuclear function of IRAK2 that facilitates the assembly of nuclear export machinery to export selected inflammatory mRNAs to the cytoplasm for translation.

Published
2017

4. IKKα negatively regulates ASC-dependent inflammasome activation.

Author

Martin, Bradley N, Wang, Chenhui, Willette-Brown, Jami, Herjan, Tomasz, Gulen, Muhammet F, Zhou, Hao, Bulek, Katarzyna, Franchi, Luigi, Sato, Takashi, Alnemri, Emad S, Narla, Goutham, Zhong, Xiao-Ping, Thomas, James, Klinman, Dennis, Fitzgerald, Katherine A, Karin, Michael, Nuñez, Gabriel, Dubyak, George, Hu, Yinling, and Li, Xiaoxia

Subjects
Macrophages, Animals, Mice, Knockout, Mice, Carrier Proteins, Down-Regulation, Protein Transport, Female, Male, Apoptosis Regulatory Proteins, I-kappa B Kinase, CARD Signaling Adaptor Proteins, Inflammasomes, NLR Family, Pyrin Domain-Containing 3 Protein, Knockout, NLR Family, Pyrin Domain-Containing 3 Protein
Abstract

The inflammasomes are multiprotein complexes that activate caspase-1 in response to infections and stress, resulting in the secretion of pro-inflammatory cytokines. Here we report that IκB kinase α (IKKα) is a critical negative regulator of apoptosis-associated specklike protein containing a C-terminal caspase-activation-andrecruitment (CARD) domain (ASC)-dependent inflammasomes. IKKα controls the inflammasome at the level of the adaptor ASC, which interacts with IKKα in the nucleus of resting macrophages in an IKKα kinase-dependent manner. Loss of IKKα kinase activity results in inflammasome hyperactivation. Mechanistically, the downstream nuclear effector IKK-related kinase (IKKi) facilitates translocation of ASC from the nucleus to the perinuclear area during inflammasome activation. ASC remains under the control of IKKα in the perinuclear area following translocation of the ASC/IKKα complex. Signal 2 of NLRP3 activation leads to inhibition of IKKα kinase activity through the recruitment of PP2A, allowing ASC to participate in NLRP3 inflammasome assembly. Taken together, these findings reveal a IKKi-IKKα-ASC axis that serves as a common regulatory mechanism for ASC-dependent inflammasomes.

Published
2014

15. IRAK2 directs stimulus-dependent nuclear export of inflammatory mRNAs

Author

Zhou, Hao, primary, Bulek, Katarzyna, additional, Li, Xiao, additional, Herjan, Tomasz, additional, Yu, Minjia, additional, Qian, Wen, additional, Wang, Han, additional, Zhou, Gao, additional, Chen, Xing, additional, Yang, Hui, additional, Hong, Lingzi, additional, Zhao, Junjie, additional, Qin, Luke, additional, Fukuda, Koichi, additional, Flotho, Annette, additional, Gao, Ji, additional, Dongre, Ashok, additional, Carman, Julie A, additional, Kang, Zizhen, additional, Su, Bing, additional, Kern, Timothy S, additional, Smith, Jonathan D, additional, Hamilton, Thomas A, additional, Melchior, Frauke, additional, Fox, Paul L, additional, and Li, Xiaoxia, additional

Published
2017
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16. Author response: IRAK2 directs stimulus-dependent nuclear export of inflammatory mRNAs

Author

Zhou, Hao, primary, Bulek, Katarzyna, additional, Li, Xiao, additional, Herjan, Tomasz, additional, Yu, Minjia, additional, Qian, Wen, additional, Wang, Han, additional, Zhou, Gao, additional, Chen, Xing, additional, Yang, Hui, additional, Hong, Lingzi, additional, Zhao, Junjie, additional, Qin, Luke, additional, Fukuda, Koichi, additional, Flotho, Annette, additional, Gao, Ji, additional, Dongre, Ashok, additional, Carman, Julie A, additional, Kang, Zizhen, additional, Su, Bing, additional, Kern, Timothy S, additional, Smith, Jonathan D, additional, Hamilton, Thomas A, additional, Melchior, Frauke, additional, Fox, Paul L, additional, and Li, Xiaoxia, additional

Published
2017
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17. Interleukin-17 regulates CXCL1 mRNA stability via an AUUUA/Tristetraprolin-independent sequence1

Author

Datta, Shyamasree, Novotny, Michael, Pavicic, Paul G., Zhao, Chenyang, Herjan, Tomasz, Hartupee, Justin, and Hamilton, Thomas

Subjects
Base Sequence, Chemokine CXCL1, RNA Stability, Interleukin-17, Molecular Sequence Data, RNA-Binding Proteins, Zinc Fingers, Article, Cell Line, Mice, Tristetraprolin, Mutagenesis, Site-Directed, Animals, Humans, RNA, Messenger, Transgenes, 3' Untranslated Regions, Cells, Cultured, HeLa Cells
Abstract

Interleukin (IL)-17 contributes to inflammatory response in part by promoting enhanced expression of chemokines such as CXCL1 by prolonging the half-life of this constitutively unstable mRNA. While IL-17 is a weak stimulus for transcription of the CXCL1 gene, it strongly potentiates message accumulation via stabilization when the mRNA is transcribed in cells stimulated with TNF. In myeloid cells, LPS-induced CXCL1 mRNA stabilization is dependent upon AUUUA-containing sequence motifs that are recognized by the RNA binding protein Tristetraprolin (TTP). Using deletion and site specific mutagenesis, we now report that IL-17-mediated stabilization of CXCL1 mRNA in non-myeloid cells depends upon a sequence that does not contain the AUUUA motif. Furthermore, a specific two nucleotide mutation within this region markedly abrogates sensitivity for IL-17-mediated stabilization. Consistent with this finding, the IL-17-sensitive sequence does not exhibit increased instability in the presence of TTP, and CXCL1 mRNA remains unstable and can be stabilized in response to treatment with IL-17 in embryo fibroblasts (MEFs) from mice in which the TTP gene has been deleted. While the RNA binding protein KSRP has been shown to participate in regulating the instability of human CXCL8 mRNA, RNAi-based reduction in KSRP does not impact the instability mediated by the IL-17-sensitive sequence motif. These findings suggest that IL-17-mediated chemokine mRNA stabilization in non-myeloid cells utilizes a mechanism that is distinct from that operating to control AU-rich mRNA stability in myeloid cells.

Published
2009

19. 272

Author

Wang, Chenhui, primary, Wu, Ling, additional, Bulek, Katarzyna, additional, Martin, Bradley N., additional, Zepp, Jarod A., additional, Kang, Zizhen, additional, Liu, Caini, additional, Herjan, Tomasz, additional, Misra, Saurav, additional, Carman, Julie A., additional, Gao, Ji, additional, Dongre, Ashok, additional, Han, Shujie, additional, Bunting, Kevin D., additional, Ko, Jennifer S., additional, Xiao, Hui, additional, Kuchroo, Vijay K., additional, Ouyang, Wenjun, additional, and Li, Xiaoxia, additional

Published
2013
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20. HuR Is Required for IL-17–Induced Act1-Mediated CXCL1 and CXCL5 mRNA Stabilization

Author

Herjan, Tomasz, primary, Yao, Peng, additional, Qian, Wen, additional, Li, Xiao, additional, Liu, Caini, additional, Bulek, Katarzyna, additional, Sun, Dongxu, additional, Yang, Wen-Pin, additional, Zhu, Jun, additional, He, Aiqing, additional, Carman, Julie A., additional, Erzurum, Serpil C., additional, Lipshitz, Howard D., additional, Fox, Paul L., additional, Hamilton, Thomas A., additional, and Li, Xiaoxia, additional

Published
2013
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22. The psoriasis-associated D10N variant of the adaptor Act1 with impaired regulation by the molecular chaperone hsp90

Author

Wang, Chenhui, primary, Wu, Ling, additional, Bulek, Katarzyna, additional, Martin, Bradley N, additional, Zepp, Jarod A, additional, Kang, Zizhen, additional, Liu, Caini, additional, Herjan, Tomasz, additional, Misra, Saurav, additional, Carman, Julie A, additional, Gao, Ji, additional, Dongre, Ashok, additional, Han, Shujie, additional, Bunting, Kevin D, additional, Ko, Jennifer S, additional, Xiao, Hui, additional, Kuchroo, Vijay K, additional, Ouyang, Wenjun, additional, and Li, Xiaoxia, additional

Published
2012
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23. CS10-3. IKKi is required for interleukin 17-dependent signaling associated with neutrophilia and pulmonary inflammation

Author

Bulek, Katarzyna, primary, Liu, Caini, additional, Swaidani, Shadi, additional, Wang, Liwen, additional, Page, Richard C., additional, Gulen, Muhammet F., additional, Herjan, Tomasz, additional, Abbadi, Amina, additional, Qian, Wen, additional, Sun, Dongxu, additional, Lauer, Mark, additional, Hascall, Vincent, additional, Misra, Saurav, additional, Chance, Mark, additional, Aronica, Mark, additional, Hamilton, Thomas, additional, and Li, Xiaoxia, additional

Published
2011
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24. The inducible kinase IKKi is required for IL-17-dependent signaling associated with neutrophilia and pulmonary inflammation

Author

Bulek, Katarzyna, primary, Liu, Caini, additional, Swaidani, Shadi, additional, Wang, Liwen, additional, Page, Richard C, additional, Gulen, Muhammet F, additional, Herjan, Tomasz, additional, Abbadi, Amina, additional, Qian, Wen, additional, Sun, Dongxu, additional, Lauer, Mark, additional, Hascall, Vincent, additional, Misra, Saurav, additional, Chance, Mark R, additional, Aronica, Mark, additional, Hamilton, Thomas, additional, and Li, Xiaoxia, additional

Published
2011
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29. Psoriasis-associated variant Act1 D10N with impaired regulation by Hsp90

Author

Wang, Chenhui, Wu, Ling, Bulek, Katarzyna, Martin, Bradley N., Zepp, Jarod A., Kang, Zizhen, Liu, Caini, Herjan, Tomasz, Misra, Saurav, Carman, Julie A., Gao, Ji, Dongre, Ashok, Han, Shujie, Bunting, Kevin D., Ko, Jennifer S., Xiao, Hui, Kuchroo, Vijay K., Ouyang, Wenjun, and Li, Xiaoxia

Abstract

Act1 is an essential adaptor molecule in IL-17-mediated signaling and is recruited to the IL-17 receptor upon IL-17 stimulation. Here, we report that Act1 is a client protein of the molecular chaperone, Hsp90. The Act1 variant (D10N) linked to psoriasis susceptibility is defective in its interaction with Hsp90, resulting in a global loss of Act1 function. Act1-/- mice modeled the mechanistic link between Act1 loss of function and psoriasis susceptibility. Although Act1 is necessary for IL-17-mediated inflammation, Act1-/- mice exhibited a hyper TH17 response and developed spontaneous IL-22-dependent skin inflammation. In the absence of IL-17-signaling, IL-22 is the main contributor to skin inflammation, providing a molecular mechanism for the association of Act1 (D10N) with psoriasis susceptibility.

Published
2012
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30. The role of interleukin-17 in tumor development and progression

Author

Zhao, Junjie, Chen, Xing, Herjan, Tomasz, and Li, Xiaoxia

Abstract

IL-17, a potent proinflammatory cytokine, has been shown to intimately contribute to the formation, growth, and metastasis of a wide range of malignancies. Recent studies implicate IL-17 as a link among inflammation, wound healing, and cancer. While IL-17–mediated production of inflammatory mediators mobilizes immune-suppressive and angiogenic myeloid cells, emerging studies reveal that IL-17 can directly act on tissue stem cells to promote tissue repair and tumorigenesis. Here, we review the pleotropic impacts of IL-17 on cancer biology, focusing how IL-17–mediated inflammatory response and mitogenic signaling are exploited to equip its cancer-promoting function and discussing the implications in therapies.

Published
2020
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31. IL-17A Recruits Rab35 to IL-17R to Mediate PKCα-Dependent Stress Fiber Formation and Airway Smooth Muscle Contractility.

Author

Xing Chen, Suidong Ouyang, Caini Liu, Majors, Alana, Aronica, Mark, Xiaoxia Li, Bulek, Katarzyna, Herjan, Tomasz, Zepp, Jarod, Bodaszewska-Lubas, Malgorzata, Parron, Vandy, Garantziotis, Stavros, Sundaram, Aparna, Sheppard, Dean, Ji Gao, Dongre, Ashok, Carman, Julie, and Echard, Arnaud

Subjects
*SMOOTH muscle
Abstract

IL-17A is a critical proinflammatory cytokine for the pathogenesis of asthma including neutrophilic pulmonary inflammation and airway hyperresponsiveness. In this study, by cell type-specific deletion of IL-17R and adaptor Act1, we demonstrated that IL-17R/Act1 exerts a direct impact on the contraction of airway smooth muscle cells (ASMCs). Mechanistically, IL-17A induced the recruitment of Rab35 (a small monomeric GTPase) and DennD1C (guanine nucleotide exchange factor [GEF]) to the IL-17R/Act1 complex in ASMCs, resulting in activation of Rab35. Rab35 knockdown showed that IL-17A-induced Rab35 activation was essential for protein kinase Ca (PKCa) activation and phosphorylation of fascin at Ser39 in ASMCs, allowing F-actin to interact with myosin to form stress fibers and enhance the contraction induced by methacholine. PKCa inhibitor or Rab35 knockdown indeed substantially reduced IL-17A-induced stress fiber formation in ASMCs and attenuated IL-17A-enhanced, methacholineinduced contraction of airway smooth muscle. Taken together, these data indicate that IL-17A promotes airway smooth muscle contraction via direct recruitment of Rab35 to IL-17R, followed by PKCa activation and stress fiber formation. [ABSTRACT FROM AUTHOR]

Published
2019
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32. 272: The psoriasis-associated D10N variant of the adaptor Act1 with impaired regulation by the molecular chaperone Hsp90.

Author

Wu, Ling, Bulek, Katarzyna, Martin, Bradley N., Zepp, Jarod A., Kang, Zizhen, Liu, Caini, Herjan, Tomasz, Misra, Saurav, Carman, Julie A., Gao, Ji, Dongre, Ashok, Han, Shujie, Bunting, Kevin D., Ko, Jennifer S., Xiao, Hui, Kuchroo, Vijay K., Ouyang, Wenjun, and Li, Xiaoxia

Subjects
*PSORIASIS, *INTERLEUKINS, *GENETIC regulation, *MOLECULAR chaperones, *HEAT shock proteins, *CELLULAR signal transduction, *DISEASE susceptibility, *LABORATORY mice
Abstract

Act1 is an essential adaptor in interleukin 17 (IL-17)-mediated signaling and is recruited to the receptor for IL-17 after stimulation with IL-17. Here we found that Act1 was a ‘client’ protein of the molecular chaperone hsp90. The D10N variant of Act1 (Act1(D10N)) that is linked to susceptibility to psoriasis was defective in its interaction with hsp90, which resulted in a global loss of Act1 function. Act1-deficient mice modeled the mechanistic link between loss of Act1 function and susceptibility to psoriasis. Although Act1 was necessary for IL-17-mediated inflammation, Act1-deficient mice had a hyperactive response of the TH17 subset of helper T cells and developed spontaneous IL-22-dependent skin inflammation. In the absence of IL-17 signaling, IL-22 was the main contributor to skin inflammation, which provides a molecular mechanism for the association of Act1(D10N) with psoriasis susceptibility. [ABSTRACT FROM AUTHOR]

Published
2013
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33. The psoriasis-associated D10N variant of the adaptor Act1 with impaired regulation by the molecular chaperone hsp90.

Author

Wang C, Wu L, Bulek K, Martin BN, Zepp JA, Kang Z, Liu C, Herjan T, Misra S, Carman JA, Gao J, Dongre A, Han S, Bunting KD, Ko JS, Xiao H, Kuchroo VK, Ouyang W, and Li X

Subjects
Animals, Cell Line, Connexin 43 genetics, Connexin 43 immunology, Disease Models, Animal, Genetic Predisposition to Disease, Humans, Interleukin-17 metabolism, Mice, Mice, Knockout, Molecular Chaperones genetics, Mutation genetics, Peptide Fragments genetics, Peptide Fragments immunology, Polymorphism, Genetic, Protein Binding genetics, Protein Binding immunology, Psoriasis genetics, Signal Transduction, Connexin 43 metabolism, HSP90 Heat-Shock Proteins metabolism, Molecular Chaperones metabolism, Peptide Fragments metabolism, Psoriasis immunology, Th17 Cells immunology
Abstract

Act1 is an essential adaptor in interleukin 17 (IL-17)-mediated signaling and is recruited to the receptor for IL-17 after stimulation with IL-17. Here we found that Act1 was a 'client' protein of the molecular chaperone hsp90. The D10N variant of Act1 (Act1(D10N)) that is linked to susceptibility to psoriasis was defective in its interaction with hsp90, which resulted in a global loss of Act1 function. Act1-deficient mice modeled the mechanistic link between loss of Act1 function and susceptibility to psoriasis. Although Act1 was necessary for IL-17-mediated inflammation, Act1-deficient mice had a hyperactive response of the T(H)17 subset of helper T cells and developed spontaneous IL-22-dependent skin inflammation. In the absence of IL-17 signaling, IL-22 was the main contributor to skin inflammation, which provides a molecular mechanism for the association of Act1(D10N) with psoriasis susceptibility.

Published
2013
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34. IL-17 regulates CXCL1 mRNA stability via an AUUUA/tristetraprolin-independent sequence.

Author

Datta S, Novotny M, Pavicic PG Jr, Zhao C, Herjan T, Hartupee J, and Hamilton T

Subjects
Animals, Base Sequence, Cell Line, Cells, Cultured, Chemokine CXCL1 physiology, HeLa Cells, Humans, Mice, Molecular Sequence Data, Mutagenesis, Site-Directed, RNA, Messenger genetics, RNA-Binding Proteins biosynthesis, RNA-Binding Proteins genetics, RNA-Binding Proteins physiology, Transgenes immunology, Tristetraprolin deficiency, Tristetraprolin physiology, Zinc Fingers genetics, Zinc Fingers immunology, 3' Untranslated Regions immunology, Chemokine CXCL1 genetics, Chemokine CXCL1 metabolism, Interleukin-17 physiology, RNA Stability immunology, RNA, Messenger metabolism, Tristetraprolin genetics, Tristetraprolin metabolism
Abstract

IL-17 contributes to inflammatory response in part by promoting enhanced expression of chemokines, such as CXCL1, by prolonging the t(1/2) of this constitutively unstable mRNA. Although IL-17 is a weak stimulus for transcription of the CXCL1 gene, it strongly potentiates message accumulation via stabilization when the mRNA is transcribed in cells stimulated with TNF. In myeloid cells, LPS-induced CXCL1 mRNA stabilization is dependent on AUUUA-containing sequence motifs that are recognized by the RNA binding protein tristetraprolin (TTP). Using deletion and site-specific mutagenesis, we report that IL-17-mediated stabilization of CXCL1 mRNA in nonmyeloid cells depends on a sequence that does not contain the AUUUA motif. Furthermore, a specific two-nucleotide mutation within this region markedly abrogates sensitivity for IL-17-mediated stabilization. Consistent with this finding, the IL-17-sensitive sequence does not exhibit increased instability in the presence of TTP, and CXCL1 mRNA remains unstable and can be stabilized in response to treatment with IL-17 in embryo fibroblasts from mice in which the TTP gene has been deleted. Whereas the RNA binding protein KSRP has been shown to participate in regulating the instability of human CXCL8 mRNA, inhibitory RNA-based reduction in KSRP does not effect the instability mediated by the IL-17-sensitive sequence motif. These findings suggest that IL-17-mediated chemokine mRNA stabilization in nonmyeloid cells uses a mechanism that is distinct from that operating to control AU-rich mRNA stability in myeloid cells.

Published
2010
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