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Author: Li-Yin Hung Publisher: ISBN: Category : Languages : en Pages :
Book Description
Results from recent studies suggest that in addition to the barrier function, airway epithelial cells (AECs) also actively participating in airway immune response. We previously demonstrated that IL-17A is a potent inducer of human [beta]-defensin (hBD) 2 and CCL20 expression in well-differentiated human AECs. In addition to the anti-microbial activity, both hBD2 and CCL20 are principal chemotactic ligands of CCR6, which is expressed by dendritic cells (DC) and T lymphocytes. To further explore the chemotactic significance of IL-17A in the mouse system, we conducted studies using primary mouse AECs and Cc10-Il17 transgenic animals, which display airway overexpression of IL-17A. We found that mouse AECs expressed elevated mCcl20 in response to mIL-17A in an NF-[kappa]B-dependent manner. Conditioned media from mIL-17A-treated mouse AECs stimulated the migration of CCR6-positive bone marrow-derived DC in vitro; this chemotactic activity was blocked by an anti-CCL20 neutralizing antibody. In Cc10-Il17 transgenic mice, we detected elevated mCcl20 in the lung and an increased number of CCR6-positive DCs in bronchoalveolar lavage fluid. These mice also display increased mucin production in their lungs compared to wild-type mice. Blocking the migration of CCR6-expressing cells in vivo by anti-CCR6 or anti-CCL20 antibody lowered mucin production in the airways, suggesting a functional role of IL-17A/CCL20 in regulating CCR6-positive DC migration and mucous cell metaplasia. IL-17A also induces the expression of IL-19, a proinflammatory cytokine in the IL-10 cytokine family, in human AECs. We have shown the association of IL-19 with asthma and that AECs were one of the potential sources of IL-19 in the disease. Using well-differentiated primary mouse AECs grown under air-liquid interface conditions, we demonstrated that Th2 cytokines such as IL-4 and IL-13 could induce Il19 expression. In the OVA mouse asthma model, Il19 expression was elevated in asthmatic lung tissue at the early stage. This elevation was observed in airway epithelial cells but not alveolar macrophages. An increase was only observed for IL-19 and not other IL-20 subfamily members, such as IL-20, IL-22, and IL-24. We further demonstrated that IL-19 could stimulate in vitro Th2 cell lineage differentiation of naïve T cells when added initially to the polarizing medium. These results demonstrate that IL-19 produced by airway epithelial cells at the early stage of the asthmatic response may further amplify the Th2 response through promoting T helper cell differentiation. IL-19 has also been shown to stimulate [beta]-defensin in keratinocytes, but its potential to induce defensin expression in the airways has not been characterized. Here we report that IL-19 is able to induce hBD gene (DEFB4) expression in human airway epithelial cell line HBE-1, as well as primary mouse airway cells. Both STAT1 and STAT3 are required in IL-19-induced DEFB4 although only STAT3 is significantly activated by IL-19 while STAT1 is constantly phosphorylated. STAT5 is also phosphorylated in HBE-1 but does not involve in DEFB4 induction; however knocking down STAT5 appears to alter basal DEFB4 level. In addition to IL-19 we also found other IL-20 subfamily cytokines, including IL-20, -22, -24, and -26, capable of stimulating DEFB4 expression in HBE-1 cells.
Author: Li-Yin Hung Publisher: ISBN: Category : Languages : en Pages :
Book Description
Results from recent studies suggest that in addition to the barrier function, airway epithelial cells (AECs) also actively participating in airway immune response. We previously demonstrated that IL-17A is a potent inducer of human [beta]-defensin (hBD) 2 and CCL20 expression in well-differentiated human AECs. In addition to the anti-microbial activity, both hBD2 and CCL20 are principal chemotactic ligands of CCR6, which is expressed by dendritic cells (DC) and T lymphocytes. To further explore the chemotactic significance of IL-17A in the mouse system, we conducted studies using primary mouse AECs and Cc10-Il17 transgenic animals, which display airway overexpression of IL-17A. We found that mouse AECs expressed elevated mCcl20 in response to mIL-17A in an NF-[kappa]B-dependent manner. Conditioned media from mIL-17A-treated mouse AECs stimulated the migration of CCR6-positive bone marrow-derived DC in vitro; this chemotactic activity was blocked by an anti-CCL20 neutralizing antibody. In Cc10-Il17 transgenic mice, we detected elevated mCcl20 in the lung and an increased number of CCR6-positive DCs in bronchoalveolar lavage fluid. These mice also display increased mucin production in their lungs compared to wild-type mice. Blocking the migration of CCR6-expressing cells in vivo by anti-CCR6 or anti-CCL20 antibody lowered mucin production in the airways, suggesting a functional role of IL-17A/CCL20 in regulating CCR6-positive DC migration and mucous cell metaplasia. IL-17A also induces the expression of IL-19, a proinflammatory cytokine in the IL-10 cytokine family, in human AECs. We have shown the association of IL-19 with asthma and that AECs were one of the potential sources of IL-19 in the disease. Using well-differentiated primary mouse AECs grown under air-liquid interface conditions, we demonstrated that Th2 cytokines such as IL-4 and IL-13 could induce Il19 expression. In the OVA mouse asthma model, Il19 expression was elevated in asthmatic lung tissue at the early stage. This elevation was observed in airway epithelial cells but not alveolar macrophages. An increase was only observed for IL-19 and not other IL-20 subfamily members, such as IL-20, IL-22, and IL-24. We further demonstrated that IL-19 could stimulate in vitro Th2 cell lineage differentiation of naïve T cells when added initially to the polarizing medium. These results demonstrate that IL-19 produced by airway epithelial cells at the early stage of the asthmatic response may further amplify the Th2 response through promoting T helper cell differentiation. IL-19 has also been shown to stimulate [beta]-defensin in keratinocytes, but its potential to induce defensin expression in the airways has not been characterized. Here we report that IL-19 is able to induce hBD gene (DEFB4) expression in human airway epithelial cell line HBE-1, as well as primary mouse airway cells. Both STAT1 and STAT3 are required in IL-19-induced DEFB4 although only STAT3 is significantly activated by IL-19 while STAT1 is constantly phosphorylated. STAT5 is also phosphorylated in HBE-1 but does not involve in DEFB4 induction; however knocking down STAT5 appears to alter basal DEFB4 level. In addition to IL-19 we also found other IL-20 subfamily cytokines, including IL-20, -22, -24, and -26, capable of stimulating DEFB4 expression in HBE-1 cells.
Author: Rola Hamed Publisher: ISBN: Category : Languages : en Pages :
Book Description
"Severe neutrophilic asthma remains a relevant clinical problem with no alternative treatment as corticosteroids fail to alleviate symptoms. Severe neutrophilic asthma patients are characterized by high levels of Interleukin (IL)-17a, a modulator of inflammation, and IL-8, a major neutrophil chemoattractant. With inconsistent data relating to the role of IL-17a in inflammation, some studies describe it as a stimulator, others as a potentiator. In addition, the contribution of IL-17a to corticosteroid-insensitivity remains unclear. This study focused on better understanding the role of IL-17a. Using airway epithelial cells as a model, experiments were carried out in the BEAS-2B cell line then key experiments and findings were confirmed in primary cells from severe neutrophilic asthmatics and healthy individuals, where we found they respond in a qualitatively similar fashion to the cell line. Firstly, the contribution of IL-17a to airway inflammation was assessed at both the mRNA and protein levels. IL-17a potentiated IL-1b and Tumor Necrosis Factor (TNF)-a induced IL-8 mRNA without affecting protein levels nor mRNA kinetics. Moreover, IL-17a did not act as a stimulus on its own. The effects of IL-17a on eotaxin 3, a major eosinophil chemoattractant present in severe asthmatic airways, was also studied to confirm the involvement of IL-17a in neutrophilic vs. eosinophilic severe asthma. IL-17a did not affect IL-4 nor IL-13 induced eotaxin 3 expression, protein levels, nor mRNA kinetics indicating it promotes a more neutrophilic environment through IL-8 potentiation. Subsequently, the contribution of IL-17a to corticosteroid-insensitivity was addressed. An inhaled corticosteroid, Budesonide, was tested where dose-response curves comparing IL-17a treated and untreated cells demonstrated that IL-17a pre-treatment leads to a higher IC50, thus decreased corticosteroid-sensitivity. The addition of a Long Acting Beta-adrenoceptor Agonist (LABA) did not reverse the decrease in corticosteroid-sensitivity observed with IL-17a pre-treatment. Thus, IL-17a does contribute to corticosteroid-insensitivity as well as neutrophilic inflammation. This study confirmed the role of IL-17a on airway epithelial cells and paves the way for mechanistic studies, which can lead to a new therapeutic target for this patient subset seeing that anti-IL-17a monoclonal antibodies showed no efficacy in the clinical setting." --
Author: Phoebe Lin Publisher: Springer Nature ISBN: 3030228274 Category : Medical Languages : en Pages : 208
Book Description
This unique, comprehensive book provides a much-needed reference on the treatment and management of non-infectious uveitis. Carefully designed, Treatment of Non-infectious Uveitis is the first book of its kind to provide an in-depth, clinically-relevant, expert-driven resource for ophthalmologists focusing on modalities of uveitis treatment, their mechanism of action, dosing, and side effects. Each chapter provides an introduction, mechanism of action, indication, dosage, side effects, and efficacy summaries from clinical trials and other published literature. Topics range from topical treatment, to locally administered therapy including drug-releasing implants, to systemic immunosuppressive treatments both tried and new, as well as surgical management, with each chapter highlighting important practice pearls as well as easy-reference dosing tables, side effects, and lab monitoring pertinent to the agents discussed. The book concludes with a discussion of novel approaches to the treatment of non-infectious uveitis, and special considerations when treating uveitis in the pediatric patient. The majority of patients with non-infectious uveitis are treated by comprehensive ophthalmologists, many of whom are less familiar with established treatment guidelines outlining the role of corticosteroids and immunomodulatory therapy. While the non-specialist, resident, or fellow is sure to benefit from this one-stop guide to uveitis treatment, retina and uveitis specialists alike will also appreciate the practice tips and thorough coverage of this expertly-written reference. Treatment of Non-infectious Uveitis is the ideal reference for all ophthalmologists who seek to improve their understanding of the causes of uveitis and learn how to best treat this condition.
Author: Steven L. Kunkel Publisher: Marcel Dekker ISBN: Category : Medical Languages : en Pages : 592
Book Description
A comprehensive text providing much of the currently available knowledge in the field of cytokines. There are four areas covered, including general overviews of each of the major cytokines, listings of the important interactions these cytokines have with inflammatory cells, discussions of current an
Author: Z. Kmiec Publisher: Springer Science & Business Media ISBN: 3642565530 Category : Science Languages : en Pages : 154
Book Description
It is only during the last decade that the functions of sinusoidal endothelial cells, Kupffer cells, hepatic stellate cells, pit cells and other intrahepatic lymphocytes have been better understood. The development of methods for isolation and co-culturing various types of liver cells has established that they communicate and cooperate via secretion of various intercellular mediators. This monograph summarizes multiple data that suggest the important role of cellular cross-talk for the functions of both normal and diseased liver. Special features of the book include concise presentation of the majority of detailed data in 19 tables. Original schemes allow for the clear illustration of complicated intercellular relationships. This is the first ever presentation of the newly emerging field of liver biology, which is important for hepatic function in health and disease and opens new avenues for therapeutic interventions.
Author: Peter Howarth Publisher: CRC Press ISBN: 9780429132582 Category : MEDICAL Languages : en Pages : 328
Book Description
This landmark volume discusses the characteristics and impact of the remodeling process on airway function and clinical disease expression within the airway in asthma, covering pharmacological therapies and possible future targets relevant to regulating the remodeling process. Emphasizes the importance of treating underlying airway inflammation and the relevance of structural alterations to the airway wall, including glandular increases, enhanced collagen deposition within the submucosa, increased vasculature, smooth hypertrophy, and hyperplasias! Tracing the development and maintenance of bronchial hyperresponsiveness, decline in lung function, and loss of reversibility evident in chronic asthma, Airway Remodelingdescribes the contribution of inflammatory cells in the development of airway structural changes examines how pharmaceutical agents act and whether existing treatments modify or prevent remodeling in chronically inflamed asthmatic airways considers whether neural pathways initiate as well as contribute to the airway inflammatory cascade that leads to remodeling reviews the action of cytokines and growth factors on ASM signaling outlines novel approaches to regulating smooth muscle growth clarifies whether permanent ventilatory incapacity in asthma is caused by the uncoupling of the airway and the role of the lung parenchyma details high-resolution computerized tomography scan to measure the internal size of the airway at baseline, during challenge, or after bronchodilatation and more!Improving lung function and quality of life by reducing the need for emergency care, hospital admissions, and systemic steroid administration, Airway Remodeling is a superb reference for pulmonologists and respiratory system specialists; physiologists; pneumologists; allergists; pharmacologists; molecular, cellular, and lung biologists; and graduate and medical school students in these disciplines.
Author: Randy Q. Cron Publisher: Springer Nature ISBN: 303022094X Category : Medical Languages : en Pages : 607
Book Description
Cytokine Storm Syndromes, including HLH and MAS, are frequently fatal disorders, particularly if not recognized early and treated during presentation. The genetics of Cytokine Storm Syndromes are being defined with many of the risk alleles giving rise to mutations in the perforin-mediated cytolytic pathway used by CD8 cytotoxic T cells and natural killer cells. These are being studied using murine models. Up to 10% of the general population may carry risk alleles for developing Cytokine Storm Syndromes, and Cytokine Storm Syndromes are being increasingly recognized around the world in pediatric and adult hospitals. A variety of infectious, rheumatic, and oncologic triggers are commonly associated with Cytokine Storm Syndromes, but understanding this disorder is critical for all researchers and physicians to ensure timely and appropriate therapy. This textbook, the first of its kind, addresses all aspects of the disorder – from genetics, pathophysiology, and ongoing research, to clinical presentations, risk factors, and treatment.
Author: Kian Fan Chung Publisher: European Respiratory Society ISBN: 1849841047 Category : Medical Languages : en Pages : 365
Book Description
Severe asthma is a form of asthma that responds poorly to currently available medication, and its patients represent those with greatest unmet needs. In the last 10 years, substantial progress has been made in terms of understanding some of the mechanisms that drive severe asthma; there have also been concomitant advances in the recognition of specific molecular phenotypes. This ERS Monograph covers all aspects of severe asthma – epidemiology, diagnosis, mechanisms, treatment and management – but has a particular focus on recent understanding of mechanistic heterogeneity based on an analytic approach using various ‘omics platforms applied to clinically well-defined asthma cohorts. How these advances have led to improved management targets is also emphasised. This book brings together the clinical and scientific expertise of those from around the world who are collaborating to solve the problem of severe asthma.
Author: Li-Yin Hung
Author: Li-Yin Hung
Author: Fei Huang
Author: Cheng-Yuan Kao
Author: Rola Hamed
Author: Phoebe Lin
Author: Steven L. Kunkel
Author: Z. Kmiec
Author: Peter Howarth
Author: Randy Q. Cron
Author: Kian Fan Chung