Loss of Peripheral Tolerance in Emphysema. Phenotypes, Exacerbations, and Disease Progression
Autor: | Ran You, Ming Shan, Xiaoyi Yuan, David B. Corry, Sivasubramanium Bhavani, Farrah Kheradmand |
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Rok vydání: | 2015 |
Předmět: |
Pulmonary and Respiratory Medicine
T-Lymphocytes Autoimmunity medicine.disease_cause Immune tolerance Mice Pulmonary Disease Chronic Obstructive Immune system medicine Animals Humans Lung cancer Autocrine signalling Lung Peripheral Tolerance business.industry Smoking Peripheral tolerance respiratory system Transatlantic Airway Conference medicine.disease Obstructive lung disease respiratory tract diseases Disease Models Animal Phenotype medicine.anatomical_structure Pulmonary Emphysema Immunology Complement C3a Disease Progression Cytokines business |
Zdroj: | Annals of the American Thoracic Society. 12:S164-S168 |
ISSN: | 2325-6621 2329-6933 |
DOI: | 10.1513/annalsats.201503-115aw |
Popis: | Heterogeneity in the development and progression of cigarette smoke-induced lung diseases strongly argues for a need to improve the clinical and phenotypic characterization of patients with chronic obstructive lung disease and emphysema. Smokers with emphysema are at a much higher risk for accelerated loss of lung function, increased cardiovascular morbidity, and development of lung cancer. Recent evidence in human translational studies and animal models suggests that emphysema is associated with activation of specialized antigen-presenting cells and that cigarette smoke can disrupt the induction of immune tolerance in the lungs. Quantitative assessment of cytokines expressed by autoreactive T lymphocytes in response to human lung elastin fragments has shown a strong positive correlation between T helper Type 1 (Th1) and Th17 cells' immune responses and emphysema. In search of factors that could reduce the threshold for induction of autoimmune inflammation, we have discovered that cleavage of complement protein 3 (C3) generates bioactive molecules (e.g., C3a) and activates lung antigen-presenting cells. The autocrine and paracrine function of C3a and its receptor are required in T cell-mediated inflammatory responses to cigarette smoke in both human and preclinical models of emphysema. Targeting upstream molecules that reduce the potential for generation of autoreactive T cells could lead to the development of novel therapeutics to prevent progression of emphysema in smokers. |
Databáze: | OpenAIRE |
Externí odkaz: |
Abstrakt: | Heterogeneity in the development and progression of cigarette smoke-induced lung diseases strongly argues for a need to improve the clinical and phenotypic characterization of patients with chronic obstructive lung disease and emphysema. Smokers with emphysema are at a much higher risk for accelerated loss of lung function, increased cardiovascular morbidity, and development of lung cancer. Recent evidence in human translational studies and animal models suggests that emphysema is associated with activation of specialized antigen-presenting cells and that cigarette smoke can disrupt the induction of immune tolerance in the lungs. Quantitative assessment of cytokines expressed by autoreactive T lymphocytes in response to human lung elastin fragments has shown a strong positive correlation between T helper Type 1 (Th1) and Th17 cells' immune responses and emphysema. In search of factors that could reduce the threshold for induction of autoimmune inflammation, we have discovered that cleavage of complement protein 3 (C3) generates bioactive molecules (e.g., C3a) and activates lung antigen-presenting cells. The autocrine and paracrine function of C3a and its receptor are required in T cell-mediated inflammatory responses to cigarette smoke in both human and preclinical models of emphysema. Targeting upstream molecules that reduce the potential for generation of autoreactive T cells could lead to the development of novel therapeutics to prevent progression of emphysema in smokers. |
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ISSN: | 23256621 23296933 |
DOI: | 10.1513/annalsats.201503-115aw |