Identification of Periplakin as a New Target for Autoreactivity in Idiopathic Pulmonary Fibrosis

Injury to alveolar epithelial cells is central to the pathophysiology of idiopathic pulmonary fibrosis (IPF). An abnormal autoimmune response directed against antigens of the alveolar epithelium may contribute to the disease. To detect circulating autoantibodies (autoAbs) directed against epithelial...

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Published in	American journal of respiratory and critical care medicine Vol. 183; no. 6; pp. 759 - 766
Main Authors	Taillé, Camille, Grootenboer-Mignot, Sabine, Boursier, Céline, Michel, Laurence, Debray, Marie-Pierre, Fagart, Jérôme, Barrientos, Lorena, Mailleux, Arnaud, Cigna, Natacha, Tubach, Florence, Marchal-Sommé, Joëlle, Soler, Paul, Chollet-Martin, Sylvie, Crestani, Bruno
Format	Journal Article
Language	English
Published	New York, NY American Thoracic Society 15.03.2011
Subjects	Adult Aged Anesthesia. Intensive care medicine. Transfusions. Cell therapy and gene therapy Antibodies Antigens Autoantibodies - blood Autoimmunity Biological and medical sciences Biomarkers - blood Case-Control Studies Cell adhesion & migration Chronic obstructive pulmonary disease Connective tissue Experiments Female Humans Idiopathic Pulmonary Fibrosis - blood Idiopathic Pulmonary Fibrosis - immunology Idiopathic Pulmonary Fibrosis - physiopathology Immunoglobulin G - blood Intensive care medicine Lavage Lung diseases Male Mass spectrometry Medical sciences Middle Aged Pathophysiology Plakins - blood Pneumology Proteins Pulmonary fibrosis Pulmonary hypertension. Acute cor pulmonale. Pulmonary embolism. Pulmonary vascular diseases Respiratory Mucosa - immunology Scientific imaging Severity of Illness Index Autoimmunity Lung disease Intensive care Pulmonary fibrosis periplakin Respiratory disease Idiopathic desmosomes Resuscitation
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ISSN	1073-449X 1535-4970 1535-4970
DOI	10.1164/rccm.201001-0076OC

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Abstract	Injury to alveolar epithelial cells is central to the pathophysiology of idiopathic pulmonary fibrosis (IPF). An abnormal autoimmune response directed against antigens of the alveolar epithelium may contribute to the disease. To detect circulating autoantibodies (autoAbs) directed against epithelial structures. We performed immunoblot by separating human placental amnion extract or alveolar epithelial cell (A549 cell line) proteins on polyacrylamide gels, blotting on nitrocellulose membranes, and incubating with serum from patients with IPF (n = 40) or healthy subjects (n = 40). Proteomic analysis and mass spectrometry characterized the target protein. Inhibition experiments performed with the correspondent recombinant protein confirmed our results. We identified IgG autoAbs recognizing a 200-kD protein in the serum of patients with IPF. Proteomic analysis identified this protein as human periplakin (PPL), a component of desmosomes. Anti-PPL Abs were found by immunoblot in both serum and bronchoalveolar lavage in patients with IPF: 16/40 (40%) of them were positive versus none of the control subjects. Immunohistochemistry revealed that PPL was strongly expressed in bronchial and alveolar epithelium, but that PPL exhibited changes in intracellular localization among normal and fibrotic alveolar epithelium. In an alveolar epithelial wound repair assay, an anti-PPL IgG decreased cell migration. Recombinant PPL induced bronchoalveolar lavage T lymphocyte proliferation. Patients with IPF with anti-PPL Abs had a more severe respiratory disease, despite no difference in survival. We found a new circulating autoAb directed against PPL in patients with IPF, associated with a more severe disease.
AbstractList	Injury to alveolar epithelial cells is central to the pathophysiology of idiopathic pulmonary fibrosis (IPF). An abnormal autoimmune response directed against antigens of the alveolar epithelium may contribute to the disease. To detect circulating autoantibodies (autoAbs) directed against epithelial structures. We performed immunoblot by separating human placental amnion extract or alveolar epithelial cell (A549 cell line) proteins on polyacrylamide gels, blotting on nitrocellulose membranes, and incubating with serum from patients with IPF (n = 40) or healthy subjects (n = 40). Proteomic analysis and mass spectrometry characterized the target protein. Inhibition experiments performed with the correspondent recombinant protein confirmed our results. We identified IgG autoAbs recognizing a 200-kD protein in the serum of patients with IPF. Proteomic analysis identified this protein as human periplakin (PPL), a component of desmosomes. Anti-PPL Abs were found by immunoblot in both serum and bronchoalveolar lavage in patients with IPF: 16/40 (40%) of them were positive versus none of the control subjects. Immunohistochemistry revealed that PPL was strongly expressed in bronchial and alveolar epithelium, but that PPL exhibited changes in intracellular localization among normal and fibrotic alveolar epithelium. In an alveolar epithelial wound repair assay, an anti-PPL IgG decreased cell migration. Recombinant PPL induced bronchoalveolar lavage T lymphocyte proliferation. Patients with IPF with anti-PPL Abs had a more severe respiratory disease, despite no difference in survival. We found a new circulating autoAb directed against PPL in patients with IPF, associated with a more severe disease. Injury to alveolar epithelial cells is central to the pathophysiology of idiopathic pulmonary fibrosis (IPF). An abnormal autoimmune response directed against antigens of the alveolar epithelium may contribute to the disease. To detect circulating autoantibodies (autoAbs) directed against epithelial structures. We performed immunoblot by separating human placental amnion extract or alveolar epithelial cell (A549 cell line) proteins on polyacrylamide gels, blotting on nitrocellulose membranes, and incubating with serum from patients with IPF (n = 40) or healthy subjects (n = 40). Proteomic analysis and mass spectrometry characterized the target protein. Inhibition experiments performed with the correspondent recombinant protein confirmed our results. We identified IgG autoAbs recognizing a 200-kD protein in the serum of patients with IPF. Proteomic analysis identified this protein as human periplakin (PPL), a component of desmosomes. Anti-PPL Abs were found by immunoblot in both serum and bronchoalveolar lavage in patients with IPF: 16/40 (40%) of them were positive versus none of the control subjects. Immunohistochemistry revealed that PPL was strongly expressed in bronchial and alveolar epithelium, but that PPL exhibited changes in intracellular localization among normal and fibrotic alveolar epithelium. In an alveolar epithelial wound repair assay, an anti-PPL IgG decreased cell migration. Recombinant PPL induced bronchoalveolar lavage T lymphocyte proliferation. Patients with IPF with anti-PPL Abs had a more severe respiratory disease, despite no difference in survival. We found a new circulating autoAb directed against PPL in patients with IPF, associated with a more severe disease. Injury to alveolar epithelial cells is central to the pathophysiology of idiopathic pulmonary fibrosis (IPF). An abnormal autoimmune response directed against antigens of the alveolar epithelium may contribute to the disease.RATIONALEInjury to alveolar epithelial cells is central to the pathophysiology of idiopathic pulmonary fibrosis (IPF). An abnormal autoimmune response directed against antigens of the alveolar epithelium may contribute to the disease.To detect circulating autoantibodies (autoAbs) directed against epithelial structures.OBJECTIVESTo detect circulating autoantibodies (autoAbs) directed against epithelial structures.We performed immunoblot by separating human placental amnion extract or alveolar epithelial cell (A549 cell line) proteins on polyacrylamide gels, blotting on nitrocellulose membranes, and incubating with serum from patients with IPF (n = 40) or healthy subjects (n = 40). Proteomic analysis and mass spectrometry characterized the target protein. Inhibition experiments performed with the correspondent recombinant protein confirmed our results.METHODSWe performed immunoblot by separating human placental amnion extract or alveolar epithelial cell (A549 cell line) proteins on polyacrylamide gels, blotting on nitrocellulose membranes, and incubating with serum from patients with IPF (n = 40) or healthy subjects (n = 40). Proteomic analysis and mass spectrometry characterized the target protein. Inhibition experiments performed with the correspondent recombinant protein confirmed our results.We identified IgG autoAbs recognizing a 200-kD protein in the serum of patients with IPF. Proteomic analysis identified this protein as human periplakin (PPL), a component of desmosomes. Anti-PPL Abs were found by immunoblot in both serum and bronchoalveolar lavage in patients with IPF: 16/40 (40%) of them were positive versus none of the control subjects. Immunohistochemistry revealed that PPL was strongly expressed in bronchial and alveolar epithelium, but that PPL exhibited changes in intracellular localization among normal and fibrotic alveolar epithelium. In an alveolar epithelial wound repair assay, an anti-PPL IgG decreased cell migration. Recombinant PPL induced bronchoalveolar lavage T lymphocyte proliferation. Patients with IPF with anti-PPL Abs had a more severe respiratory disease, despite no difference in survival.MEASUREMENTS AND MAIN RESULTSWe identified IgG autoAbs recognizing a 200-kD protein in the serum of patients with IPF. Proteomic analysis identified this protein as human periplakin (PPL), a component of desmosomes. Anti-PPL Abs were found by immunoblot in both serum and bronchoalveolar lavage in patients with IPF: 16/40 (40%) of them were positive versus none of the control subjects. Immunohistochemistry revealed that PPL was strongly expressed in bronchial and alveolar epithelium, but that PPL exhibited changes in intracellular localization among normal and fibrotic alveolar epithelium. In an alveolar epithelial wound repair assay, an anti-PPL IgG decreased cell migration. Recombinant PPL induced bronchoalveolar lavage T lymphocyte proliferation. Patients with IPF with anti-PPL Abs had a more severe respiratory disease, despite no difference in survival.We found a new circulating autoAb directed against PPL in patients with IPF, associated with a more severe disease.CONCLUSIONSWe found a new circulating autoAb directed against PPL in patients with IPF, associated with a more severe disease.
Author	Tubach, Florence Crestani, Bruno Taillé, Camille Mailleux, Arnaud Fagart, Jérôme Boursier, Céline Marchal-Sommé, Joëlle Chollet-Martin, Sylvie Soler, Paul Grootenboer-Mignot, Sabine Cigna, Natacha Michel, Laurence Barrientos, Lorena Debray, Marie-Pierre
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Keywords	Autoimmunity Lung disease Intensive care Pulmonary fibrosis periplakin Respiratory disease Idiopathic desmosomes Resuscitation
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Snippet	Injury to alveolar epithelial cells is central to the pathophysiology of idiopathic pulmonary fibrosis (IPF). An abnormal autoimmune response directed against...
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SubjectTerms	Adult Aged Anesthesia. Intensive care medicine. Transfusions. Cell therapy and gene therapy Antibodies Antigens Autoantibodies - blood Autoimmunity Biological and medical sciences Biomarkers - blood Case-Control Studies Cell adhesion & migration Chronic obstructive pulmonary disease Connective tissue Experiments Female Humans Idiopathic Pulmonary Fibrosis - blood Idiopathic Pulmonary Fibrosis - immunology Idiopathic Pulmonary Fibrosis - physiopathology Immunoglobulin G - blood Intensive care medicine Lavage Lung diseases Male Mass spectrometry Medical sciences Middle Aged Pathophysiology Plakins - blood Pneumology Proteins Pulmonary fibrosis Pulmonary hypertension. Acute cor pulmonale. Pulmonary embolism. Pulmonary vascular diseases Respiratory Mucosa - immunology Scientific imaging Severity of Illness Index
Title	Identification of Periplakin as a New Target for Autoreactivity in Idiopathic Pulmonary Fibrosis
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