TY - JOUR
T1 - Novel insights in fibrotic pulmonary sarcoidosis
AU - Comes, Alessia
AU - Sofia, Carmelo
AU - Richeldi, Luca
PY - 2022
Y1 - 2022
N2 - Purpose of review In chronic pulmonary sarcoidosis, the transition from the inflammatory to the fibrotic stage of the lungs occurs in about 10-20% of cases, eventually causing end-stage fibrotic disease. To date, pathogenetic mechanisms and clinical management remain challenging; thus, we highlight the recent evidence in pulmonary fibrotic processes, clinical signs for an early detection and the potential role of the current investigated antifibrotic agents and promising targeted therapies. Recent findings Recent findings of relevant key cellular pathways can be considered as a glimmer of light in the complexity of sarcoidosis. In some patients, granulomas persist and serve as a nidus for fibrosis growth, sustained by several fibrosis-stimulating cytokines. Preclinical studies have detected profibrotic, antifibrotic and pleiotropic T cells as promoters of fibrosis. Epigenetics, genetics and transcriptomics research can lead to new target therapies. Antifibrotic drug nintedanib has shown a positive effect on non-idiopathic pulmonary fibrosis fibrotic lung diseases including fibrotic sarcoidosis; other antifibrotic drugs are under investigation. Pulmonary fibrosis strongly impacts the outcome of sarcoidosis, and a better understanding of the underlying pathogenic mechanisms can facilitate the development of novel treatments, improving clinical care and life expectancy of these patients. The greatest challenge is to investigate effective antifibrotic therapies once fibrosis develops. The role of these findings in fibrotic sarcoidosis can be translated into other interstitial lung diseases characterized by the coexistence of inflammatory and fibrotic processes.
AB - Purpose of review In chronic pulmonary sarcoidosis, the transition from the inflammatory to the fibrotic stage of the lungs occurs in about 10-20% of cases, eventually causing end-stage fibrotic disease. To date, pathogenetic mechanisms and clinical management remain challenging; thus, we highlight the recent evidence in pulmonary fibrotic processes, clinical signs for an early detection and the potential role of the current investigated antifibrotic agents and promising targeted therapies. Recent findings Recent findings of relevant key cellular pathways can be considered as a glimmer of light in the complexity of sarcoidosis. In some patients, granulomas persist and serve as a nidus for fibrosis growth, sustained by several fibrosis-stimulating cytokines. Preclinical studies have detected profibrotic, antifibrotic and pleiotropic T cells as promoters of fibrosis. Epigenetics, genetics and transcriptomics research can lead to new target therapies. Antifibrotic drug nintedanib has shown a positive effect on non-idiopathic pulmonary fibrosis fibrotic lung diseases including fibrotic sarcoidosis; other antifibrotic drugs are under investigation. Pulmonary fibrosis strongly impacts the outcome of sarcoidosis, and a better understanding of the underlying pathogenic mechanisms can facilitate the development of novel treatments, improving clinical care and life expectancy of these patients. The greatest challenge is to investigate effective antifibrotic therapies once fibrosis develops. The role of these findings in fibrotic sarcoidosis can be translated into other interstitial lung diseases characterized by the coexistence of inflammatory and fibrotic processes.
KW - Humans
KW - Lung
KW - Lung Diseases, Interstitial
KW - Pulmonary Fibrosis
KW - Sarcoidosis
KW - Sarcoidosis, Pulmonary
KW - antifibrotic therapy
KW - fibrotic sarcoidosis
KW - interstitial lung diseases
KW - pulmonary fibrosis
KW - sarcoidosis
KW - Humans
KW - Lung
KW - Lung Diseases, Interstitial
KW - Pulmonary Fibrosis
KW - Sarcoidosis
KW - Sarcoidosis, Pulmonary
KW - antifibrotic therapy
KW - fibrotic sarcoidosis
KW - interstitial lung diseases
KW - pulmonary fibrosis
KW - sarcoidosis
UR - http://hdl.handle.net/10807/219688
U2 - 10.1097/MCP.0000000000000893
DO - 10.1097/MCP.0000000000000893
M3 - Editorial
SN - 1070-5287
VL - 28
SP - 478
EP - 484
JO - Current Opinion in Pulmonary Medicine
JF - Current Opinion in Pulmonary Medicine
ER -