Robert P Baughman,Jan C Grutters,Elyse E Lower,Ying Zhou,Marlies Wijsenbeek,Athol U Wells,Marcel Veltkamp,Dominique Valeyre,Paolo Spagnolo,Michelle Sharp,Jacobo Sellares,Ogugua N Obi,Hilario Nunes,Marc A Judson,Daniel A Culver,Francesco Bonella,Arata Azuma,Ingrid H E Korenromp
{"title":"肺结节病临床试验终点:德尔菲研究。","authors":"Robert P Baughman,Jan C Grutters,Elyse E Lower,Ying Zhou,Marlies Wijsenbeek,Athol U Wells,Marcel Veltkamp,Dominique Valeyre,Paolo Spagnolo,Michelle Sharp,Jacobo Sellares,Ogugua N Obi,Hilario Nunes,Marc A Judson,Daniel A Culver,Francesco Bonella,Arata Azuma,Ingrid H E Korenromp","doi":"10.1183/13993003.00943-2025","DOIUrl":null,"url":null,"abstract":"BACKGROUND\r\nCorticosteroids (CS), the most commonly prescribed treatment for sarcoidosis, are associated with significant toxicity, especially with long term usage. New intervention trials designed to reduce or eliminate CS require pertinent and precise clinical trial endpoints. However, consensus is lacking. The aim of the current study is to develop consensus for trial endpoints in pulmonary sarcoidosis.\r\n\r\nMETHODS\r\nA Delphi survey was developed by an Expert Panel of 30 sarcoidosis investigators. For Round 1, the panel created 97 statements regarding potential endpoints for a clinical trial of symptomatic pulmonary CS treated sarcoidosis patients. After anonymous voting in Round 2, the 97 statements were refined by all Stakeholders, including the Expert Panel and an additional 70 individuals interested in sarcoidosis therapies.\r\n\r\nRESULTS\r\nAfter Round 2, the Expert Panel achieved consensus for combination endpoints and 38 statements across six domains that supported the following endpoints: prednisone reduction by 50% or discontinuation, 10% predicted or greater improvement in FVC%, FEV1%, and DLCO% predicted, and improvement in the Kings Sarcoidosis Questionnaire (KSQ)-Lung and KSQ-General Health. Additionally, the majority of Stakeholders agreed to all statements which reached consensus by the Expert Panel.\r\n\r\nCONCLUSIONS\r\nUtilizing the Delphi technique, international sarcoidosis experts successfully achieved consensus for 38 specific clinical trial endpoints which can be utilized in the development of novel steroid-sparing and eliminating therapies for pulmonary sarcoidosis.","PeriodicalId":12265,"journal":{"name":"European Respiratory Journal","volume":"103 1","pages":""},"PeriodicalIF":21.0000,"publicationDate":"2025-08-07","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Pulmonary Sarcoidosis Clinical Trial Endpoints: A Delphi Study.\",\"authors\":\"Robert P Baughman,Jan C Grutters,Elyse E Lower,Ying Zhou,Marlies Wijsenbeek,Athol U Wells,Marcel Veltkamp,Dominique Valeyre,Paolo Spagnolo,Michelle Sharp,Jacobo Sellares,Ogugua N Obi,Hilario Nunes,Marc A Judson,Daniel A Culver,Francesco Bonella,Arata Azuma,Ingrid H E Korenromp\",\"doi\":\"10.1183/13993003.00943-2025\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"BACKGROUND\\r\\nCorticosteroids (CS), the most commonly prescribed treatment for sarcoidosis, are associated with significant toxicity, especially with long term usage. New intervention trials designed to reduce or eliminate CS require pertinent and precise clinical trial endpoints. However, consensus is lacking. The aim of the current study is to develop consensus for trial endpoints in pulmonary sarcoidosis.\\r\\n\\r\\nMETHODS\\r\\nA Delphi survey was developed by an Expert Panel of 30 sarcoidosis investigators. For Round 1, the panel created 97 statements regarding potential endpoints for a clinical trial of symptomatic pulmonary CS treated sarcoidosis patients. After anonymous voting in Round 2, the 97 statements were refined by all Stakeholders, including the Expert Panel and an additional 70 individuals interested in sarcoidosis therapies.\\r\\n\\r\\nRESULTS\\r\\nAfter Round 2, the Expert Panel achieved consensus for combination endpoints and 38 statements across six domains that supported the following endpoints: prednisone reduction by 50% or discontinuation, 10% predicted or greater improvement in FVC%, FEV1%, and DLCO% predicted, and improvement in the Kings Sarcoidosis Questionnaire (KSQ)-Lung and KSQ-General Health. 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Pulmonary Sarcoidosis Clinical Trial Endpoints: A Delphi Study.
BACKGROUND
Corticosteroids (CS), the most commonly prescribed treatment for sarcoidosis, are associated with significant toxicity, especially with long term usage. New intervention trials designed to reduce or eliminate CS require pertinent and precise clinical trial endpoints. However, consensus is lacking. The aim of the current study is to develop consensus for trial endpoints in pulmonary sarcoidosis.
METHODS
A Delphi survey was developed by an Expert Panel of 30 sarcoidosis investigators. For Round 1, the panel created 97 statements regarding potential endpoints for a clinical trial of symptomatic pulmonary CS treated sarcoidosis patients. After anonymous voting in Round 2, the 97 statements were refined by all Stakeholders, including the Expert Panel and an additional 70 individuals interested in sarcoidosis therapies.
RESULTS
After Round 2, the Expert Panel achieved consensus for combination endpoints and 38 statements across six domains that supported the following endpoints: prednisone reduction by 50% or discontinuation, 10% predicted or greater improvement in FVC%, FEV1%, and DLCO% predicted, and improvement in the Kings Sarcoidosis Questionnaire (KSQ)-Lung and KSQ-General Health. Additionally, the majority of Stakeholders agreed to all statements which reached consensus by the Expert Panel.
CONCLUSIONS
Utilizing the Delphi technique, international sarcoidosis experts successfully achieved consensus for 38 specific clinical trial endpoints which can be utilized in the development of novel steroid-sparing and eliminating therapies for pulmonary sarcoidosis.
期刊介绍:
The European Respiratory Journal (ERJ) is the flagship journal of the European Respiratory Society. It has a current impact factor of 24.9. The journal covers various aspects of adult and paediatric respiratory medicine, including cell biology, epidemiology, immunology, oncology, pathophysiology, imaging, occupational medicine, intensive care, sleep medicine, and thoracic surgery. In addition to original research material, the ERJ publishes editorial commentaries, reviews, short research letters, and correspondence to the editor. The articles are published continuously and collected into 12 monthly issues in two volumes per year.