1.300.000 Amerikalı’nın Romatoid artritten muzdarip olduğu tahmin edilmektedir.
Araştırmacılar ilk kez bir anti-fibrotik ilaç sınıfının romatoid artritli (RA) kişilerde interstisyel akciğer hastalığının (ILD) ilerlemesini engellediğini gösterdi. Kısmen Ulusal Yahudi Sağlığında yürütülen araştırmaya göre, pirfenidonun bu kişilerde güvenli ve etkili olduğu gösterildi. Bu ayın başlarında dergide yayınlanan araştırma
Rheumatoid arthritis (RA) is one of the most common autoimmune diseases in the world. The treatment for Rheumatoid Arthritis and Interstitial Lung Disease 1 (TRIAL1) was a randomized, double-blind, placebo-controlled phase 2 trial done in 34 academic centers specializing in ILD across four countries. Patients with RA-ILD were treated for 52 weeks with either pirfenidone, an anti-scarring medication, or a placebo.
The COVID-19 pandemic prevented trial participant enrollment goals from being reached, but the results showed that pirfenidone was safe, well tolerated, and slowed down the rate of progression of lung fibrosis over a year. This was the first and only prospective multi-centered international interventional treatment trial focused on RA-ILD.
While the trial was foreshortened because of recruitment challenges during the pandemic, the intervention appeared safe and in context, slowed the rate of forced vital capacity (FVC) decline; as FVC decline is associated with early mortality, slowing the decline may be associated with longer life.
“With this study, we are demonstrating that anti-fibrotics as a class of medications have a reproducible effect in reducing the rate of disease progression when measured by force vital capacity,” said Dr. Ivan Rosas, corresponding author of the paper, and professor of medicine and section chief of pulmonary, critical care and sleep medicine at Baylor College of Medicine. “This could have an impact on the overall survival of these patients.”
Reference: “Safety, tolerability, and efficacy of pirfenidone in patients with rheumatoid arthritis-associated interstitial lung disease: a randomised, double-blind, placebo-controlled, phase 2 study” by Joshua J. Solomon, MD, Sonye K. Danoff, MD, Felix A. Woodhead, MD, Shelley Hurwitz, Ph.D., Rie Maurer, MD, Ian Glaspole, MD, Professor Paul F. Dellaripa, MD, Professor Bibek Gooptu, MD, Professor Robert Vassallo, MD, Professor P. Gerard Cox, MB, Professor Kevin R. Flaherty, MD, Huzaifa I. Adamali, MD, Michael A. Gibbons, MD, Lauren Troy, MD, Ian A. Forrest, MD, Professor Joseph A. Lasky, MD, Lisa G. Spencer, MD, Professor Jeffrey Golden, MD, Mary Beth Scholand, MD, Nazia Chaudhuri, MD, Mark A. Perrella, MD, Professor David A. Lynch, MB BCh, Professor Daniel C. Chambers, MD, Professor Martin Kolb, MD, Professor Cathie Spino, ScD, Professor Ganesh Raghu, MD, Hilary J. Goldberg, MD and Professor Ivan O. Rosas, for the TRAIL1 Network Investigators, 5 September 2022, The Lancet Respiratory Medicine.
DOI: 10.1016/S2213-2600(22)00260-0