One major subgroup of patients with interstitial lung disease (ILD) arising from polymyositis/dermatomyositis (PM/DM) survived significantly longer when serum levels of interferon-λ3 were relatively low, researchers found.
Some 70% of patients in this subgroup showing serum interferon-λ3 above 120 pg/mL at baseline -- the median among the 52 patients in this analysis -- remained alive 6 months later, compared with 90% of those with lower levels (P=0.049), according to Tomoyuki Fujisawa, MD, PhD, of Hamamatsu University in Japan, and colleagues. The survival difference was even greater in a separate, smaller cohort.
This PM/DM-ILD subgroup is defined by the presence of anti-melanoma differentiation-associated gene 5 (MDA5) autoantibodies; previous studies had shown that this form of the disease is clinically distinct from others, Fujisawa and colleagues explained in their report .
In their new study, involving a total of 221 PM/DM-ILD patients, elevated interferon-λ3 was seen only in the roughly 35% with anti-MDA5 antibodies. Survival in this group was worst among those older than 53 and with partial arterial oxygen pressure (PaO2) below 75 mm Hg.
Fujisawa's group got interested in interferon-λ3 in the context of PM/DM-ILD after seeing numerous reports that this cytokine was elevated in a variety of other autoimmune diseases including rheumatoid arthritis, lupus, and systemic sclerosis. Because it's believed to modulate immune activity at the epithelial barrier, it made sense that it might play a role in autoimmune ILD. However, no previous studies had examined interferon-λ3 in PM/DM patients.
The researchers initially analyzed a cohort of 155 PM/DM patients with ILD who had been treated at Hamamatsu University's medical center. Of these, 52 were positive for anti-MDA5 antibodies; most of the rest instead carried antibodies against aminoacyl-tRNA synthetase (ARS). Median follow-up after baseline testing was 49 months. Fujisawa and colleagues also examined a separate group (validation cohort) of 66 PM/DM-ILD patients, among whom 41% were positive for anti-MDA5 antibodies and who had median follow-up of 30 months.
Median patient age was 59 across both cohorts, and two-thirds were women. The disease was considered acute in some 30%, subacute in 30%, and chronic in 40%.
Interestingly, all the deaths in both cohorts occurred within the first 5 months of follow-up, even though observation continued for several years in both groups. Just under 20% of the validation cohort with interferon-λ3 levels below 120 pg/mL at baseline died, compared with fully half of those with higher levels. None of the patients with anti-ARS antibodies or those lacking any known autoantibodies had detectable levels of interferon-λ3.
Each 10-pg/mL increment in interferon-λ3 was associated with a 4.5% increase in mortality risk after adjustment for covariates (P=0.01). Age was also a factor, with a 9.5% increase in mortality for each additional year of age (P=0.004).
Among 17 patients older than 53, with interferon-λ3 at 120 pg/mL or higher, and PaO2 below 75 mm Hg, almost 80% died within 5 months. In contrast, mortality among patients with two of these characteristics but not all three (n=26) was about 25%.
Fujisawa and colleagues refrained from speculating on whether interferon-λ3 might represent a therapeutic target as well as a diagnostic marker. They did, however, call for prospective studies to better understand the connection between interferon-λ3 and ILD and to confirm the biomarker's potential as a clinically useful prognostic indicator. Further research could also identify the most appropriate cutoff values for decision-making.
Limitations to the study included the relatively small numbers of patients and the lack of testing for other possible influences such as other interferon species. Also, interferon-λ3 levels were measured only once in each patient, and thus the potential for variability over time was not examined.
Disclosures
Funding for the study was provided by the Japan Society for the Promotion of Science. Several co-authors reported extensive relationships with pharmaceutical companies.
Primary Source
Arthritis & Rheumatology
Fukada A, et al "Prognostic role of interferon-lambda 3 in anti-MDA5–positive dermatomyositis-associated ILD" Arthritis Rheumatol 2023; DOI: 10.1002/art.42785.