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Abstract Number: 2030

Krebs von den Lungen 6 levels (∆KL6) is a reliable marker of disease activity and response to therapy in CTD-ILD

fredeswinda Romero-Bueno1, lydia Abasolo Alcazar2, Mª Jesus Rodriguez-Nieto3, Cristina Vadillo Font4, Maria asuncion Nieto4, Laura Cebrian5, Belen Lopez Muñiz6, Jesus Loarce Martos7, Juan A Rigual7, Hilda Godoy Tundidor8, Rosalia Laporta9, Irene Llorente Cubas10, Gema Bonilla11, Luis Gomez Carrera12, Rosario Garcia Vicuña13, Ana Jaureguizar7, Jose Luis Morell Hita7, Claudia Valenzuela10 and Olga Sanchez Pernaute14, 1University Hospital Fundación Jiménez Díaz"", Madrid, Spain, 2IdISSC. HCSC, Madrid, Madrid, Spain, 3Fundacion Jimenez Diaz (IIS-HUFJD), Madrid, Spain, 4Hospital Clínico S Carlos, Madrid, Spain, 5Department of Rheumatology, Hospital Universitario Infanta Leonor / Universidad Complutense de Madrid, Madrid, Spain, Madrid, Spain, 6Hospital Universitario Infanta Leonor, Madrid, Spain, 7Hospital Ramón y Cajal, Madrid, Spain, 8Hospital Universitario puerta de hierro, Madrid, Spain, 9Hospital Puerta de Hierro Majadahonda, Madrid, Spain, 10Hospital Universitario Princesa, Madrid, Spain, 11Hospital Universitario La Paz, Rheumatology, Madrid, Madrid, Spain, 12Hospital Universitario La Paz, Madrid, Spain, 13Hospital Universitario de la Princesa, Madrid, Spain, 14Clinica Universidad de Navarra, Madrid, Madrid, Spain

Meeting: ACR Convergence 2025

Keywords: autoimmune diseases, Biomarkers, interstitial lung disease, pulmonary

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Session Information

Date: Tuesday, October 28, 2025

Title: (2015–2051) Miscellaneous Rheumatic & Inflammatory Diseases Poster III

Session Type: Poster Session C

Session Time: 10:30AM-12:30PM

Background/Purpose: Krebs von den Lungen-6 (KL6) is produced by type 2 alveolar epithelial cells. High circulating KL6 levels show a good accuracy in the diagnosis of interstitial lung diseases, including those associated to CTD (CTD-ILD). Increased levels of KL6 have been found to predict mortality in idiopathic pulmonary fibrosis, and also in some cohorts of CTD-ILD patients. Previous data from our prospective CTD-ILD cohort have shown that KL6 changes over time correlate with disease course. Our aim was to evaluate KL-6 sensitivity to change upon different therapeutic interventions

Methods: The study was conducted in CTD-ILD patients included in a multicenter prospective register (NEREA) from Madrid. Demographics and process related variables are recorded and updated with clinical visits (at 6-monthly periods on average). For the aim of the study we selected treatment-naïve incident cases and extracted data regarding underlying disease, date of ILD onset, radiographic patterns, presence of fibrosis at the time of first KL6 determination, FVC (% from reference) and DLco (% from reference). Serum KL-6 concentrations were measured at baseline (blKL-6) and within the following 6 to 24 months (fuKL-6). Changes in KL6 levels (∆KL6%) were also determined. Data are shown as mean ± SD. 95% confident intervals (95CI) were calculated to assess the effect size. Statistical analysis included t test, Wilcoxon rank sum and linear regression. Alpha value was set at 0.05.

Results: The study population comprised 57 subjects (84% women), aged 64.7 ± 10.4 years. There were 25 never smokers (44% of the cohort) and only 3 active smokers. Clinical diagnosis included 24 IPAF cases (42%), 12 patients with SSc or related conditions (21%), 4 with RA (7%), and 4 classified as PM/DM (7%), 3 with SS/lupus (5%) and 10 with other autoimmune conditions (17.5%). Radiographic patterns were classified as NSIP in 18 patients (31%), UIP in 22 (39%), and others in 17 (30%). Signs of fibrotic disease were observed in 34 patients (60%). FVC at baseline was 82±21%, while DLco was 64±25%, with 30 patients (53%) showing DLco > 60%. 26 patients (45.6%) remained untreated during the observation period, while 31 patients (54.4%) were put on immunossupressants or/and corticosteroids related to ILD. At baseline, KL-6 levels (blKL-6) were 2029 ± 2118 IU/ml (median 1512 IU/ml). A second KL6 determination (fuKL6) was availble at a median of 11.7 (6-12) months of follow-up. Patients treated with immunosuppresants showed a significant reduction in KL6 levels as compared to those remaining untreated (∆KL6is%: -22.1 ± 38 [95CI: -39.1; -8.2] vs ∆KL60: 9.0 ± 46.8 [95CI: -9.9; -27.9], p 0.001). After adjustment by age and sex, treatment with immunosupressants resulted in a risk reduction of KL6 increasing over time (+∆KL6) of 25.9 ± 11.7 [95CI: 2.5; 49.3] vs no treatment (p 0.031). After adjustment for sex and age, treatment initiation was associated with a 22.0 ± 9.7 risk reduction [95CI: 2.7; 41.4] of a +∆KL6

Conclusion: Our results support the role of KL6 as activity biomarker in CTD-ILD, and underscore its value as surrogate marker of reponse to immunosuppresants both in interventional trials and in clinical practice.


Disclosures: f. Romero-Bueno: None; l. Abasolo Alcazar: None; M. Rodriguez-Nieto: None; C. Vadillo Font: None; M. Nieto: None; L. Cebrian: None; B. Lopez Muñiz: None; J. Loarce Martos: None; J. A Rigual: None; H. Godoy Tundidor: None; R. Laporta: None; I. Llorente Cubas: None; G. Bonilla: None; L. Gomez Carrera: None; R. Garcia Vicuña: None; A. Jaureguizar: None; J. Morell Hita: None; C. Valenzuela: None; O. Sanchez Pernaute: None.

To cite this abstract in AMA style:

Romero-Bueno f, Abasolo Alcazar l, Rodriguez-Nieto M, Vadillo Font C, Nieto M, Cebrian L, Lopez Muñiz B, Loarce Martos J, A Rigual J, Godoy Tundidor H, Laporta R, Llorente Cubas I, Bonilla G, Gomez Carrera L, Garcia Vicuña R, Jaureguizar A, Morell Hita J, Valenzuela C, Sanchez Pernaute O. Krebs von den Lungen 6 levels (∆KL6) is a reliable marker of disease activity and response to therapy in CTD-ILD [abstract]. Arthritis Rheumatol. 2025; 77 (suppl 9). https://acrabstracts.org/abstract/krebs-von-den-lungen-6-levels-%e2%88%86kl6-is-a-reliable-marker-of-disease-activity-and-response-to-therapy-in-ctd-ild/. Accessed .
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