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Anti-ceramide antibody and sphingosine-1-phosphate as potential biomarkers of unresectable non-small cell lung cancer
Bűdi, L. ✉ [Büdi, Lilla (Pulmonológia), author] Department of Pulmonology (SU / FM / C)
;
Hammer, D. [Hammer, Dániel (Pulmonológia), author] Department of Pulmonology (SU / FM / C)
;
Varga, R.
;
Müller, V. [Müller, Veronika (Pulmonológia), author] Department of Pulmonology (SU / FM / C)
;
Tárnoki, Á.D. [Tárnoki, Ádám Domonkos (radiológia), author] Orvosi Képalkotó Klinika (SU / FM / C)
;
Tárnoki, D.L. [Tárnoki, Dávid László (radiológia), author] Orvosi Képalkotó Klinika (SU / FM / C)
;
Mészáros, M. [Mészáros, Martina (Pulmonológia), author] Department of Pulmonology (SU / FM / C)
;
Bikov, A. [Bikov, András (Pulmonológia), author]
;
Horváth, P. [Horváth, Péter (Pulmonológia), author] Department of Pulmonology (SU / FM / C)
English Article (Journal Article) Scientific
Published:
PATHOLOGY AND ONCOLOGY RESEARCH 1219-4956 1532-2807
30
Paper: 1611929
, 10 p.
2024
SJR Scopus - Medicine (miscellaneous): Q2
Identifiers
MTMT: 35716050
DOI:
10.3389/pore.2024.1611929
WoS:
001399977700001
Scopus:
85215298487
PubMed:
39835329
Fundings:
(UNKP-20-5)
(ÚNKP-21-5)
(National Tumor Biology Laboratory, NLP-17) Funder: The Hungarian National Laboratories Excellence program
Subjects:
Respiratory systems
Objectives: Spingosine-1-phosphate (S1P) and ceramides are bioactive sphingolipids that influence cancer cell fate. Anti-ceramide antibodies might inhibit the effects of ceramide. The aim of this study was to assess the potential role of circulating S1P and anti-ceramide antibody as biomarkers in non-small cell lung cancer (NSCLC). Methods: We recruited 66 subjects (34 controls and 32 patients with NSCLC). Patient history and clinical variables were taken from all participants. Venous blood samples were collected to evaluate plasma biomarkers. If bronchoscopy was performed, bronchial washing fluid (BWF) was also analyzed. We measured the levels of S1P and anti-ceramide antibody with ELISA. Results: S1P levels were significantly higher in the NSCLC group (3770.99 ± 762.29 ng/mL vs. 366.53 ± 249.38 ng/mL, patients with NSCLC vs. controls, respectively, p < 0.001). Anti-ceramide antibody levels were significantly elevated in the NSCLC group (278.70 ± 19.26 ng/mL vs. 178.60 ± 18 ng/mL, patients with NSCLC vs. controls, respectively, p = 0.007). Age or BMI had no significant effect on anti-ceramide antibody or S1P levels. BWF samples had higher levels of anti-ceramide antibody (155.29 ± 27.58 ng/mL vs. 105.87 ± 9.99 ng/mL, patients with NSCLC vs. controls, respectively, p < 0.001). Overall survival (OS) was 13.36 months. OS was not affected by anti-ceramide antibody or S1P levels. Conclusion: Higher levels of S1P and anti-ceramide antibody were associated with active cancer. These results suggest that sphingolipid alterations might be important features of NSCLC. Copyright © 2025 Bűdi, Hammer, Varga, Müller, Tárnoki, Tárnoki, Mészáros, Bikov and Horváth.
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2025-04-25 10:59
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Citation styles:
IEEE
ACM
APA
Chicago
Harvard
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