Abstract 2204P
Background
Malignant pleural mesothelioma (MPM) is a rare thoracic malignancy with bad prognosis. Asbestos exposure has been described as the main risk factor with a key role in its pathogenesis. The aim of this study is to identify the impact of systemic inflammation biomarkers as clinical prognostic factors for MPM.
Methods
Patients (pts) diagnosed of MPM from 2004 to 2023 from a Medical Oncology Intercenter Unit in Malaga (Spain) were enrolled. We analyzed epidemiologic, clinical and pathological characteristics and correlated them with survival outcomes.
Results
Among the 140 pts, median age was 70 years (range 23-94), ECOG 0-1 in 76,4% (n=104), mainly males (70,7%, n=99). 95 pts (67,9%) were epithelioid subtype. Median follow up was 21,6 months (mo) (range 1-217). Median overall survival (OS) 13,5 mo (CI 95% 9,6-17,4), progression-free survival (PFS) 10,1 mo (CI 95% 7,2-13). 19 pts (13,6%) were considered for surgery. In non-resectable pts (n=121, 86,4%), age over 65, malnutrition and ECOG 2-4 at diagnosis were associated to poor OS (21,6 mo CI95% 14,4-28,8; 7,1 mo, CI95% 5,8-8,2; 4,7 mo, CI95% 3-6,5 respectively). Inflammatory biomarkers including high LDH or CRP, neutrophilia, Lung Immune Prognostic Index (LIPI) intermediate-poor, and high dNLR suggested a trend towards poor survival (9,5 mo CI 95% 3,5-15,4; 8,5 mo CI 95% 4,5-12,5; 7,1 mo CI 95% 1,5-3,9; 9,5 mo CI95% 4,5-14,4; 9,5 mo CI95% 4,8-14, respectively; p>0.5). Anemia, moderate-to-severe value of neutrophil to lymphocyte ratio (NLR≥6) and not receiving immunotherapy were significantly associated with worse prognosis. Multivariate analysis showed age and NLR value as independent prognostic factors (p<0.01).
Conclusions
Host inflammation status at diagnosis may be a subrogate biomarker of survival for MPM, even for pts not receiving immunotherapy. Modulating the immune system and inflammatory pathways appear as promising strategies for increasing effectiveness in MPM treatment. Table: 2204P
Univariate analysis | Multivariate analysis | |||||
HR | CI 95% | P | HR | CI 95% | P | |
Age ≤65 | 0,56 | 0,36-0,88 | 0,01 | 0,44 | 0,23-0,82 | 0,01 |
ECOG | 1,65 | 1,3-2,6 | 0,00 | - | - | 0,37 |
Malnutrition | 0,47 | 0,29-0,74 | 0,00 | - | - | 0,78 |
Anemia | 9,86 | 0,76-0,96 | 0,01 | - | - | 0,29 |
High C reactive protein | 1,87 | 0,77-4,52 | 0,16 | - | - | - |
Neutrophilia | 2,38 | 0,31-18,41 | 0,40 | - | - | - |
High LDH | 1,47 | 0,93-2,34 | 0,09 | - | - | - |
NLR (absent-mild vs moderate severe) | 0,5 | 0,28-0,90 | 0,02 | 0,30 | 0,14-0,61 | 0,00 |
dLNR (high vs normal) | 0,91 | 0,58-1,42 | 0,69 | - | - | - |
LIPI score (good vs intermediate-poor) | 1,47 | 0,96-2,27 | 0,07 | - | - | - |
Immunotherapy | 0,48 | 0,24-0,96 | 0,04 | - | - | 0,62 |
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
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