Assessing the Relevance of Non-Molecular Prognostic Systems for Myelodysplastic Syndrome in the Era of Next-Generation Sequencing

Marco LINCANGO; Verónica ANDREOLI; Hernán García RIVELLO; Andrea BENDER; Ana I CATALÁN; Marilina RAHHAL; Rocío DELAMER; Mariana ASINARI; Adrián Mosquera ORGUEIRA; María Belén CASTRO; María José Mela OSORIO; Alicia NAVICKAS; Sofia GRILLE; Evangelina AGRIELLO; Jorge ARBELBIDE; Ana Lisa BASQUIERA; Carolina B BELLI

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Assessing the Relevance of Non-Molecular Prognostic Systems for Myelodysplastic Syndrome in the Era of Next-Generation Sequencing

Author: Marco LINCANGO ¹ ; Verónica ANDREOLI ; Hernán García RIVELLO ; Andrea BENDER ; Ana I CATALÁN ; Marilina RAHHAL ; Rocío DELAMER ; Mariana ASINARI ; Adrián Mosquera ORGUEIRA ; María Belén CASTRO ; María José Mela OSORIO ; Alicia NAVICKAS ; Sofia GRILLE ; Evangelina AGRIELLO ; Jorge ARBELBIDE ; Ana Lisa BASQUIERA ; Carolina B BELLI
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1. Laboratorio de Genética Hematológica, Instituto de Medicina Experimental (IMEX–CONICET)/Academia Nacional de Medicina, Ciudad de Buenos Aires, Argentina
Publication Type:Original Article
From:Annals of Laboratory Medicine 2025;45(1):44-52
CountryRepublic of Korea
Language:English
Abstract: Background:The Molecular International Prognostic Scoring System (IPSS-M) has improved the prediction of clinical outcomes for myelodysplastic syndromes (MDS). The Artificial Intelligence Prognostic Scoring System for MDS (AIPSS-MDS), based on classical clinical parameters, has outperformed the IPSS, revised version (IPSS-R). For the first time, we validated the IPSS-M and other molecular prognostic models and compared them with the established IPSS-R and AIPSS-MDS models using data from South American patients.
Methods:Molecular and clinical data from 145 patients with MDS and 37 patients with MDS/myeloproliferative neoplasms were retrospectively analyzed.
Results:Prognostic power evaluation revealed that the IPSS-M (Harrell’s concordance [C]-index: 0.75, area under the receiver operating characteristic curve [AUC]: 0.68) predicted overall survival better than the European MDS (EuroMDS; C-index: 0.72, AUC: 0.68) and Munich Leukemia Laboratory (MLL) (C-index: 0.70, AUC: 0.64) models. The IPSS-M prognostic discrimination was similar to that of the AIPSS-MDS model (C-index: 0.74, AUC:0.66) and outperformed the IPSS-R model (C-index: 0.70, AUC: 0.61). Considering simplified low- and high-risk groups for clinical management, after restratifying from IPSS-R (57% and 32%, respectively, hazard ratio [HR]: 2.8; P = 0.002) to IPSS-M, 12.6% of patients were upstaged, and 5% were downstaged (HR: 2.9; P = 0.001). The AIPSS-MDS recategorized 51% of the low-risk cohort as high-risk, with no patients being downstaged (HR: 5.6;P < 0.001), consistent with most patients requiring disease-modifying therapy.
Conclusions:The IPSS-M and AIPSS-MDS models provide more accurate survival prognoses than the IPSS-R, EuroMDS, and MLL models. The AIPSS-MDS model is a valid option for assessing risks for all patients with MDS, especially in resource-limited centers where molecular testing is not currently a standard clinical practice.