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Abstract
Aims Given the time, expense and clinical expertise required for a myelodysplastic syndrome (MDS) diagnosis, there is a clear need for a cost-effective screening laboratory test that can rapidly and accurately distinguish patients with cytopenias related to MDS from other causes.
Methods We measured conventional and research use only complete blood cell (CBC) parameters using the Sysmex XN-series haematology analyser in 102 MDS patients (70 patients with active MDS and 32 patients in remission), 43 patients with cytopenia without morphological evidence of MDS and 484 age-adjusted controls. A variety of algorithms, including random forest machine learning, were used to construct parameter-based models to predict the presence of MDS using both CBC and molecular data or CBC data alone and correlated individual pathogenic variants/genetic pathways with CBC parameters changes.
Results Using the CBC parameters alone, our predictive model for active MDS showed a 0.86 receiver operating characteristic curve (ROC)/area under the ROC curve (AUC), with 0.87 sensitivity and 0.72 specificity; with the addition of the molecular and demographic status, the ROC/AUC improved to 0.93, sensitivity to 0.89 and specificity to 0.84. The most discriminatory MDS parameters were reflective of dysplastic neutrophil morphology, red cell count fragmentation and degree of platelet immaturity. Specific patterns of parameters were associated with individual gene pathogenic variants or affected pathways.
Conclusions CBC research parameters can be used as an adjunct to the haematological workup of cytopenia(s) to help screen for patients with high likelihood of MDS.
- hematology
- myelodysplastic syndromes
- information technology
- cell count
- morphological and microscopic findings
Data availability statement
All data relevant to the study are included in the article or uploaded as online supplemental information.
Statistics from Altmetric.com
- hematology
- myelodysplastic syndromes
- information technology
- cell count
- morphological and microscopic findings
Data availability statement
All data relevant to the study are included in the article or uploaded as online supplemental information.
Footnotes
Handling editor Tahir S Pillay.
Contributors OP and AK: designed the study, collected data, performed analyses and wrote the paper; RSN and TK: designed statistical platform and performed analyses; LG, NR and DB: collected data. OP is acting as guarantor.
Funding This work was supported through a research grant from Sysmex America.
Disclaimer This financial support had no influence on the interpretation of the results or findings stated by the authors.
Competing interests None declared.
Provenance and peer review Not commissioned; externally peer reviewed.
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