Deep Learning-Based Blood Abnormalities Detection as a Tool for VEXAS Syndrome Screening

被引:0
|
作者
Braga, Cedric De Almeida [1 ]
Bauvais, Maxence [2 ]
Sujobert, Pierre [3 ]
Heiblig, Mael [4 ]
Jullien, Maxime [5 ]
Le Calvez, Baptiste [5 ]
Richard, Camille [2 ]
Le Roc'h, Valentin [2 ]
Rault, Emmanuelle [6 ]
Herault, Olivier [6 ]
Peterlin, Pierre [7 ]
Garnier, Alice [7 ]
Chevallier, Patrice [5 ,7 ]
Bouzy, Simon [2 ]
Le Bris, Yannick [2 ,3 ]
Neel, Antoine [8 ]
Graveleau, Julie [9 ]
Kosmider, Olivier [10 ]
Paul-Gilloteaux, Perrine [11 ]
Normand, Nicolas [1 ]
Eveillard, Marion [2 ,5 ]
机构
[1] Nantes Univ, Ecole Cent Nantes, Nantes, France
[2] Nantes Univ Hosp, Hematol Biol, Nantes, France
[3] Hop Lyon Sud, Hematol Biol, Hosp Civils Lyon, Pierre Benite, France
[4] Hop Lyon Sud, Hematol Clin, Hosp Civils Lyon, Pierre Benite, France
[5] Nantes Univ, CNRS, INSERM, CRCI2NA,U1307, F-44000 Nantes, France
[6] Tours Univ Hosp, Hematol Biol, Tours, France
[7] Nantes Univ Hosp, Hematol Clin, Nantes, France
[8] Nantes Univ Hosp, Internal Med, Nantes, France
[9] St Nazaire Gen Hosp, St Nazaire, France
[10] Hop Cochin, AP HP, Hematol Biol, Paris, France
[11] Nantes Univ, CHU Nantes, CNRS, Inserm,BioCore, Nantes, France
关键词
artificial intelligence; deep learning; multilabel classification; polymorphonuclears; VEXAS;
D O I
10.1111/ijlh.14368
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Introduction: VEXAS is a syndrome described in 2020, caused by mutations of the UBA1 gene, and displaying a large pleomorphic array of clinical and hematological features. Nevertheless, these criteria lack significance to discriminate VEXAS from other inflammatory conditions at the screening step. This work hence first focused on singling out dysplastic features indicative of the syndrome among peripheral blood (PB) polymorphonuclears (PMN). A deep learning algorithm is then proposed for automatic detection of these features. Methods: A multicentric dataset, comprising 9514 annotated PMN images was gathered, including UBA1 mutated VEXAS (n = 25), UBA1 wildtype myelodysplastic (n = 14), and UBA1 wildtype cytopenic patients (n = 25). Statistical analysis on a subset of patients was performed to screen for significant abnormalities. Detection of these features on PB was then automated with a convolutional neural network (CNN) for multilabel classification. Results: Significant differences were observed in the proportions of PMNs with pseudo-Pelger, nuclear spikes, vacuoles, and hypogranularity between patients with VEXAS and both cytopenic and myelodysplastic controls. Automatic detection of these abnormalities yielded AUCs in the range [0.85-0.97] and a F1-score of 0.70 on the test set. A VEXAS screening score was proposed, leveraging the model outputs and predicting the UBA1 mutational status with 0.82 sensitivity and 0.71 specificity on the test patients. Conclusion: This study suggests that computer-assisted analysis of PB smears, focusing on suspected VEXAS cases, can provide valuable insights for determining which patients should undergo molecular testing. The presented deep learning approach can help hematologists direct their suspicions before initiating further analyses.
引用
收藏
页码:120 / 129
页数:10
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