Background: The Banff Classification may not adequately address protocol transplant biopsies categorized as normal in patients experiencing unexplained graft function deterioration. This study seeks to employ convolutional neural networks to automate the segmentation of glomerular cells and capillaries and assess their correlation with transplant function.

Methods: A total of 215 patients were categorized into three groups. In the Training cohort, glomerular cells and capillaries from 37 patients were manually annotated to train the networks. The Test cohort (24 patients) compared manual annotations vs automated predictions, while the Application cohort (154 protocol transplant biopsies) examined predicted factors in relation to kidney function and prognosis.

Results: In the Test cohort, the networks recognized histological structures with Precision, Recall, F-score and Intersection Over Union exceeding 0.92, 0.85, 0.89 and 0.74, respectively. Univariate analysis revealed associations between the estimated glomerular filtration rate (eGFR) at biopsy and relative endothelial area (r = 0.19, = .027), endothelial cell density (r = 0.20, = .017), mean parietal epithelial cell area (r = -0.38, < .001), parietal epithelial cell density (r = 0.29, < .001) and mesangial cell density (r = 0.22, = .010). Multivariate analysis retained only endothelial cell density as associated with eGFR (Beta = 0.13, = .040). Endothelial cell density (r = -0.22, = .010) and mean podocyte area (r = 0.21, = .016) were linked to proteinuria at biopsy. Over 44 ± 29 months, 25 patients (16%) reached the primary composite endpoint (dialysis initiation, or 30% eGFR sustained decline), with relative endothelial area, mean endothelial cell area and parietal epithelial cell density below medians linked to this endpoint [hazard ratios, respectively, of 2.63 (= .048), 2.60 (= .039) and 3.23 (= .019)].

Conclusion: This study automated the measurement of intraglomerular cells and capillaries. Our results suggest that the precise segmentation of endothelial and epithelial cells may serve as a potential future marker for the risk of graft loss.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10873504PMC
http://dx.doi.org/10.1093/ckj/sfae019DOI Listing

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