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1.
J Imaging ; 10(2)2024 Jan 25.
Article En | MEDLINE | ID: mdl-38392081

Histological staining is the primary method for confirming cancer diagnoses, but certain types, such as p63 staining, can be expensive and potentially damaging to tissues. In our research, we innovate by generating p63-stained images from H&E-stained slides for metaplastic breast cancer. This is a crucial development, considering the high costs and tissue risks associated with direct p63 staining. Our approach employs an advanced CycleGAN architecture, xAI-CycleGAN, enhanced with context-based loss to maintain structural integrity. The inclusion of convolutional attention in our model distinguishes between structural and color details more effectively, thus significantly enhancing the visual quality of the results. This approach shows a marked improvement over the base xAI-CycleGAN and standard CycleGAN models, offering the benefits of a more compact network and faster training even with the inclusion of attention.

2.
Diagnostics (Basel) ; 11(8)2021 Jul 29.
Article En | MEDLINE | ID: mdl-34441298

The ciliary ultrastructure can be damaged in various situations. Such changes include primary defects found in primary ciliary dyskinesia (PCD) and secondary defects developing in secondary ciliary dyskinesia (SCD). PCD is a genetic disease resulting from impaired ciliary motility causing chronic disease of the respiratory tract. SCD is an acquired condition that can be caused, for example, by respiratory infection or exposure to tobacco smoke. The diagnosis of these diseases is a complex process with many diagnostic methods, including the evaluation of ciliary ultrastructure using transmission electron microscopy (the golden standard of examination). Our goal was to create a program capable of automatic quantitative analysis of the ciliary ultrastructure, determining the ratio of primary and secondary defects, as well as analysis of the mutual orientation of cilia in the ciliary border. PCD Quant, a program developed for the automatic quantitative analysis of cilia, cannot yet be used as a stand-alone method for evaluation and provides limited assistance in classifying primary and secondary defect classes and evaluating central pair angle deviations. Nevertheless, we see great potential for the future in automatic analysis of the ciliary ultrastructure.

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