4.2 Article

Accuracy of Subclassification and Grading of Renal Tumors on Fine Needle Aspiration Cytology Alone

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ACTA CYTOLOGICA
卷 65, 期 2, 页码 140-149

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KARGER
DOI: 10.1159/000513065

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Fine needle aspiration; Renal cancer; Interpretation of cytological features according to clinical and molecular genetic data

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Fine needle aspiration of renal masses can distinguish between benign and malignant neoplasms. Cytology alone may not always accurately subclassify renal cell carcinomas due to increasing molecular classification. A study on FNA of renal tumors found a 35% correct diagnosis rate among cytopathologists, with chromophobe RCCs having the highest accuracy. Inter-rater variability was fair and core needle biopsy may be necessary for accurate classification.
Background: Fine needle aspiration (FNA) of renal masses can distinguish between benign and malignant neoplasms in 73-94% of cases. Previous studies suggested the correct subclassification of renal cell carcinomas (RCCs) by cytomorphology can be achieved in up to 80% of cases. However, as RCCs become increasingly subclassified by molecular signatures, correct subclassification based on cytology alone is increasingly difficult. Design: Two FNA passes (2 stained with Diff-Quik (R) and 2 with the Papanicolaou method) were performed on all fresh nephrectomy specimens for a 1-year period. There were 30 cases in this study, with 29 primary renal tumors and 1 case of metastatic lung adenocarcinoma. Each case was assigned a random number and came with 2 slides (1 from each staining method). Eight cytopathologists were asked to provide a diagnosis and the World Health Organization/International Society of Urological Pathology (WHO/ISUP) grading if applicable. Fleiss' Kappa and Cohen's Kappa equations were used to look at inter-rater variability. Results: When compared to the surgical pathology diagnosis, the average percent correct diagnosis for all cytopathologist was 35%. Chromophobe RCCs had the best average percent accuracy at 72% followed by clearcell RCC at 48%. Average accuracy for grading RCCs was 40%. Inter-rater variability among the cytopathologists for all RCC diagnoses was fair with a Fleiss' Kappa coefficient of 0.28. For the WHO/ISUP grade, the weighted coefficient for each pathologist ranged from 0.11 to 0.45, ranging from fair to moderate, respectively. Conclusions: Renal tumors are difficult to classify on cytopathology alone. Core needle biopsy and ancillary studies are necessary if diagnosis will change management.

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