Faculty Bibliography

Introduction: Our study aimed to assess the sensitivity (SN) and specificity (SP) of fluorescence-in-situ-hybridization (FISH) alone and as an adjunct to routine cytology for the detection of malignancy in biliary tract lesions.
Material(s) and Method(s): Bile duct brush specimens with FISH results from 1/2013-1/2020 were tabulated yielding 55 cases. Cases were classified as "Benign" where surgical resection showed benign findings or follow-up was uneventful >18 months and as "Malignant" where surgical pathology or clinical follow up identified malignancy in the pancreatobillary system (40 cases). Cases not falling under these categories were excluded. Cytologically suspicious and positive cases were designated as "positive." FISH positive and "equivocal" results were also designated as "positive." When examining the combined cytology-FISH results, cases were designated as "positive" if either cytology or FISH test was "positive." Atypical cytology cases were excluded.
Result(s): 21/40 cases fell under benign or malignant categories. 5/21 cases had malignant surgical follow-up: 4 pancreaticobiliary ductal adenocarcinoma and 1 Hodgkin lymphoma. FISH showed high SP (100%) and low SN (33.3%) in diagnosing malignancy in bile brush cytology. In cytology alone, FISH alone and the combined cytology-FISH testing, there was a statistically significant difference in risk-of-malignancy between Positive and Negative diagnostic categories, p<0.05(Table 1). Accuracy improved using combined cytology-FISH results over either test alone, area under the curve (AUC: Cytology=0.8; FISH=0.717; Combined test=0.85) (Figure1).
Conclusion(s): Cytology, FISH and combined cytology-FISH results all showed higher risk-of-malignancy values in positive compared to negative categories. The FISH-cytology combination may improve the SN of detecting malignancy in biliary tract lesions. Sample size may have been too small to detect a significant difference between combined cytology-FISH results versus either test alone. However, due to the potential clinical impact of improving bile duct brush cytology accuracy, our results should be evaluated further in larger samples. [Formula presented] [Formula presented]
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Introduction: Pancreatic neuroendocrine tumors (PNET) are relatively uncommon neoplasms. Endoscopic ultrasound-guided fine-needle aspiration (EUS-FNA) has been shown to be an efficient method for preoperative assessment of pancreatic tumors; however, the role of cytologic grading of PNETs is unclear. We aim to evaluate cytologic diagnosis and grading of PNETs by correlating with histopathology.
Material(s) and Method(s): Cytopathology cases with a diagnosis of PNET from 6/2011-6/2020 were tabulated and compared with their corresponding surgical pathology to evaluate the diagnostic accuracy of EUS-FNA. In addition, tumor grading based on Ki-67 immunohistochemistry was correlated between cytologic and histologic specimens (Cohen's kappa coefficient).
Result(s): Thirty-nine cases of EUS-FNAs with PNET diagnosis and concomitant histologic evaluation were included. EUS-FNA showed a positive predictive value of 85% for PNET diagnosis. There were 6 discrepant cases (15%), including: 1 mixed ductal-neuroendocrine carcinoma, 1 PNET with concomitant high-grade carcinoma, 1 metastatic renal cell carcinoma, 1 solid pseudopapillary neoplasm, and 2 cases of chronic pancreatitis, potentially explained by under-sampling, scant cellularity and/or absence of adequate cell block for immunostaining (Table 1).Nineteen cases had Ki-67 immunostaining on both cytologic and histologic specimens with a concordance of 58% (Table 2). All discrepancies in Ki-67 evaluation were due to underscoring in cytologic samples. Cyto-histologic grading correlation was fair (Cohen's Kappa coefficient=0.24).
Conclusion(s): EUS-FNA is a valuable minimally invasive diagnostic tool in the preoperative diagnosis of PNETs with a positive predictive value of 85% in this cohort. Cyto-histologic grading correlation was fair, which suggests that applying surgical pathology ki-67 grading cut-off points to cytology sample evaluations may not be appropriate. All cyto-histologic grading discrepancies in our study were due to underscoring in cytologic samples, which might be related to sampling issues or tumor heterogeneity.
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Introduction: The Paris System classifies polyoma virus cytopathic effect (P-CPE) as "negative for high grade urothelial carcinoma (HGUC)". However, P-CPE may raise false suspicion for HGUC. Conversely, HGUC cells may display considerable degenerative nuclear changes mimicking P-CPE. Thus, P-CPE remains a known source of "atypia" in urine cytology. The aim of our study was to determine the frequency of P-CPE cases reported as atypical urothelial cells (AUC) in our laboratory, and to assess the diagnostic utility of SV40 immunostaining (IHC) in this setting.
Material(s) and Method(s): Urine cytology cases, all processed as single Thin prep (TP) slides, were searched for P-CPE diagnosis from 2018 to 2020. An additional slide was prepared for a subset of 40 randomly selected cases (19 P-CPEs, 21 negative controls) for SV40 IHC validation on TP slides.
Result(s): There were 111 urines with P-CPE. 51% were included in this study (Figure 1). Of these, 25% were diagnosed as negative for HGUC, 72% as AUC, and 3% as suspicious for HGUC. Follow-up histology showed HGUC in 3 (5%) cases (2 with AUC and 1 with suspicious for HGUC presurgical cytology). SV40 IHC was positive in 61.5% of cases in the P-CPE group and negative in 38.5% including one with confirmed HGUC on biopsy (Figure 2). In the control group, SV40 IHC was negative in 88% and equivocal in 12% (Figure 3). The difference in SV40 IHC between the P-CPE and control group was statistically significant (p<0.001).
Conclusion(s): Majority of urine samples with P-CPE were reported as AUC with a very low incidence of confirmed HGUC. SV40 IHC aided in the confirmation of viral infection. Our study shows that once the source of atypia is confirmed as polyoma virus with SV40 IHC, downgrading atypia to negative can safely be accomplished without the concern for missing a high-grade lesion. [Formula presented] [Formula presented] [Formula presented]
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Introduction: TERT promoter mutations in thyroid carcinoma suggest worse prognosis based on findings of a small number of studies. Additionally, pathologic features and clinical behavior of indeterminate thyroid nodules (ITN) with TERT promoter mutations remain less studied. Our study aims to explore the clinicopathologic features of ITN with TERT promoter mutations.
Material(s) and Method(s): A search conducted in our electronic medical record between 2015-2018 identified 18 cases with indeterminate thyroid fine-needle aspiration (FNA) cytology (Bethesda Class III, IV, and V) and a TERT mutation on molecular testing. 17 patients underwent thyroidectomy and were the subjects of this study.
Result(s): The mean age was 65 (range 38-83) with a female to male ratio of 9:8. The FNA Bethesda diagnoses were Class III in 9, IV in 8, and V in 1. Majority of patients who underwent thyroidectomy had malignant nodules (14,78%). Thyroidectomy diagnoses included classic PTC (5,29%), FVPTC (5,29%), follicular variant of papillary carcinoma (3,17%), poorly differentiated thyroid carcinoma (1, 6%), follicular adenoma (2,11%) and NIFTP (1,6%). Additional alterations were present in 11 cases, including NRAS(6), KRAS(2), and BRAF V600E (3). Of three cases with concurrent BRAF V600E mutation, two were metastatic, and one had tall cell features. Of two follicular adenoma cases, one had a concomitant NRAS mutation, and the other displayed negative results on Afirma testing. Malignant cases tended to occur in older patients, the majority exhibited follicular architecture, frequent oncocytic morphology, and higher pathologic stage (pT3 in 92%, pT2 in 8%).
Conclusion(s): Most TERT promoter mutations in ITN cytology are associated with high risk of malignancy and these malignancies are associated with unfavorable features such as advanced stage, capsular/vascular invasion, and metastatic disease. Few TERT promoter mutations have a benign outcome. Further studies on ITNs with TERT mutations are needed to determine the optimal management of these nodules.
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Introduction: Preoperative diagnosis of pancreas ductal adenocarcinoma (PDAC) on endoscopic ultrasound guided fine needle aspiration (FNA) cytology is often required to determine proper therapy. Accurate cytopathology diagnosis on FNA may be challenging due to limited/suboptimal cellularity and gastrointestinal contamination with accurate diagnoses necessitating consideration of the full clinical and radiologic picture in evaluating the pancreatic lesions. In this study, we investigated predictive value of integrating cytology diagnosis, radiologic and clinical features in diagnosing pancreatic adenocarcinoma.
Material(s) and Method(s): Pancreatic FNA cases from 1/2016-12/2018 with >18 months of follow-up or histopathology diagnosis on surgical resection were retrieved (n=203). Cases were categorized as "Adenocarcinoma" or "Benign" according to the surgical resection pathology or clinical follow-up. Their documented serum CA19-9 level, and in-house radiologic reports were studied (n=177, Table 1). A multiplayer perceptron neural network (MNN) was trained and tested for the ability of using the integrated clinical and radiologic features and cytologic diagnosis to distinguish between benign and malignant cases.
Result(s): The sensitivity, specificity, and accuracy for pancreatic FNA cytology alone was 77.5%, 97.6%, and 88.4%, respectively. There were significant correlations between malignant outcome and cytology diagnosis, CA19-9 level and involvement of common bile duct (CBD), pancreatic duct (PD), superior mesenteric artery (SMA) or superior mesenteric vein (SMV) (Table 1, p<0.001). Integration of the cytology diagnosis and CA19-9 level showed 92% accuracy in predicting surgical outcome. The MNN highlighted cytopathology to be the most important factor in predicting pancreatic lesion outcomes, followed by the serum CA19-9 level and involvement of the SMA (Figure 1).
Conclusion(s): Integration of the clinical and radiologic information with cytology diagnosis can improve accuracy in evaluating pancreatic adenocarcinomas, especially in suboptimal FNA cytology specimens. [Formula presented] [Formula presented]
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Background: Thyroseq next-generation sequencing assay and Afirma gene expression classifier (GEC) are used to risk-stratify thyroid nodules with indeterminate cytology: Bethesda III (atypia of undetermined significance, AUS/FLUS) and IV (suspicious for follicular neoplasm, SFN). In this study, we performed a paired comparison of both tests on the same group of indeterminate thyroid nodules with surgical followup.
Design(s): Of 645 AUS/FLUS/SFN cases with both molecular testing and surgical resection in 2014-2017, 40 cases had both Thyroseq (v2) and Afirma GEC performed on the same specimen. Cross-tabulations and ROC curves were created. McNemar tests were done to compare the performance of Thyroseq versus Afirma. The diagnostic performance of combined results were also examined: the combined result was called positive only if both Thyroseq and Afirma were positive/suspicious. Non-invasive follicular thyroid with papillary like nuclear features (NIFTP) on surgical resections was defined as ?positive.? Results: 20/40 (50%) cases were ?positive? on surgical pathology: 8 papillary thyroid carcinoma (PTC), 11 NIFTP, and 1 follicular carcinoma. Thyroseq and Afirma both showed high sensitivity and low specificity in diagnosing malignancy in indeterminate thyroid nodules. Next, the results of both tests were combined. The overall accuracy of combined testing was higher than either test alone (Figure 1). Compared to Afirma alone, the combined test had significantly higher specificity (30% vs 70%, p<0.05, Table 1), while the sensitivity declined from 90% to 75% (p=0.25, Table 1). Compared to Thyroseq alone, there was no significant difference in specificity (45% vs 70% p=0.06) or sensitivity (80% vs 75%, p=1.00, Table 1). Positive predictive value (PPV) improved compared to either test alone. Negative predictive value (NPV) improved compared to Thyroseq alone, and declined only slightly compared to Afirma alone.
Conclusion(s): Molecular testing of cytologically indeterminate thyroid nodules helps determine the extent of surgery. Low diagnostic performance metrics may limit the utility of molecular studies in distinguishing benign from malignant thyroid lesions. Our results show that the combined results of Thyroseq and Afirma improved the specificity and overall accuracy of molecular testing, and provided additional value in the surgical management of patients with indeterminate thyroid nodules. To the best of our knowledge, this is the first study that compares the performance of these two molecular tests on the same thyroid nodules

Introduction: Due to the diagnostic dilemma with indeterminate thyroid Bethesda categories III and IV (atypia of undetermined significance, AUS and Suspicious for follicular neoplasm, SFN), many laboratories utilize molecular testing to aid in risk stratification of these nodules. In this study, we evaluated the risk of malignancy (ROM) in AUS and SFN thyroid nodules with subsequent negative molecular (ThyroSeq) test results.
Material(s) and Method(s): This study was designed to evaluate the negative molecular thyroid fine needle aspiration (FNA) cases at a tertiary medical center in the metropolitan area. 109 cases of AUS and SFN thyroid FNAs over 3 years with surgical pathology follow up were included in the study.
Result(s): Of 109 AUS and SFN cases, 4 cases showed insufficient material for ThyroSeq testing (3.7%), 76 cases showed a molecular alteration (69.7%), and 29 cases were negative for an alteration on ThyroSeq (26.6%). Among the cases with negative ThyroSeq results, 26 cases were benign on surgical pathology (89.7%) (7/26 were follicular adenomas), and 3/29 cases were malignant on histopathology (papillary thyroid carcinoma) (ROM=10.3%, Table 1). AUS and SFN cases with molecular alterations showed a significantly higher ROM (ROM= 60.5%) compared to cases testing negative for molecular alterations (p<0.01, z = -4.61).
Conclusion(s): Our study found that indeterminate thyroid nodules that tested negative for a molecular alteration displayed an ROM of 10.3%. This ROM is comparable to the lower limit of ROM of FNA alone (without additional molecular testing data) in the AUS and SFN categories (10-30%), but is significantly lower than the ROM of indeterminate thyroid cases with known molecular mutations. Therefore, clinical follow-up is recommended for thyroid FNA indeterminate nodules, even those testing negative for a molecular alteration, due to the maintained, albeit lower, ROM. [Formula presented]
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Introduction: Urothelial carcinomas (UC) of the upper urinary tract (UUT) are rare, and usually show higher grade and poorer prognosis than carcinomas of the bladder. The Paris System (TPS) has been integrated into our standard terminology for interpreting urine cytology. Here we compare TPS diagnoses to the traditional reporting system (TD) in interpreting UC of UUT and lower urinary tract (LUT) in correlation with surgical pathology diagnoses (SD).
Material(s) and Method(s): A search of the cytopathology database on urine specimens from 7/1/2014-6/30/2016 (TD) and 7/1/2017-6/30/2019 (TPS) with corresponding lesions in SD, yielded 14-TD cases and 19-TPS in UUT; and 178-TD and 243-TPS cases in LUT. The cytopathology diagnosis using TD and TPS were compared to their corresponding SD.
Result(s): In UUT, 51.5% (17/33) were UC on SD. High-grade UC (HGUC) was correctly identified in UUT in 100% (5/5) with TD, and 75%(3/4) with TPS. No low-grade (LG) diagnoses were rendered in TD or TPS though there were 8 low-grade urothelial neoplasms (LGUN). LGUN was classified as "atypical" (2/3-TD, 2/5-TPS) or "negative" (1/3-TD, 3/5-TPS). Rates of "atypical" diagnoses of UUT were 28.6% (TPS) and 26.3% (TD), with no HGUC on SD. The risk of LGUN with "atypical" diagnoses decreased using TPS from 75.0% (3/4) to 60.0% (3/5). In LUT, HGUC was correctly diagnosed in 55.0%(44/80) (TD) and 47.4%(46/97) (TPS). 4% of LGUNs were classified as LG (3/60-TPS, 1/40-TD). "Atypical" diagnoses for TD and TPS showed 29.5% (23/78) and 30.0% (27/90) risk of LGUN and 34.6%(27/78) and 37.8%(34/90) risk of HGUC respectively. (Table-1)
Conclusion(s): The TD and TPS systems showed high accuracy in reporting UUT-HGUC. However, urine cytology is not optimal to identify LGUN in both TD and TPS systems. Additionally, our results suggest that urine cytology may be more sensitive in detecting HGUC in UUT versus LUT samples.[Table presented]
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Introduction: In urine cytology, the atypical category suffers from interobserver variability and a wide range of risk of malignancy (ROM). This leads to confusion and inconsistent clinical management of patients with atypical urine diagnoses. Our study identified the rate of atypical diagnoses at our institution over a five-year period and examined the concurrent or follow-up surgical pathology diagnoses (SD) to understand the clinical significance of atypical urine specimens.
Material(s) and Method(s): A retrospective review of adult urine cytology specimens pre- 7/1/2014-6/30/2016 (TD) and post- 7/1/2017-6/30/2019 (TPS) implementation of the Paris System for Reporting Urinary Cytology was performed, which identified 10,132 total urine specimens. Of these, 2,457 specimens from 1,727 patients were categorized as "atypical." 177 cytology specimens were found to have corresponding urinary tract SD within 90 days. Pre- and post-Paris System (TD and TPS) urine cytology diagnoses were compared.
Result(s): The overall rate of "atypical" diagnoses was 2,457/10,132 (24.3%). 177 of 2,457 atypical specimens (7.2%) had corresponding urinary tract SD, of which the ROM was 37.9% (TD 37.8%, TPS 37.9%, p=0.992). 61 of 177 atypical urines (34.5%) were high grade (HGUC/CIS) on SD (TD 32.9%, TPS 35.8%). 66 of 177 atypical urines (37.3%) were low grade urothelial neoplasms (LGUNs), atypical, or dysplastic on SD (TD 39.0%, TPS 35.8%, p=0.660). 44 of 177 atypical urines (24.9%) were benign on SD (TD 23.2%, TPS 26.3%) (Table 1).
Conclusion(s): While the atypical diagnosis rate of nearly 1 in 4 urines is fairly high, over one-third of atypical results signified a high grade malignancy, and over an additional one-third of atypical urines represented LGUN, atypical, or dysplastic surgical pathology diagnoses. These findings emphasize the need for close follow-up in patients with atypical diagnoses on urine cytology. Our findings did not show a significant difference between pre and post TPS follow up data. [Formula presented]
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Neutropenic enterocolitis (NE) is a predominantly cecum-based disease with high mortality seen in patients post chemotherapy. The pathogenesis of NE is poorly understood and probably multifactorial involving mucosal injury, neutropenia, and impaired host defense to intestinal organisms. The clinical presentation is characterized as ileocolonic inflammation and bowel wall thickening in patients with neutropenia, fever, and abdominal pain. The pathological features of NE include patchy necrosis, hemorrhage, ulcer, edema, perforation, infiltrating organisms, and characteristically, depletion of inflammatory cells (neutrophils). NE should always be considered as a possible diagnosis in immunosuppressed patients, especially those receiving chemotherapy. High clinical and histological diagnostic discordance rate exists. High index of clinical suspicion and prompt appropriate personalized management are essential to achieve a lower mortality rate.