1.p40 in metastatic pulmonary trophoblastic tumour: potential diagnostic pitfall on histopathology
Archana George Vallonthaiel ; Ritika Walia ; Raja Pramanik ; MC Sharma ; Deepali Jain
The Malaysian Journal of Pathology 2017;39(2):175-179
p40, one of the two isomers of p63, is nowadays widely used for diagnosis of squamous cell
carcinoma, especially in subtyping non-small cell carcinoma on lung biopsies. We describe a case
in which lung tumour was misdiagnosed as squamous cell carcinoma due to p40 immunopositivity.
A 36-year-old lady presented with cough and left sided chest pain of 2 months duration. Chest
imaging revealed a lesion in left lower lobe of the lung and biopsy was suggestive of squamous
cell carcinoma. However, past history revealed amputation of great toe for non-healing discharging
ulcer which on histopathology was diagnosed as choriocarcinoma. She also had a history of
hysterectomy five years ago, details of which were not available. Post-amputation β-hCG levels
were high and she had been treated with multimodality chemotherapy for choriocarcinoma. She
had good response to chemotherapy initially, however became resistant later on. Review of the
lung biopsy in the light of the past history along with extensive literature review led to the final
diagnosis of metastatic trophoblastic tumour to lung. Hence, awareness that p40 immunopositivity
can be seen in trophoblastic tumours is essential to avoid misdiagnosis, especially in sites like the
lung where squamous cell carcinoma is common.
2.Quantitative histology-based classification system for assessment of the intestinal mucosal histological changes in patients with celiac disease
Prasenjit DAS ; Gaurav PS GAHLOT ; Alka SINGH ; Vandana BALODA ; Ramakant RAWAT ; Anil K VERMA ; Gaurav KHANNA ; Maitrayee ROY ; Archana GEORGE ; Ashok SINGH ; Aasma NALWA ; Prashant RAMTEKE ; Rajni YADAV ; Vineet AHUJA ; Vishnubhatla SREENIVAS ; Siddhartha Datta GUPTA ; Govind K MAKHARIA
Intestinal Research 2019;17(3):387-397
BACKGROUND/AIMS: The existing histological classifications for the interpretation of small intestinal biopsies are based on qualitative parameters with high intraobserver and interobserver variations. We have developed and propose a quantitative histological classification system for the assessment of intestinal mucosal biopsies. METHODS: We performed a computer-assisted quantitative histological assessment of digital images of duodenal biopsies from 137 controls and 124 patients with celiac disease (CeD) (derivation cohort). From the receiver-operating curve analysis, followed by multivariate and logistic regression analyses, we identified parameters for differentiating control biopsies from those of the patients with CeD. We repeated the quantitative histological analysis in a validation cohort (105 controls and 120 patients with CeD). On the basis of the results, we propose a quantitative histological classification system. The new classification was compared with the existing histological classifications for interobserver and intraobserver agreements by a group of qualified pathologists. RESULTS: Among the histological parameters, intraepithelial lymphocyte count of ≥25/100 epithelial cells, adjusted villous height fold change of ≤0.7, and crypt depth-to-villous height ratio of ≥0.5 showed good discriminative power between the mucosal biopsies from the patients with CeD and those from the controls, with 90.3% sensitivity, 93.5% specificity, and 96.2% area under the curve. Among the existing histological classifications, our quantitative histological classification showed the highest intraobserver (69.7%–85.03%) and interobserver (24.6%–71.5%) agreements. CONCLUSIONS: Quantitative assessment increases the reliability of the histological assessment of mucosal biopsies in patients with CeD. Such a classification system may be used for clinical trials in patients with CeD.
Biopsy
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Celiac Disease
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Classification
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Cohort Studies
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Epithelial Cells
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Humans
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Intestine, Small
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Logistic Models
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Lymphocyte Count
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Observer Variation
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Sensitivity and Specificity