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Real-world histopathological approach to malignancy of undefined primary origin (MUO) to diagnose cancers of unknown primary (CUPs)

Alberto Pisacane, Eliano Cascardi, Enrico Berrino, Alessio Polidori, Ivana Sarotto, Laura Casorzo, Mara Panero, Carla Boccaccio, Federica Verginelli, Silvia Benvenuti, Miriam Dellino, Paolo M. Comoglio, Filippo Montemurro, Elena Geuna, Caterina Marchiò, Anna Sapino

2022Archiv für Pathologische Anatomie und Physiologie und für Klinische Medicin19 citationsDOIOpen Access PDF

Abstract

The aim of this study is to envisage a streamlined pathological workup to rule out CUPs in patients presenting with MUOs. Sixty-four MUOs were classified using standard histopathology. Clinical data, immunocytochemical markers, and results of molecular analysis were recorded. MUOs were histologically subdivided in clear-cut carcinomas (40 adenocarcinomas, 11 squamous, and 3 neuroendocrine carcinomas) and unclear-carcinoma features (5 undifferentiated and 5 sarcomatoid tumors). Cytohistology of 7/40 adenocarcinomas suggested an early metastatic cancer per se. In 33/40 adenocarcinomas, CK7/CK20 expression pattern, gender, and metastasis sites influenced tissue-specific marker selection. In 23/40 adenocarcinomas, a "putative-immunophenotype" of tissue of origin addressed clinical-diagnostic examinations, identifying 9 early metastatic cancers. Cell lineage markers were used to confirm squamous and neuroendocrine differentiation. Pan-cytokeratins were used to confirm the epithelial nature of poorly differentiated tumors, followed by tissue and cell lineage markers, which identified one melanoma. In total, 47/64 MUOs (73.4%) were confirmed CUP. Molecular analysis, feasible in 37/47 CUPs (78.7%), had no diagnostic impact. Twenty CUP patients, mainly with squamous carcinomas and adenocarcinomas with putative-gynecologic-immunophenotypes, presented with only lymph node metastases and had longer median time to progression and overall survival (< 0.001), compared with patients with other metastatic patterns. We propose a simplified histology-driven workup which could efficiently rule out CUPs and identify early metastatic cancer.

Topics & Concepts

PathologyMalignancyImmunophenotypingHistopathologyMetastasisCancerBiologyLymph nodeCarcinomaHistologyImmunohistochemistryMedicineInternal medicineFlow cytometryGeneticsCancer Diagnosis and TreatmentTumors and Oncological CasesOral and Maxillofacial Pathology