| Literature DB >> 26826416 |
Fabien Forest1, Violaine Yvorel2, Georgia Karpathiou2, Marie-Laure Stachowicz2, Jean-Michel Vergnon3, Pierre Fournel4, Olivier Tiffet5, Béatrice Trombert6, Michel Péoc'h2.
Abstract
In pleomorphic, spindle cell, and giant cell carcinoma (PSCGC) of the lung, we wondered if an integrated diagnosis including morphological and immunohistochemical features could be related to molecular status. We performed immunohistochemistry on 35 PSCGCs against TTF1, napsin A, p40, ALK, ROS1, and c-MET. Mutational status regarding EGFR, KRAS, BRAF, HER2, and PIK3CA genes was established. Of 18 PSCGCs with adenocarcinomatous or "undifferentiated" carcinoma differentiation, 8 were mutated for EGFR (n = 1), KRAS (n = 2), BRAF (n = 1), HER2 (n = 3), and PIK3CA (n = 1). No PSCGC (0/4) with only squamous cell or adenosquamous (0/2) differentiation was mutated. c-MET overexpression was only seen in PSCGC with adenocarcinomatous or undifferentiated component (n = 5) without squamous cell component. ROS1 and ALK were negative. The presence of a "targetable mutation" was correlated to the presence of morphological or immunohistochemical adenocarcinomatous differentiation (P = .0137). Integrated diagnosis of an adenocarcinomatous component in PSCGC could be associated with the presence of targetable gene mutation. Because only PSCGC with adenocarcinomatous or undifferentiated carcinoma harbors mutations, whereas PSCGC with only squamous or adenosquamous differentiation does not in our study, this might represent a prescreening for patients with PSCGC to be tested for molecular targets. Our results emphasize that careful morphological examination and the use of immunohistochemistry might be useful for the selection of PSCGC tested for a mutational target.Entities:
Keywords: Lung neoplasms; Molecular targeted therapy; Sarcomatoid carcinoma; TTF1 protein; p40 protein
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Year: 2015 PMID: 26826416 DOI: 10.1016/j.humpath.2015.10.006
Source DB: PubMed Journal: Hum Pathol ISSN: 0046-8177 Impact factor: 3.466