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Mucinous Adenocarcinoma With Intrapulmonary Metastasis Harboring<i>KRAS</i>and<i>GNAS</i>Mutations Arising in Congenital Pulmonary Airway Malformation

Ximena Fernandez de Cordova, Huiying Wang, Mitra Mehrad, Rosana Eisenberg, Joyce Johnson, Qiang Wei, Scott C. Borinstein, Melissa E. Danko, Jiancong Liang

2020American Journal of Clinical Pathology16 citationsDOI

Abstract

OBJECTIVES: Mucinous adenocarcinoma arising in unresected congenital pulmonary airway malformation (CPAM) is rare. Underlying driver mutations in addition to KRAS gain-of-function mutations in this setting and the long-term outcomes of these patients are unknown. METHODS: We report a case of metastatic mucinous adenocarcinoma harboring both KRAS and GNAS mutations arising in a type 1 CPAM of a 14-year-old male. A literature review was performed. RESULTS: Next-generation sequencing revealed identical KRAS (G12V) mutations in both the CPAM and metastatic adenocarcinoma and a missense mutation in the GNAS (R201C) gene in the metastatic adenocarcinoma only. Median survival was 23 and 4 years for patients with localized (no or limited spread within the same lobe of CPAM) and distant involvement (spread to any different lobe of CPAM) of mucinous cells, respectively (95% confidence interval, 23-23 and 1.5-22 years, respectively; P = .017). CONCLUSIONS: Mucinous cell proliferation associated with type 1 CPAM has exceptionally good long-term outcomes if confined within the same lobe of CPAM. A second oncogenic mutation in the GNAS gene may be necessary for progression to malignancy and distant spread.

Topics & Concepts

GNAS complex locusKRASAdenocarcinomaMedicineMissense mutationMalignancyOncologyPathologyInternal medicineMutationCancer researchCancerColorectal cancerBiologyGeneGeneticsCongenital Diaphragmatic Hernia StudiesTracheal and airway disordersNeonatal Respiratory Health Research