Clinicopathological characteristics and molecular analysis of lung cancer associated with ciliated muconodular papillary tumor/bronchiolar adenoma

Author:

Higashiyama Masahiro12,Motoi Noriko34ORCID,Yotsukura Masaya1,Yoshida Yukihiro1,Nakagawa Kazuo1,Yagishita Shigehiro5,Shirasawa Masayuki36,Yoshida Tatsuya6,Shiraishi Kouya3,Kohno Takashi3,Ohe Yuichiro26,Watanabe Shun‐ichi1

Affiliation:

1. Department of Thoracic Surgery National Cancer Center Hospital Tokyo Japan

2. Course of Advanced Clinical Research of Cancer Juntendo University Graduate School of Medicine Bunkyo‐ku Japan

3. Division of Genome Biology National Cancer Center Research Institute Chuo‐ku Tokyo Japan

4. Department of Diagnostic Pathology National Cancer Center Hospital Chuo‐ku Tokyo Japan

5. Division of Molecular Pharmacology National Cancer Center Research Institute Chuo‐ku Tokyo Japan

6. Department of Thoracic Oncology National Cancer Center Hospital Chuo‐ku Tokyo Japan

Abstract

AbstractCiliated muconodular papillary tumor/bronchiolar adenoma (CMPT/BA) is a recently introduced benign lung tumor. It remains unclear whether CMPT/BA is associated with a specific type of lung cancer (LC). We studied the clinicopathological characteristics and genetic profiles of the coexisting primary LC and CMPT/BA (LCCM) cases. We identified eight LCCM (0.4%) from the resected Stage 0–III primary LC (n = 1945). The LCCM cohort was male‐dominant (n = 8), elderly (median 72 years old), and most were smokers (n = 6). In addition to the adenocarcinoma (n = 8), we detected two squamous cell carcinomas and one small cell carcinoma—in some cases, multiple cancer. The target sequence/whole exome sequence (WES) revealed no shared mutations between CMPT/BA and LC. One exceptional case was invasive mucinous adenocarcinoma harboring an HRAS mutation (I46N, c.137T>A), but it was likely to be a single nucleotide polymorphism based on variant allele frequency (VAF). Other driver mutations in LC included EGFR (InDel, n = 2), BRAF(V600E) (n = 1), KRAS (n = 2), GNAS (n = 1), and TP53 (n = 2). BRAF(V600E) was the most frequent mutation in CMPT/BA (60%). In contrast, LC showed no specific trend in driver gene mutations. In conclusion, our study revealed differences in the gene mutation profiles of CMPT/BA and LC in coexisting cases, suggesting mostly independent clonal tumorigenesis of CMPT/BA from LC.

Publisher

Wiley

Subject

General Medicine,Pathology and Forensic Medicine

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