Molecular Genetic Positioning of Small Intestine and Papilla of Vater Carcinomas Including Clinicopathological Classification

Overview

Journal Cancer Med

Specialty Oncology

Date 2023 Mar 31

PMID 36999887

Authors

Masanori Nakamura

Yukiyasu Okamura

Keiichi Ohshima

Teiichi Sugiura

Ryo Ashida

Katsuhisa Ohgi

Etsuro Bando

Keiichi Fujiya

Akio Shiomi

Hiroyasu Kagawa

Taisuke Imamura

Goro Nakayama

Yasuhiro Kodera

Katsuhiko Uesaka

Nobuyuki Ohike

Tomoko Norose

Keiko Sasaki

Takashi Sugino

Sumiko Ohnami

Takeshi Nagashima

Kenichi Urakami

Yasuto Akiyama

Ken Yamaguchi

Affiliations

Soon will be listed here.

Abstract

Background: Small intestine carcinoma (SIC) cases in Japan have recently been treated with chemotherapy according to colorectal carcinoma classification, while papilla of Vater carcinoma (PVC) cases according to cholangiocarcinoma (CHC) classification. However, few research reports support the molecular genetic validity of these therapeutic choices.

Patients And Methods: Here, we investigated the clinicopathological and molecular genetic factors of SIC and PVC. We used the data from the Japanese version of The Cancer Genome Atlas. Additionally, molecular genetic data on gastric adenocarcinoma (GAD), colorectal adenocarcinoma (CRAD), pancreatic ductal adenocarcinoma (PDAC), and CHC were also referred to.

Results: This study consisted of tumor samples from 12 patients of SIC and three patients of PVC treated from January 2014 to March 2019. Among them, six patients had pancreatic invasion. t-Distributed stochastic neighbor embedding analysis showed that the gene expression pattern of SIC was similar not only to those of GAD and CRAD, but also to that of PDAC in the pancreatic invasion patients. In addition, PVC resembled the GAD, CRAD, and PDAC, rather than the CHC. The molecular genetic characteristics of the six patients with pancreatic invasion were: one had high microsatellite instability, two had a TP53 driver mutation, and three had tumor mutation burden values <1 mutation/Mb with no driver mutation.

Conclusions: In this study, the extensive gene expression profiling of organ carcinomas newly suggests that SIC or PVC may resemble GAD, CRAD, and PDAC. In addition, the data demonstrate that pancreatic invasive patients may be classified into several subtypes using molecular genetic factors.

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Molecular genetic positioning of small intestine and papilla of Vater carcinomas including clinicopathological classification.

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