AUTHOR=Tachibana Shion , Mizukami Yusuke , Ono Yusuke , Sugiyama Yuya , Okada Tetsuhiro , Kitazaki Arisa , Sasajima Junpei , Tominaga Motoya , Sakamoto Jun , Kimura Keisuke , Omori Yuko , Furukawa Toru , Kimura Taichi , Tanaka Shinya , Nagashima Kazuo , Karasaki Hidenori , Ohta Tomoyuki , Okumura Toshikatsu 

TITLE=Genetic Tracing of Clonal Expansion and Progression of Pancreatic Ductal Adenocarcinoma: A Case Report and Multi-Region Sequencing Analysis

JOURNAL=Frontiers in Oncology

VOLUME=10

YEAR=2020

URL=https://www.frontiersin.org/journals/oncology/articles/10.3389/fonc.2020.00728

DOI=10.3389/fonc.2020.00728

ISSN=2234-943X

ABSTRACT=<p>Pancreatobiliary tumors frequently contain multiple malignant and precancerous lesions; however, the origin of the driver mutations and the mechanisms that underlie the generation of distinct clones within an organ field remain unclear. Herein, we describe a 76-year-old male suffering from moderately differentiated adenocarcinomas of the pancreas that primarily involved the distal bile duct and multiple “dispersing” invasive lesions in the pancreatic head. The patient underwent pylorus-preserving pancreaticoduodenectomy with superior mesenteric vein resection, and targeted sequencing of 18 genes associated with pancreatic tumorigenesis and immunohistochemical analysis of RNF43 and ARID1A were performed on each tumor compartment, including the invasive and non-invasive areas. Multi-region sequencing revealed shared <italic>KRAS</italic> and <italic>TGFBR1</italic> mutations in all invasive foci, including those involving the distal bile duct. Distinct <italic>KRAS</italic> variants were found to be present in other non-continuous and non-invasive lesions in the pancreas. Intraductal lesions with <italic>KRAS</italic> G12D and <italic>RNF43</italic> V50R mutations were evident in the main pancreatic duct. This appeared to be a founder clone, given that the mutation profile was common to the invasive foci as well as the additional high-grade dysplasia harboring <italic>ARID1A</italic> mutations, thereby suggesting a clonal branch-off during tumor evolution. In addition, we also observed independent intraductal papillary mucinous neoplasms with <italic>KRAS</italic> G12V and <italic>GNAS</italic> R201H mutations. Our theory, learned from this patient, was that lesions skipped dissemination and wide-spread movement potentially through the pancreatic ductal system as a process of pancreatic cancer development.</p>