1. Cancer of the ampulla of Vater: analysis of the whole genome sequence exposes a potential therapeutic vulnerability
- Author
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Michael J. Demeure, Tyler Izatt, Lawrence Koep, Jennifer Dinh, Shripad Sinari, Jessica Aldrich, Irene Cherni, Galen Hostetter, John D. Carpten, Jeffrey M. Trent, Daniel D. Von Hoff, Tracy M. Moses, Douglas F. Lake, Alexis Christoforides, Angela Baker, David Craig, Ardis Decker, and April Watanabe
- Subjects
medicine.medical_treatment ,Bioinformatics ,medicine.disease_cause ,Bile duct cancer ,03 medical and health sciences ,0302 clinical medicine ,medicine ,Genetics ,PTEN ,Genetics(clinical) ,Molecular Biology ,Genetics (clinical) ,030304 developmental biology ,0303 health sciences ,Common bile duct ,biology ,business.industry ,Research ,Ampulla of Vater ,Cancer ,medicine.disease ,Pancreaticoduodenectomy ,3. Good health ,medicine.anatomical_structure ,030220 oncology & carcinogenesis ,Cancer research ,biology.protein ,Molecular Medicine ,KRAS ,business ,Carcinogenesis - Abstract
Background Recent advances in the treatment of cancer have focused on targeting genomic aberrations with selective therapeutic agents. In rare tumors, where large-scale clinical trials are daunting, this targeted genomic approach offers a new perspective and hope for improved treatments. Cancers of the ampulla of Vater are rare tumors that comprise only about 0.2% of gastrointestinal cancers. Consequently, they are often treated as either distal common bile duct or pancreatic cancers. Methods We analyzed DNA from a resected cancer of the ampulla of Vater and whole blood DNA from a 63 year-old man who underwent a pancreaticoduodenectomy by whole genome sequencing, achieving 37× and 40× coverage, respectively. We determined somatic mutations and structural alterations. Results We identified relevant aberrations, including deleterious mutations of KRAS and SMAD4 as well as a homozygous focal deletion of the PTEN tumor suppressor gene. These findings suggest that these tumors have a distinct oncogenesis from either common bile duct cancer or pancreatic cancer. Furthermore, this combination of genomic aberrations suggests a therapeutic context for dual mTOR/PI3K inhibition. Conclusions Whole genome sequencing can elucidate an oncogenic context and expose potential therapeutic vulnerabilities in rare cancers.
- Published
- 2011