Exome sequencing characterizes the somatic mutation spectrum of early serrated lesions in a patient with serrated polyposis syndrome (SPS)

Sukanya Horpaopan,Jutta Kirfel,Sophia Peters,Michael Kloth,Robert Hüneburg,Janine Altmüller,Dmitriy Drichel,Margarete Odenthal,Glen Kristiansen,Christian P. Strassburg,Jacob Nattermann,Per Hoffmann,Peter Nürnberg,Reinhard Büttner,Holger Thiele,Philip Kahl,Isabel Spier,Stefan Aretz

Exome sequencing characterizes the somatic mutation spectrum of early serrated lesions in a patient with serrated polyposis syndrome (SPS)

2017

Sukanya Horpaopan
Jutta Kirfel
Sophia Peters
Michael Kloth
Robert Hüneburg
Janine Altmüller
Dmitriy Drichel
Margarete Odenthal
Glen Kristiansen
Christian P. Strassburg
Jacob Nattermann
Per Hoffmann
Peter Nürnberg
Reinhard Büttner
Holger Thiele
Philip Kahl
Isabel Spier
Stefan Aretz

Background Serrated or Hyperplastic Polyposis Syndrome (SPS, HPS) is a yet poorly defined colorectal cancer (CRC) predisposition characterised by the occurrence of multiple and/or large serrated polyps throughout the colon. A serrated polyp-CRC sequence (serrated pathway) of CRC formation has been postulated, however, to date only few molecular signatures of serrated neoplasia (BRAF, KRAS, RNF43 mutations, CpG Island Methylation, MSI) have been described in a subset of SPS patients and neither the etiology of the syndrome nor the distinct genetic alterations during tumorigenesis have been identified.

Keywords:

Methylation
CpG site
Pathology
Genetics
Exome sequencing
Colorectal cancer
Human genetics
KRAS
Carcinogenesis
Germline mutation
Medicine
Mutation
Sanger sequencing
Missense mutation
Candidate gene

Correction
Source
Cite
Save

References

Citations