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Abstract
Mutation analysis of the KRAS oncogene is now established as a predictive biomarker
in colorectal cancer (CRC). Large prospective clinical trials have shown that only
CRCs with wild-type KRAS respond to anti-epidermal growth factor receptor (EGFR) treatment.
Therefore, mutation analysis is mandatory before treatment, and reliable benchmarks
for the frequency and types of KRAS mutations have to be established for routinely
testing large numbers of metastatic CRCs. A thousand and eighteen cases (879 primary
tumors and 139 metastases) of metastatic colorectal cancer were analyzed for the KRAS
mutational status of codons 12 and 13 of the KRAS gene by genomic sequencing in a
routine setting. Results were analyzed separately for specimens derived from primary
tumors and metastases. KRAS mutations in codons 12 and 13 were present in 39.3% of
all analyzed CRCs. The most frequent types of mutations were glycine to aspartate
on codon 12 (p.G12D, 36.0%), glycine to valine on codon 12 (pG12V, 21.8%), and glycine
to aspartate on codon 13 (p.G13D, 18.8%). They account for 76.6% of all mutations
and prevail in primary tumors and distant metastases, indicating a robustness of the
KRAS mutational status during neoplastic dissemination. The frequency of KRAS mutations
and the preponderance of three types of mutations in codons 12 and 13 in a large,
unselected cohort of metastatic CRC confirm the previous data of small and selected
CRC samples. Thus, a mutation frequency of 40% and a cluster of three mutation types
(p.G12D, pG12V, and p.G13D) in primaries and metastases can be defined as benchmarks
for routine KRAS analyses.