Synapse - Multiplex PCR/LDR for detection of K-ras mutations in primary colon tumors

Multiplex PCR/LDR for detection of K-ras mutations in primary colon tumors Journal Article

Authors:	Khanna, M.; Park, P.; Zirvi, M.; Cao, W.; Picon, A.; Day, J.; Paty, P.; Barany, F.
Article Title:	Multiplex PCR/LDR for detection of K-ras mutations in primary colon tumors
Abstract:	Point mutations in codons 12, 13, and 61 of the K-ras gene occur early in the development of colorectal cancer and are preserved throughout the course of tumor progression. These mutations can serve as biomarkers for shed or circulating tumor cells and may be useful for diagnosis of early, curable tumors and for staging of advanced cancers. We have developed a multiplex polymerase chain reaction/ligase detection reaction (PCR/LDR) method which identifies all 19 possible single-base mutations in K-ras codons 12, 13, and 61, with a sensitivity of 1 in 500 wild-type sequences. In a blinded study, 144 paraffin-embedded archival colon carcinomas were microdissected and K-ras mutations determined by both dideoxy-sequencing and multiplex PCR/LDR. Results were concordant for 134 samples. The ten discordant samples were re-evaluated using higher sensitivity uniplex PCR/LDR, and the original multiplex PCR/LDR result was confirmed in nine of these ten cases. Multiplex PCR/LDR was able to identify mutations in solid tumors or paraffin-embedded tissues containing a majority of wild-type stromal cells, with or without microdissection. The technique is well suited for large scale studies and for analysis of clinical samples containing a minority population of mutated cells.
Keywords:	human tissue; gene mutation; gene sequence; solid tumor; cancer staging; polymerase chain reaction; colorectal cancer; cancer screening; tumor marker; early diagnosis; mutation rate; oncogene k ras; tumor growth; codon; point mutation; stroma cell; microdissection; k-ras mutations; ligase chain reaction; ligase detection reaction; human; priority journal; article; thermostable ligase
Journal Title:	Oncogene
Volume:	18
Issue:	1
ISSN:	0950-9232
Publisher:	Nature Publishing Group
Date Published:	1999-01-07
Start Page:	27
End Page:	38
Language:	English
DOI:	10.1038/sj.onc.1202291
PUBMED:	9926917
PROVIDER:	scopus
DOI/URL:	https://www.scopus.com/inward/record.uri?eid=2-s2.0-0033531235&partnerID=40&md5=d2fe60b43157972e0481d308c6dfcd3c
Notes:	Article -- Export Date: 16 August 2016 -- Source: Scopus

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