a novel approach for determining cancer genomic breakpoints in the presence of normal dna一个新颖的方法来确定癌症基因组dna断点的正常.pdfVIP
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a novel approach for determining cancer genomic breakpoints in the presence of normal dna一个新颖的方法来确定癌症基因组dna断点的正常
A Novel Approach for Determining Cancer Genomic
Breakpoints in the Presence of Normal DNA
Yu-Tsueng Liu*, Dennis A. Carson
Moores UCSD Cancer Center, University of California San Diego, La Jolla, California, United States of America
CDKN2A (encodes p16INK4A and p14ARF) deletion, which results in both Rb and p53 inactivation, is the most common
chromosomal anomaly in human cancers. To precisely map the deletion breakpoints is important to understanding the
molecular mechanism of genomic rearrangement and may also be useful for clinical applications. However, current methods
for determining the breakpoint are either of low resolution or require the isolation of relatively pure cancer cells, which can be
difficult for clinical samples that are typically contaminated with various amounts of normal host cells. To overcome this
hurdle, we have developed a novel approach, designated Primer Approximation Multiplex PCR (PAMP), for enriching
breakpoint sequences followed by genomic tiling array hybridization to locate the breakpoints. In a series of proof-of-concept
experiments, we were able to identify cancer-derived CDKN2A genomic breakpoints when more than 99.9% of wild type
genome was present in a model system. This design can be scaled up with bioinformatics support and can be applied to
validate other candidate cancer-associated loci that are revealed by other more systemic but lower throughput assays.
Citation: Liu Y-T, Carson DA (2007) A Novel Approach for Determining Cancer Genomic Breakpoints in the Presence of Normal DNA. PLoS ONE 2(4):
e380. doi:10.1371/journal.pone.0000380
INTRODUCTION for deletion mapping, including Southern blotting [25], fluorescent
Tumors evolve through the continuous accumulati
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