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Genomic profiling by DNA amplification of laser capture microdissected tissues and array CGH
Author(s) -
Joana Cardoso
Publication year - 2004
Publication title -
nucleic acids research
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 9.008
H-Index - 537
eISSN - 1362-4954
pISSN - 0305-1048
DOI - 10.1093/nar/gnh142
Subject(s) - biology , comparative genomic hybridization , copy number analysis , laser capture microdissection , dna microarray , genomic dna , microdissection , dna profiling , polymerase chain reaction , microbiology and biotechnology , multiple displacement amplification , gene duplication , molecular inversion probe , dna , genetics , copy number variation , computational biology , dna extraction , genome , gene , genotyping , gene expression , genotype
Comparative genomic hybridization by means of BAC microarrays (array CGH) allows high-resolution profiling of copy-number aberrations in tumor DNA. However, specific genetic lesions associated with small but clinically relevant tumor areas may pass undetected due to intra-tumor heterogeneity and/or the presence of contaminating normal cells. Here, we show that the combination of laser capture microdissection, φ29 DNA polymerase-mediated isothermal genomic DNA amplification, and array CGH allows genomic profiling of very limited numbers of cells. Moreover, by means of simple statistical models, we were able to bypass the exclusion of amplification distortions and variability prone areas, and to detect tumor-specific chromosomal gains and losses. We applied this new combined experimental and analytical approach to the genomic profiling of colorectal adenomatous polyps and demonstrated our ability to accurately detect single copy gains and losses affecting either whole chromosomes or small genomic regions from as little as 2 ng of DNA or 1000 microdissected cells

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