End-sequence profiling: Sequence-based analysis of aberrant genomes

S Volik, SY Zhao, K Chin, JH Brebner, DR Herndon, QZ Tao, D Kowbel, GQ Huang, A Lapuk, WL Kuo, G Magrane, P de Jong, JW Gray, C Collins*

*Corresponding author for this work

    Research output: Contribution to journalArticleAcademicpeer-review

    114 Citations (Scopus)

    Abstract

    Genome rearrangements are important in evolution, cancer, and other diseases. Precise mapping of the rearrangements is essential for identification of the involved genes, and many techniques have been developed for this purpose. We show here that end-sequence profiling (ESP) is particularly well suited to this purpose. ESP is accomplished by constructing a bacterial artificial chromosome (BAC) library from a test genome, measuring BAC end sequences, and mapping end-sequence pairs onto the normal genome sequence. Plots of BAC end-sequences density identify copy number abnormalities at high resolution. BACs spanning structural aberrations have end pairs that map abnormally far apart on the normal genome sequence. These pairs can then be sequenced to determine the involved genes and breakpoint sequences. ESP analysis of the breast cancer cell line MCF-7 demonstrated its utility for analysis of complex genomes. End sequencing of approximate to8,000 clones (0.37-fold haploid genome clonal coverage) produced a comprehensive genome copy number map of the MCF-7 genome at better than 300-kb resolution and identified 381 genome breakpoints, a subset of which was verified by fluorescence in situ hybridization mapping and sequencing.

    Original languageEnglish
    Pages (from-to)7696-7701
    Number of pages6
    JournalProceedings of the National Academy of Sciences of the United States of America
    Volume100
    Issue number13
    Publication statusPublished - 24-Jun-2003

    Keywords

    • BREAST-CANCER
    • HYBRIDIZATION
    • CONSTRUCTION
    • CHROMOSOME-4
    • CARCINOMA
    • LIBRARIES
    • ZNF217

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