signatures of selection in fusion transcripts resulting from chromosomal translocations in human cancer签名融合转录本的选择造成染色体易位在人类癌症.pdfVIP
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signatures of selection in fusion transcripts resulting from chromosomal translocations in human cancer签名融合转录本的选择造成染色体易位在人类癌症
Signatures of Selection in Fusion Transcripts Resulting
From Chromosomal Translocations in Human Cancer
˜ ´ ´
Inigo Ortiz de Mendıbil, Jose L. Vizmanos, Francisco J. Novo*
Department of Genetics, University of Navarra, Pamplona, Spain
Abstract
Background: The recurrence and non-random distribution of translocation breakpoints in human tumors are usually
attributed to local sequence features present in the vicinity of the breakpoints. However, it has also been suggested that
functional constraints might contribute to delimit the position of translocation breakpoints within the genes involved, but a
quantitative analysis of such contribution has been lacking.
Methodology: We have analyzed two well-known signatures of functional selection, such as reading-frame compatibility
and non-random combinations of protein domains, on an extensive dataset of fusion proteins resulting from chromosomal
translocations in cancer.
Conclusions: Our data provide strong experimental support for the concept that the position of translocation breakpoints
in the genome of cancer cells is determined, to a large extent, by the need to combine certain protein domains and to keep
an intact reading frame in fusion transcripts. Additionally, the information that we have assembled affords a global view of
the oncogenic mechanisms and domain architectures that are used by fusion proteins. This can be used to assess the
functional impact of novel chromosomal translocations and to predict the position of breakpoints in the genes involved.
´
Citation: Ortiz de Mendıbil I, Vizmanos JL, Novo FJ (2009) Signatures of Selection in Fusion Transcripts Resulting From Chromosomal Translocations in Human
Cancer. PLoS ONE 4(3): e4805. doi:10.1371/journal.pone.0004805
Editor: Michael J. Pazin, Nationa
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