Distinct p53 genomic binding patterns in normal and cancer-derived human cells

Botcheva, K; R, McCorkle S; R, McCombie W; J, Dunn J; W, Anderson C

doi:10.4161/cc.10.24.18383

Title: Distinct p53 genomic binding patterns in normal and cancer-derived human cells

Journal Article · Thu Dec 15 00:00:00 EST 2011 · Cell Cycle

DOI:https://doi.org/10.4161/cc.10.24.18383· OSTI ID:1041595

Botcheva, K; R, McCorkle S; R, McCombie W; J, Dunn J; W, Anderson C

We report here genome-wide analysis of the tumor suppressor p53 binding sites in normal human cells. 743 high-confidence ChIP-seq peaks representing putative genomic binding sites were identified in normal IMR90 fibroblasts using a reference chromatin sample. More than 40% were located within 2 kb of a transcription start site (TSS), a distribution similar to that documented for individually studied, functional p53 binding sites and, to date, not observed by previous p53 genome-wide studies. Nearly half of the high-confidence binding sites in the IMR90 cells reside in CpG islands, in marked contrast to sites reported in cancer-derived cells. The distinct genomic features of the IMR90 binding sites do not reflect a distinct preference for specific sequences, since the de novo developed p53 motif based on our study is similar to those reported by genome-wide studies of cancer cells. More likely, the different chromatin landscape in normal, compared with cancer-derived cells, influences p53 binding via modulating availability of the sites. We compared the IMR90 ChIPseq peaks to the recently published IMR90 methylome1 and demonstrated that they are enriched at hypomethylated DNA. Our study represents the first genome-wide, de novo mapping of p53 binding sites in normal human cells and reveals that p53 binding sites reside in distinct genomic landscapes in normal and cancer-derived human cells.

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Research Organization:: Brookhaven National Lab. (BNL), Upton, NY (United States)

Sponsoring Organization:: USDOE SC OFFICE OF SCIENCE (SC)

DOE Contract Number:: DE-AC02-98CH10886

OSTI ID:: 1041595

Report Number(s):: BNL-96203-2011-JA; R&D Project: BO-129; KP1602020; TRN: US201212%%13

Journal Information:: Cell Cycle, Vol. 10, Issue 24; ISSN 1538-4101

Country of Publication:: United States

Language:: English

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Related Subjects

59 BASIC BIOLOGICAL SCIENCES
60 APPLIED LIFE SCIENCES
ANIMAL CELLS
AVAILABILITY
CHROMATIN
DISTRIBUTION
DNA
FIBROBLASTS
NEOPLASMS
TRANSCRIPTION
p53
whole genome binding
tumor suppressor
transcription factor
CpG island
ChIP-seq

Title: Distinct p53 genomic binding patterns in normal and cancer-derived human cells

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