Project description:We report genome wide mapping of the histone variant H2A.Z during G0/G1 and mitosis in T24 bladder cancer cells. The results show that the broad enrichment pattern of H2A.Z near transcription start sites of active genes is maintained during mitosis. Furthermore, using H2A.Z localization to visualize nucleosome positioning near the start site, we see that the +1 nucleosome of active genes shifts upstream to occupy the transcription start sites during mitosis and the nucleosome depleted region is shortened. H2A.Z is also maintained on the -2 nucleosome which also shifts towrds the transcription start site during mitosis, further contributing to the shorteneing of the nucleosome depleted region. Examination of H2A.Z duing G0/G1 and mitosis in bladder cancer cells

Project description:Genome wide mapping of PSF binding sites in prostate cancer cells

Project description:Transcriptomes of human bladder cells and cells in bladder cancer

Project description:Transcriptome-wide mapping of human Staufen1 binding sites

Project description:Genome-wide expression profiling in bladder cancer cells

Project description:Genome-wide mapping of PRDM14 binding sites in human embryonic stem cells

Project description:Genome-wide mapping of REST-bound sites in human CD4+ T cells

Project description:FoxA transcription factors are involved in development and tumorigenesis of the gastrointestinal tract. However, the downstream programs controlled by FoxA factors remain poorly understood. The goal of this study is to understand the transcriptional responses regulated by FoxA proteins in liver and colon cancer cells. Human liver cancer cell line HepG2 and colon cancer cell line LS174T infected with lentivirus expressing shRNAs targeting human FoxA1 and FoxA2.

Project description:Genome-Wide Mapping of Hypomethylated Sites in Human Genomes

Project description:Bladder cancer cells