Abstract

The long term objectives are to understand (i) fundamental aspects of transcription initiation, elongation, and termination mechanisms by DNA polymerases and """"""""common"""""""" accessory factors and (ii) the overall control of gene expression (transcription) during cell growth and proliferation, cell differentiation and infection or transformation by viruses; focusing on key target genes the general objective is to elucidate the structure, mechanism of action, and regulation of key effectors (regulatory factors) of these processes, thus leading to an understanding of important intracellular signals and control points. Taking advantage of the ability to reproduce natural transcription initiation and regulatory events in reconstituted cell free systems, and the recent identification, purification and cloning of common initiation factors, regulatory factors, and a new class of cofactors, the specific aims are as follows. Relative to the first general objective, (1) to complete the cloning and expression and to provide detailed information on the structure and mechanisms of action of the numerous """"""""common"""""""" transcription factors, (2) to determine the mechanism(s) of action of distinct classes of gene specific activators and repressors, including identification of targets in the basic transcriptional machinery and the structure and function of common or activator-specific cofactors required for these functions, (3) to investigate the role of higher order template organization, including chromatin assembly and nuclear matrix delocalization, in regulatory factor functions (induction or repression), and, ultimately, to use artificial nuclei to reconstitute a natural nuclear environment with purified genes and factors. Relative to these aims and to the second general objective, (4) to determine the mechanisms of activation of viral (adenovirus, herpesvirus, HIV, lymphotropic papovavirus) genes by both cellular factors (USF, Rel and PU.1 oncoproteins) and virus-coded factors (EIA, IE/ICP4, VP16/OTF1), (5) to investigate the regulation of cellular genes in relation to cell growth and proliferation; including elucidation of mechanisms involved in activation/repression of small structural RNA genes (5S, tRNA, snRNA), histone genes (H2B), and cellular protooncogenes (c-fos, c-myc) and determination of the functions of the products of protooncogenes (Myc) and tumor suppressor genes (Rb, P53), (6) to investigate gene regulation during B cell differentiation; including elaboration of the nature and mechanism of action of lymphoid specific factors implicated in activation of immunoglobulin genes (e.g. OCT2, BAF, NPkB, PU.1) and other stage- specific (e.g. pre B-specific) marker genes, as well as studies of the regulation of genes encoding these factors, and (7) to investigate the role of transcription (including specific factors) in DNA replication and in recombination (immunoglobulin gene rearrangements).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Unknown (R35)
Project #
2R35CA042567-08
Application #
3479433
Study Section
Special Emphasis Panel (SRC (88))
Project Start
1986-07-01
Project End
2000-04-30
Budget Start
1993-08-15
Budget End
1994-04-30
Support Year
8
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Rockefeller University
Department
Type
Other Domestic Higher Education
DUNS #
071037113
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Chong, Jayhong A; Moran, Magdalene M; Teichmann, Martin et al. (2005) TATA-binding protein (TBP)-like factor (TLF) is a functional regulator of transcription: reciprocal regulation of the neurofibromatosis type 1 and c-fos genes by TLF/TRF2 and TBP. Mol Cell Biol 25:2632-43
Zakharova, Natalia; Lymar, Elena S; Yang, Edward et al. (2003) Distinct transcriptional activation functions of STAT1alpha and STAT1beta on DNA and chromatin templates. J Biol Chem 278:43067-73
An, Woojin; Roeder, Robert G (2003) Direct association of p300 with unmodified H3 and H4 N termini modulates p300-dependent acetylation and transcription of nucleosomal templates. J Biol Chem 278:1504-10
Wallberg, Annika E; Yamamura, Soichiro; Malik, Sohail et al. (2003) Coordination of p300-mediated chromatin remodeling and TRAP/mediator function through coactivator PGC-1alpha. Mol Cell 12:1137-49
Wang, Hengbin; An, Woojin; Cao, Ru et al. (2003) mAM facilitates conversion by ESET of dimethyl to trimethyl lysine 9 of histone H3 to cause transcriptional repression. Mol Cell 12:475-87
Wallberg, Annika E; Pedersen, Kia; Lendahl, Urban et al. (2002) p300 and PCAF act cooperatively to mediate transcriptional activation from chromatin templates by notch intracellular domains in vitro. Mol Cell Biol 22:7812-9
Kato, Hiroyuki; Tjernberg, Agneta; Zhang, Wenzhu et al. (2002) SYT associates with human SNF/SWI complexes and the C-terminal region of its fusion partner SSX1 targets histones. J Biol Chem 277:5498-505
Murphy, Christine; Wang, Zhengxin; Roeder, Robert G et al. (2002) RNA polymerase III in Cajal bodies and lampbrush chromosomes of the Xenopus oocyte nucleus. Mol Biol Cell 13:3466-76
Baek, Hwa Jin; Malik, Sohail; Qin, Jun et al. (2002) Requirement of TRAP/mediator for both activator-independent and activator-dependent transcription in conjunction with TFIID-associated TAF(II)s. Mol Cell Biol 22:2842-52
Zhang, D; Penttila, T L; Morris, P L et al. (2001) Cell- and stage-specific high-level expression of TBP-related factor 2 (TRF2) during mouse spermatogenesis. Mech Dev 106:203-5

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