Author: Gunjan Akash Brown David T. van Holde K.E. Wolffe A.P. Luger K. Widom J. Adams C.C. Paranjape S.M. Kornberg R.D. Grunstein M. Widom J. Wolffe A.P. Zlatanova J. Croston G.E. Laybourn P.J. Kamakaka R.T. Wolffe A.P. Shimamura A. Thoma F. Zlatanova J. Weintraub H. Pennings W. Ura K. Juan L.-J. Polach K.L. Nacheva G.A. Kamakaka R.T. Hill D.A. Ding H.-F. Dimitrov S. Karetsou Z. Ramakrishnan V. Clark K.L. Cerf C. Cirillo L.A. Cairns B.R. Gregory P.D. Panetta G. Sera T. Bouvet P. Kandolf H. Steinbach O.C. Shen X. Brown D.T. Brown D.T. Brown D.T. Zaret K.S. Richard-Foy H. Fragoso G. Archer T.K. Li Q. Li Q. Cordingley M.G. Pina B. Archer T.K. Truss M.J. Bresnick W.H. Sambrook J. Gilman M. Lee H.-L. Felsenfeld G. Smith C.L. Bartsch J. Ura K. Nightingale K.P. Nan X. Lee K.M. Usachenko S.I. Yang Y.-S. Dong Y. Talasz H. Fryer C.J. Chavez S. Zweidler A.
Publisher: Oxford University Press
ISSN: 1362-4962
Source: Nucleic Acids Research, Vol.27, Iss.16, 1999-08, pp. : 3355-3363
Disclaimer: Any content in publications that violate the sovereignty, the constitution or regulations of the PRC is not accepted or approved by CNPIEC.
Abstract
BALB/c 3T3 cell lines containing integrated copies of the MMTV promoter driving a reporter gene were constructed. Expression vectors in which either of two H1 variants, H10 or H1c, were under control of an inducible promoter were introduced into these lines. Surprisingly, overproduction of either variant resulted in a dramatic increase in basal and hormone-induced expression from the MMTV promoter. H1 overproduction also slowed the loss of MMTV promoter activity associated with prolonged hormone treatment. Transiently transfected MMTV reporter genes, which do not adopt a phased nucleosomal arrangement, do not display increased activity upon H1 overproduction. Thus the effects observed for stable constructs most likely represents a direct effect of H1 on a chromatin-mediated process specific to the nucleosomal structure of the integrated constructs. Induction of increased levels of acetylated core histones by treatment with trichostatin A also potentiated MMTV activity and this effect was additive to that caused by H1 overproduction. However, the effects of TSA treatment, in control or H1-overproducing cells, were eliminated by inhibiting protein synthesis. TSA treatment does not necessarily potentiate MMTV promoter activity by increasing core histone acetylation within the MMTV promoter but perhaps by altering the synthesis of an unlinked transcriptional regulator.
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