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Dive into the research topics where Kenneth Lynn Wright is active.

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Featured researches published by Kenneth Lynn Wright.


Cell Biochemistry and Biophysics | 1989

Modifications in molecular mechanisms associated with control of cell cycle regulated human histone gene expression during differentiation

Gary S. Stein; Janet L. Stein; Jane B. Lian; Andre J. van Wijnen; Kenneth Lynn Wright; Urs Pauli

Histone proteins are preferentially synthesized during the S-phase of the cell cycle, and the temporal and functional coupling of histone gene expression with DNA replication is mediated at both the transcriptional and posttranscriptional levels. The genes are transcribed throughout the cell cycle, and a 3–5-fold enhancement in the rate of transcription occurs during the first 2 h following initiation of DNA synthesis. Control of histone mRNA stability also accounts for some of the 20–100fold increase in cellular histone mRNA levels during S-phase and for the rapid and selective degradation of the mRNAs at the natural completion of DNA replication or when DNA synthesis is inhibited.Two segments of the proximal promoter, designated Sites I and II, influence the specificity and rate of histone gene transcription. Occupancy of Sites I and II during all periods of the cell cycle by three transacting factors (HiNF-A, HiNF-C., and HiNF-D) suggests that these protein-DNA interactions are responsible for the constitutive transcription of histone genes. Binding of HiNF-D in Site II is selectively lost, whereas occupancy of Site I by HiNF-A and -C persists when histone gene transcription is down regulated when cells terminally differentiate. These results are consistent with a primary role for interactions of HiNF-D with a proximal promoter element in rendering cell growth regulated human histone genes transcribable in proliferating cells.


Proceedings of the National Academy of Sciences of the United States of America | 1990

Coordinate occupancy of AP-1 sites in the vitamin D-responsive and CCAAT box elements by Fos-Jun in the osteocalcin gene: model for phenotype suppression of transcription.

Thomas A. Owen; Rita Bortell; S A Yocum; S L Smock; M Zhang; C Abate; Victoria Shalhoub; Neil Aronin; Kenneth Lynn Wright; A. J. Van Wijnen


Proceedings of the National Academy of Sciences of the United States of America | 1992

Sequence-specific DNA-binding proteins are components of a nuclear matrix-attachment site.

Steven I. Dworetzky; Kenneth Lynn Wright; Edward G. Fey; Sheldon Penman; Jane B. Lian; Janet L. Stein; Gary S. Stein


Science | 1990

Tumor cells exhibit deregulation of the cell cycle histone gene promoter factor HiNF-D

J Holthuis; Thomas A. Owen; A. J. Van Wijnen; Kenneth Lynn Wright; Anna L. Ramsey-Ewing; Mb Kennedy; Ruth Carter; Sc Cosenza; Kenneth J. Soprano; Jane B. Lian


Journal of Biological Chemistry | 1989

Human H4 histone gene transcription requires the proliferation-specific nuclear factor HiNF-D. Auxiliary roles for HiNF-C (Sp1-like) and HiNF-A (high mobility group-like).

A. J. Van Wijnen; Kenneth Lynn Wright; Jane B. Lian; Janet L. Stein; Gary S. Stein


Nucleic Acids Research | 1988

Two target sites for protein binding in the promoter region of a cell cycle regulated human H1 histone gene

Andre J. Van Wijnen; Kenneth Lynn Wright; Robert F. Massung; Martijn Gerretsen; Janet L. Stein; Gary S. Stein


Proceedings of the National Academy of Sciences of the United States of America | 1989

Altered binding of human histone gene transcription factors during the shutdown of proliferation and onset of differentiation in HL-60 cells

Gary S. Stein; Jane B. Lian; Janet L. Stein; R Briggs; Victoria Shalhoub; Kenneth Lynn Wright; U Pauli; A. J. Van Wijnen


Biochemistry | 1992

Multiple mechanisms regulate the proliferation-specific histone gene transcription factor HiNF-D in normal human diploid fibroblasts

Kenneth Lynn Wright; Robert Dell'Orco; Andre J. Van Wijnen; Janet L. Stein; Gary S. Stein


Proceedings of the National Academy of Sciences of the United States of America | 1991

Involvement of the cell cycle-regulated nuclear factor HiNF-D in cell growth control of a human H4 histone gene during hepatic development in transgenic mice

A. J. Van Wijnen; T K Choi; Thomas A. Owen; Kenneth Lynn Wright; Jane B. Lian; R Jaenisch; Janet L. Stein; Gary S. Stein


Journal of Biological Chemistry | 1988

The human H1 histone gene FNC16 is functionally expressed in proliferating HeLa S3 cells and is down-regulated during terminal differentiation in HL60 cells.

D. G. Collart; Kenneth Lynn Wright; A. J. Van Wijnen; A. L. Ramsey; Jane B. Lian; Janet L. Stein; Gary S. Stein

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A. J. Van Wijnen

University of Massachusetts Medical School

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Andre J. Van Wijnen

University of Massachusetts Medical School

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Thomas A. Owen

University of Massachusetts Amherst

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Victoria Shalhoub

University of Massachusetts Amherst

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A. L. Ramsey

University of Massachusetts Medical School

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