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Raymond J. MacDonald

Researcher at University of Texas Southwestern Medical Center

Publications -  124
Citations -  31069

Raymond J. MacDonald is an academic researcher from University of Texas Southwestern Medical Center. The author has contributed to research in topics: Gene expression & Pancreas. The author has an hindex of 56, co-authored 121 publications receiving 30650 citations. Previous affiliations of Raymond J. MacDonald include University of Pennsylvania & Howard Hughes Medical Institute.

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The Parahox gene Pdx1 is required to maintain positional identity in the adult foregut

TL;DR: A model is proposed in which the posterior dominance of classical Hox genes is mirrored by the Parahox genes, providing further evidence of the functional conservation of the Parhox genes.
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A comprehensive survey of DNA-binding transcription factor gene expression in human fetal and adult organs.

TL;DR: A global survey of RNA from 14 fetal and 12 adult human organs by RT-PCR determined the expression patterns of 790 genes encoding DNA-binding transcription factors, a resource to help define the spectrum of transcription factor control.
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Integration of tetracycline regulation into a cell-specific transcriptional enhancer

TL;DR: Results show that a foreign and artificial transcriptional activator, tTA, can be incorporated into an enhancer to create a novel, efficient, and regulatable transcriptional control region whose cell specificity is retained.
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Synthesis of single-stranded hybridization probes from reusable DNA templates bound to solid support

TL;DR: A convenient and rapid technique for preparing radiolabeled single-stranded DNA hybridization probes has been developed that has a major advantage is that the restriction enzyme-cleaved, cellulose-bound template can be stored and reused repeatedly.
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Analysis of transcriptional regulatory regions in vivo.

TL;DR: A summary of the in vivo regulatory properties of the pancreas-specific transcriptional enhancer of the rat elastase 1 gene (ELA1) and the role individual elements in this enhancer play in directing high level, cell- specific transcription illustrates the nature, revelations and limitations of transgenic analysis.