Literature DB >> 8537408

Keratinocyte transglutaminase promoter analysis. Identification of a functional response element.

L Mariniello1, Q Qin, B A Jessen, R H Rice.   

Abstract

Keratinocyte transglutaminase catalyzes isopeptide bond formation to yield the highly insoluble cross-linked envelope during terminal differentiation of epidermal cells. Transcriptional response elements were identified in the 5'-flanking DNA of the gene for this enzyme by a combination of transient transfection and electrophoretic mobility shift analyses. Since human keratinocytes transcribed ineffectively transfected transglutaminase flanking DNA, a key feature of these experiments was the use of rat bladder epithelial cells as recipients. Serial deletion experiments identified by transient transfection an important response region containing three putative AP2-like response elements approximately 0.5 kilobases from the transcription initiation site. Oligonucleotides, each containing a single one of the elements, formed specific complexes with keratinocyte nuclear proteins. Two of the response elements were found to be functional by transfection in site-specific deletion experiments. Of these one formed specific DNA-protein complexes with nuclear proteins only from cells exhibiting keratinocyte differentiation. UV cross-linking experiments estimated the protein component of the complex to be approximately 85 kDa. This response element alone increased substantially the transcription of a minimal transglutaminase promoter in transient transfections. Further characterization of the putative transcription factor binding to this response element may provide insight into the regulation of keratinocyte transglutaminase.

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Year:  1995        PMID: 8537408     DOI: 10.1074/jbc.270.52.31358

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  2 in total

1.  Cardiac expression of the Drosophila Transglutaminase (CG7356) gene is directly controlled by myocyte enhancer factor-2.

Authors:  Jennifer Iklé; Jennifer A Elwell; Anton L Bryantsev; Richard M Cripps
Journal:  Dev Dyn       Date:  2008-08       Impact factor: 3.780

2.  A distal region of the human TGM1 promoter is required for expression in transgenic mice and cultured keratinocytes.

Authors:  Marjorie A Phillips; Bart A Jessen; Ying Lu; Qin Qin; Mary E Stevens; Robert H Rice
Journal:  BMC Dermatol       Date:  2004-04-05
  2 in total

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