Regulation of tissue transglutaminase gene expression as a molecular model for retinoid effects on proliferation and differentiation. Academic Article

abstract

• Retinoids (structural and functional analogs of vitamin A) are potent antiproliferative agents whose mode of action is poorly understood. It has been suggested that the molecular events that underscore their action involve alterations in gene expression, but no gene has yet been shown to be directly regulated by these molecules. Several years ago, we found that retinoic acid caused an accumulation of the enzyme tissue transglutaminase in murine peritoneal macrophages and in human promyelocytic leukemia (HL-60) cells. We now report that this induction is caused by an increase in the mRNA for this enzyme. Retinoic acid is the only mediator of this induction, since its effects do not depend on the presence of serum proteins. The induction of tissue transglutaminase mRNA is not due to an increase in its stability but to an increase in the relative transcription rate of its gene. We present a model to correlate the retinoid induction of tissue transglutaminase with retinoid effects on cellular growth and differentiation.

authors

• Davies, Peter

published proceedings

• J Cell Biochem

altmetric score

• 3

author list (cited authors)

• Chiocca, E. A., Davies, P. J., & Stein, J. P.

citation count

• 61

complete list of authors

• Chiocca, EA||Davies, PJ||Stein, JP

publication date

• March 1989

publisher

• Wiley  Publisher

published in

• Journal of Cellular Biochemistry  Journal

keywords

• Animals
• Blotting, Northern
• Cell Differentiation
• Cell Division
• Densitometry
• Enzyme Induction
• Gene Expression Regulation
• Mice
• Models, Genetic
• RNA, Messenger
• Retinoids
• Retinol-binding Proteins
• Transcription, Genetic
• Transglutaminases

PubMed Central ID

• 2565341

Digital Object Identifier (DOI)

• 10.1002/jcb.240390309

start page

• 293

end page

• 304

volume

• 39

issue

• 3

URL

• http://dx.doi.org/10.1002/jcb.240390309