TITLE
Modulation of steroid receptor-mediated gene expression by vitamin
B6. 70 REFS
AUTHOR
Tully DB; Allgood VE; Cidlowski JA
ORGANIZATION
Department of Physiology, University of North Carolina at Chapel Hill
27599-7545.
SOURCE
FASEB J 1994 Mar 1; 8 (3): 343-9
LANGUAGE OF ORIGIN
English
ABSTRACT
Gene transcription mediated by steroid hormones has become one of the
most extensively characterized model systems for studying the regulation
of gene expression in eukaryotic cells. However, specific details of gene
regulation by steroid hormones are often complex and may be unique in specific
cell types. Diverse regulatory mechanisms leading to either activation
or repression of particular genes frequently involve interactions between
steroid hormone receptors and other ubiquitous and/or cell-specific transcription
factors that act on the complex promoter of the regulated gene. Interplay
between steroid receptor-mediated and other signal transduction pathways
may also be involved. In addition, recent novel results indicate that moderate
variations in the intracellular concentration of pyridoxal 5'-phosphate
(PLP), the biologically active form of vitamin B6, can have pronounced
modulatory effects on steroid-induced gene expression. Specifically, elevation
of intracellular PLP levels leads to decreased transcriptional responses
to glucocorticoid, progesterone, androgen, or estrogen hormones. Conversely,
cells in a vitamin B6-deficient state exhibit enhanced responsiveness to
steroid hormones. One aspect of the mechanism by which these transcriptional
modulatory effects of PLP occur has recently been shown to involve interruption
of functional interactions between steroid hormone receptors and the nuclear
transcription factor NF1. These findings -- that the vitamin B6 nutritional
status of cells modulates their capacity to respond to steroid hormones
-- impose an additional level of cell-specific control over steroid hormone
regulation of gene expression and will serve as the focal point for this
review. (AUTHOR)
MJTR: Gene Expression DE. Pyridoxine PD. Receptors, Steroid PH.
MNTR: Animal. Human. In Vitro. Pyridoxal Phosphate PD. Receptors, Glucocorticoid
DE. Receptors, Glucocorticoid PH. Receptors, Steroid DE. Support, Non-U.S.
Gov't. Support, U.S. Gov't, P.H.S.. Transcription, Genetic DE. JOURNAL
ARTICLE. REVIEW. REVIEW, TUTORIAL
RNUM: 0 (Receptors, Glucocorticoid); 0 (Receptors, Steroid); 54-47-7
(Pyridoxal Phosphate); 65-23-6 (Pyridoxine)
GEOT: UNITED STATES
IDEN: ISSN: 0892-6638. JOURNAL-CODE: FAS. ENTRY-DATE: 940504. NIH-GRANT-NUMBER:
DK 32459DKNIDDK. JOURNAL-SUBSET: M X. IM-DATE: 9407.
ACCE: 94192903
