Glucocorticoid Receptors and the Cell Cycle: Evidence that the Accumulation of Glucocorticoid Receptors during the S Phase of the Cell Cycle is Dependent on Ribonucleic Acid and Protein Synthesis*
- 1 May 1982
- journal article
- research article
- Published by The Endocrine Society in Endocrinology
- Vol. 110 (5) , 1653-1662
- https://doi.org/10.1210/endo-110-5-1653
Abstract
HeLa S3 cells contain high affinity, saturable protein receptor molecules which steriospecifically bind active glucocorticoids. The number of glucocorticoid receptors per cell changes as cells in culture proceed through the cell cycle (1). HeLa S3 cells brought to the GI/S boundary by the double thymidine block procedure undergo a rapid synchronous round of DNA synthesis when released into thymidine-free medium. Analysis of glucocorticoid receptor binding indicates a rapid rise in cellular receptor number when measurements are made in whole cells at either 3 C (cytoplasmic) or 37 C (nuclear). Cytoplasmic receptors are maintained at levels about 150% above late GI values throughout S and GII phases until mitosis occurs, whereas the nuclear binding of hormone is dramatically reduced during GII and remains low during mitosis and early GI. Similar cell cycle-dependent alterations in receptor number occur in synchronized cell populations obtained by unit gravity sedimentation. Sucrose density gradient analysis and Sephacryl S-200 gel filtration of cytoplasmic receptors during the cell cycle indicate a rapid increase in approximately 7–8S dexamethasonebinding component during early S phase, when receptors accumulate in cells. The role of RNA, protein, and DNA syntheses in mediating this S phase increase in receptor number were next examined. Both cycloheximide and puromycin blocked the increased receptor accumulation that occurs during the S phase, whereas delayed addition of these inhibitors led to partial increases in receptor binding. Several inhibitors of RNA synthesis [actinomycin D, L-521,818-00E10 (Merck), and a-amanitin] all effectively inhibited the S phase accumulation of receptor. Increased receptor binding during the S phase was not dependent on DNA replication. These data suggest that the increase in glucocorticoid receptor number during the S phase results from alterations in RNA and protein synthetic processesKeywords
This publication has 7 references indexed in Scilit:
- Pyridoxal phosphate induced alterations in glucocorticoid receptor metabolism by proteasesBiochemistry, 1980
- Glucocorticoids and lymphocytes. II. Cell cycle-dependent changes in glucocorticoid receptor content.The Journal of Immunology, 1980
- Modulation of glucocorticoid effects and steroid receptor binding in butyrate-treated HeLa S3 cellsArchives of Biochemistry and Biophysics, 1980
- The asymmetric segregation of parental nucleosomes during chromosome replicationCell, 1979
- Comparison of glucocorticoid-receptor complex binding to nuclei and DNA cellulose Evidence for different forms of interactionBiochimica et Biophysica Acta (BBA) - General Subjects, 1978
- Synchronization of mammalian cells in vitro by inhibition of the DNA synthesisExperimental Cell Research, 1966
- A Method for Determining the Sedimentation Behavior of Enzymes: Application to Protein MixturesJournal of Biological Chemistry, 1961