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   Effects of PB190 and PB212,new σ receptor ligands,on glucocorticoid receptor-mediated gene transcription in LMCAT cells  
   
نویسنده skuza g. ,szymańska m. ,budziszewska b. ,abate c. ,berardi f.
منبع pharmacological reports - 2011 - دوره : 63 - شماره : 6 - صفحه:1564 -1568
چکیده    The hyperactivity of the hypothalamic-pituitary-adrenocortical (hpa) axis is often observed in patientswith major depression. it has even been implicated in the pathophysiology of this disease. some antidepressant drugs (ads) inhibit glucocorticoid receptor (gr) function under in vitro conditions. the σ1 receptor agonists reveal potential antidepressant activity in animals,moreover,igmesine is promising as an ad in humans. as already shown,σ receptors are involved in stress-induced responses (e.g.,conditioned fear stress in mice). the aim of the present study was to find out whether the new selective σ receptor ligands,pb190 and pb212,are able to affect directly the endocrine system activity. to this end,we evaluated their influence on gr function in mouse fibroblast cells (l929),stably transfected with mouse mammary tumor virus-chloramphenicol acetyltransferase (mmtv-cat) plasmid (lmcat cells). fluvoxamine,a selective serotonin reuptake inhibitor,recognized as a σ1 receptor agonist was used for comparison. the obtained results showed that both pb190 and pb212 (potential σ1 receptor agonist and antagonist,respectively) like fluvoxamine,decreased the corticosterone-induced cat activity in a concentration-dependent manner. the significance of this fact remains ambiguous and requires further studies. copyright © 2011 by institute of pharmacology polish academy of sciences.
کلیدواژه Fibroblast cells; Glucocorticoid-mediated gene transcription; PB190; PB212; Selective σ ligands
آدرس department of pharmacology,polish academy of sciences,pl 31-343 kraków, Poland, department of experimental neuroendocrinology,polish academy of sciences,smȩtna 12,pl 31-343 kraków, Poland, department of experimental neuroendocrinology,polish academy of sciences,smȩtna 12,pl 31-343 kraków,poland,department of biochemical toxicology,jagiellonian university,medical college,medyczna 9,pl 30-688 kraków, Poland, dipartimento farmacochimico,università degli studi di bari,via orabona 4,70125 bari, Italy, dipartimento farmacochimico,università degli studi di bari,via orabona 4,70125 bari, Italy
 
     
   
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