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   Assessment of novel muscarinic acetylcholine receptors in rat cerebral cortex by a tissue segment binding method  
   
نویسنده lee k.-s. ,nishimune a. ,yoshiki h. ,anisuzzaman a.s.m. ,suzuki f. ,wang m.-h. ,cheng j.-t. ,muramatsu i.
منبع journal of pharmacological sciences - 2010 - دوره : 112 - شماره : 4 - صفحه:444 -451
چکیده    Muscarinic acetylcholine receptors (machrs) of rat cerebral cortex were evaluated using a tissue segment radioligand binding assay. [3h]-quinuclidinyl benzilate (qnb,a hydrophobic ligand) specifically bound to machrs in the cortex segments. the total machrs level was approximately 2,000 fmol/mg protein,which was estimated after incubation for 120 min at 37°c or for 8 h at 4°c. these machrs were a mixture of high - and low-affinity sites for n-methylsco-polamine (nms) in a 70:30 ratio. in contrast,only a single high-affinity site for nms was detected following incubation for 30 min at 37°c,whose abundance was about 70% of that of the total machrs. atropine showed a single affinity for machrs under all conditions. these indicate that machrs are constitutively expressed not only on plasma membrane sites but also at intracellular sites in rat cerebral cortex and that the receptors at both sites have different affinities for nms. acetylcholine completely inhibited [3h]-qnb binding to both machrs without any change in the subcellular distribution,suggesting the possibility that acetylcholine can access,and bind to,both machrs in intact tissue. two different affinity states for acetylcholine were detected only in plasma membrane machrs at 37°c. the present study demonstrates a unique subcellular distribution,and distinct pharmacological profiles,of machrs in rat cerebral cortex. ©2010 the japanese pharmacological society.
کلیدواژه Intracellular receptor; Muscarinic acetylcholine receptor; Quinuclidinyl benzilate; Rat cerebral cortex; Tissue segment binding assay
آدرس division of pharmacology,department of biochemistry and bioinformative sciences,school of medicine,eiheiji-matsuoka,fukui 910-1193,japan,department of surgery,kaohsiung municipal hsiao-kang hospital,faculty of medicine,college of medicine,kaohsiung medical university,kaohsiung 80708, Taiwan, division of pharmacology,department of biochemistry and bioinformative sciences,school of medicine,eiheiji-matsuoka,fukui 910-1193,japan,organization for life science advancement programs,university of fukui,eiheiji-matsuoka,fukui 910-1193, Japan, division of pharmacology,department of biochemistry and bioinformative sciences,school of medicine,eiheiji-matsuoka,fukui 910-1193, Japan, division of pharmacology,department of biochemistry and bioinformative sciences,school of medicine,eiheiji-matsuoka,fukui 910-1193, Japan, division of pharmacology,department of biochemistry and bioinformative sciences,school of medicine,eiheiji-matsuoka,fukui 910-1193,japan,organization for life science advancement programs,university of fukui,eiheiji-matsuoka,fukui 910-1193, Japan, division of pharmacology,department of biochemistry and bioinformative sciences,school of medicine,eiheiji-matsuoka,fukui 910-1193, Japan, department of pharmacology,college of medicine,national cheng kung university,tainan 70101, Taiwan, division of pharmacology,department of biochemistry and bioinformative sciences,school of medicine,eiheiji-matsuoka,fukui 910-1193,japan,organization for life science advancement programs,university of fukui,eiheiji-matsuoka,fukui 910-1193, Japan
 
     
   
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