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Comparison of CCK-8 Receptors in the Pancreas and Brain of Rats Using CCK-8 Analogues

机译:使用CCK-8类似物比较大鼠胰腺和脑中CCK-8受体

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References(31) Cited-By(4) The characteristics of cholecystokinin (CCK) receptors in rat pancreatic acini and in various regions of the brain were examined using synthetic CCK-8 or CCK-7 analogues. 3H-propionylated CCK-8 ([3H]CCK-8) was used as a ligand. 1) The pancreatic CCK receptor had a single high affinity binding component with a dissociation constant, Kd, of 0.76 nM and a maximum number of specific binding sites, BmaX, of 271.91 fmol/mg protein. On the other hand, the CCK receptor in the cerebral cortex had a Kd of 1.66 nM and a BmaX of 30.15 fmol/mg protein. 2) The order of the potencies of CCK-7 and CCK-8 analogues with a substitution at position 3 or 4 to displace [3H]CCK-8 specific binding to the pancreatic acini was as follows: CCK-8CCK-7=SucCCK-7Suc[Sar3]CCK-7Suc[D-Trp3]CCK-7 Suc[D-Ala3]CCK-7[D-Trp4]CCK-8=[D-Ala4]CCK-8. This order of potencies of CCK analogues was greatly different from that in the cerebral cortex. 3) The carboxy-terminal tetra-peptide (CCK-4) and penta-peptide (CCK-5) had very weak potencies in displacing [3H]CCK-8 binding in the pancreatic acini, which were 20 to 30-fold less than their potencies in the cerebral cortex. These results suggest that the recognition sites for CCK analogues in the pancreatic and brain CCK receptors are different.
机译:参考文献(31)(4)用合成的CCK-8或CCK-7类似物检查了大鼠胰腺腺泡和大脑各个区域的胆囊收缩素(CCK)受体的特征。 3H-丙酰化的CCK-8([3H] CCK-8)用作配体。 1)胰腺CCK受体具有单个高亲和力结合组分,其解离常数Kd为0.76 nM,最大特异性结合位点BmaX为271.91 fmol / mg蛋白。另一方面,大脑皮层中的CCK受体的Kd为1.66 nM,BmaX为30.15 fmol / mg蛋白。 2)在3或4位被取代的CCK-7和CCK-8类似物取代[3H] CCK-8特异性结合胰腺腺泡的能力的顺序如下:CCK-8> CCK-7 = SucCCK-7> Suc [Sar3] CCK-7> Suc [D-Trp3] CCK-7> Suc [D-Ala3] CCK-7> [D-Trp4] CCK-8 = [D-Ala4] CCK-8。 CCK类似物的这种效力顺序与大脑皮层的效力有很大不同。 3)羧基末端四肽(CCK-4)和五肽(CCK-5)在置换[3H] CCK-8在胰腺腺泡中的结合时具有很弱的效力,比后者少20至30倍。它们在大脑皮层的效力。这些结果表明,在胰腺和脑CCK受体中CCK类似物的识别位点是不同的。

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