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大鼠脑中具有高亲和力(3H)地西泮结合特性的特异性苯二氮䓬受体。

Specific benzodiazepine receptors in rat brain characterized by high-affinity (3H)diazepam binding.

作者信息

Braestrup C, Squires R F

出版信息

Proc Natl Acad Sci U S A. 1977 Sep;74(9):3805-9. doi: 10.1073/pnas.74.9.3805.

Abstract

[3H]Diazepam appears to bind specifically to a single, saturable, binding site located on rat brain membranes, with an affinity constant near 3 nM at pH 7.4. Specific binding constitutes more than 90% of total binding at 0 degrees and less than 10% of total binding at 37 degrees. Arrhenius plots suggest a sharp conformational change in the diazepam receptor near 18 degrees. Mitochondrial fractions from rat kidney, liver, and lung exhibit some [3H]diazepam binding that can be displaced by nonradioactive diazepam and several other benzodiazepines. However, Ro-4864, which is almost inactive in displacing [3H]diazepam from brain membranes, is extremely potent in displacing it from kidney mitochondria. Conversely, clonazepam, the most potent inhibitor of brain binding, is an extremely weak inhibitor of kidney binding. Furthermore, diazepam binding to kidney mitochondria has an affinity constantof 40 nM, about 15 times higher than that in brain. No specific diazepam binding was detected in intestine or skeletal muscle. Thus, specific [3H]diazepam binding to membranes appears to be restricted to brain, where it is unevenly distributed: the density of diazepam receptors is about five times higher in cortex (the highest density) than in pons-meddula (lowest density). Trypsin and chymotrypsin completely abolished specific [3H]diazepambinding in brain and kidney.

摘要

[3H]地西泮似乎特异性地结合于大鼠脑膜上的单一、可饱和结合位点,在pH 7.4时其亲和常数接近3 nM。特异性结合在0℃时占总结合的90%以上,在37℃时占总结合的不到10%。阿累尼乌斯曲线表明地西泮受体在18℃附近有急剧的构象变化。大鼠肾脏、肝脏和肺的线粒体组分表现出一些[3H]地西泮结合,可被非放射性地西泮和其他几种苯二氮䓬类药物取代。然而,Ro-4864在从脑膜上取代[3H]地西泮方面几乎没有活性,但在从肾脏线粒体中取代它方面却极具效力。相反,氯硝西泮是脑结合的最有效抑制剂,却是肾脏结合的极弱抑制剂。此外,地西泮与肾脏线粒体的结合亲和常数为40 nM,约为脑中的15倍。在肠道或骨骼肌中未检测到特异性地西泮结合。因此,[3H]地西泮与膜的特异性结合似乎仅限于脑,且在脑中分布不均:地西泮受体密度在皮质(最高密度)比在脑桥-延髓(最低密度)高约五倍。胰蛋白酶和糜蛋白酶完全消除了脑和肾中的特异性[3H]地西泮结合。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5c6c/431738/0a487234971e/pnas00031-0190-a.jpg

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