Kastin A J, Akerstrom V
Veterans Affairs Medical Center, New Orleans, Louisiana, USA.
J Pharmacol Exp Ther. 1999 Apr;289(1):219-23.
We determined the ability of orexin A and orexin B, recently discovered endogenous appetite enhancers, to cross the blood-brain barrier (BBB) of mice. Multiple time-regression analysis showed that an i.v. bolus of 125I-orexin A rapidly entered the brain from the blood, with an influx rate (Ki = 2.5 +/- 0.3 x 10(-4) ml/g.min) many times faster than that of the 99mTc-albumin control. This relatively rapid rate of entry was not reduced by administration of excess orexin A (or leptin) or by fasting for 22 h, even when penetration into only the hypothalamus was measured. Lack of saturability also was shown by perfusion in blood-free buffer. HPLC revealed that most of the injected 125I-orexin A reached the brain as intact peptide. Capillary depletion studies showed that the administered peptide did not remain bound to the endothelial cells comprising the BBB but reached the brain parenchyma. Efflux of 125I-orexin A from the brain occurred at the same rate as 99mTc-albumin. The octanol/buffer partition coefficient of 0.232 showed that orexin A was highly lipophilic, whereas the value for orexin B was only 0.030. Orexin B, moreover, was rapidly degraded in blood, so no 125I-orexin B could be detected in intact form in brain when injected peripherally. Thus, although orexin B is rapidly metabolized in blood and has low lipophilicity, orexin A rapidly crosses the BBB from blood to reach brain tissue by the process of simple diffusion.
我们测定了近期发现的内源性食欲增强剂食欲素A和食欲素B穿越小鼠血脑屏障(BBB)的能力。多次回归分析显示,静脉注射大剂量的125I-食欲素A能迅速从血液进入大脑,其流入速率(Ki = 2.5 +/- 0.3 x 10(-4) ml/g.min)比99mTc-白蛋白对照快许多倍。即使仅测量其在下丘脑的渗透情况,给予过量的食欲素A(或瘦素)或禁食22小时也不会降低这种相对较快的进入速率。在无血缓冲液中灌注也显示缺乏饱和性。高效液相色谱法显示,大部分注射的125I-食欲素A以完整肽的形式到达大脑。毛细血管耗竭研究表明,给予的肽并未与构成血脑屏障的内皮细胞结合,而是到达了脑实质。125I-食欲素A从大脑的流出速率与99mTc-白蛋白相同。辛醇/缓冲液分配系数为0.232,表明食欲素A具有高度亲脂性,而食欲素B的值仅为0.030。此外,食欲素B在血液中迅速降解,因此外周注射时,在大脑中无法检测到完整形式的125I-食欲素B。因此,尽管食欲素B在血液中迅速代谢且亲脂性低,但食欲素A通过简单扩散过程迅速从血液穿过血脑屏障到达脑组织。
