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Insulin transport across the blood–brain barrier can occur independently of the insulin receptor

机译:血脑屏障过的胰岛素输送可以独立于胰岛素受体发生

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Key points Insulin enters the brain from the blood via a saturable transport system. It is unclear how insulin is transported across the blood–brain barrier (BBB). Using two models of the signalling‐related insulin receptor loss or inhibition, we show insulin transport can occur in vivo without the signalling‐related insulin receptor. Insulin in the brain has multiple roles including acting as a metabolic regulator and improving memory. Understanding how insulin is transported across the BBB will aid in developing therapeutics to further increase CNS concentrations. Abstract A saturable system transports insulin from blood across the blood–brain barrier (BBB) and into the central nervous system. Whether or not the classic or signalling‐related insulin receptor plays a role in mediating this transport in vivo is controversial. Here, we employed kinetics methods that distinguish between transport across the brain endothelial cell and reversible luminal surface receptor binding. Using a previously established line of mice with endothelial‐specific loss of the signalling‐related insulin receptor (EndoIRKO) or inhibiting the insulin receptor with the selective antagonist S961, we show insulin transport across the BBB is maintained. Rates of insulin transport were similar in all groups and transport was still saturable. Unlike transport, binding of insulin to the brain endothelial cell was decreased with the loss or inhibition of the signalling‐related insulin receptor. These findings demonstrate that the signalling‐related insulin receptor is not required for insulin transport across the BBB.
机译:关键点胰岛素通过可饱和的运输系统从血液进入脑。目前尚不清楚胰岛素在血脑屏障(BBB)上如何运输。使用与信号传导相关的胰岛素受体损失或抑制的两种模型,我们展示胰岛素运输可以在没有信号相关的胰岛素受体的情况下在体内发生。大脑中的胰岛素具有多种作用,包括作为代谢调节剂和改善记忆。了解胰岛素在BBB上如何运输,将有助于开发治疗方法以进一步增加CNS浓度。摘要一种可饱和的系统将胰岛素从血脑屏障(BBB)中的血液中传递给中枢神经系统。无论经典或信令相关的胰岛素受体是否在介导这种情况下在体内发挥作用是有争议的。在这里,我们采用动力学方法,区分脑内皮细胞和可逆腔表面受体结合的运输。使用先前建立的小鼠与信号相关胰岛素受体(Endoirko)的内皮特异性损失或用选择性拮抗剂S961抑制胰岛素受体,我们在保持BBB上显示胰岛素输送。所有组的胰岛素转运率相似,并且运输仍然是可饱和的。与传输不同,随着信号传导相关的胰岛素受体的损失或抑制,降低了胰岛素对脑内皮细胞的结合。这些发现表明,信令相关的胰岛素受体不需要在BBB上进行胰岛素输送。

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