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首页> 外文期刊>Recent Patents on CNS Drug Discovery >Insulin-Like Growth Factor-1 and its Derivatives: Potential Pharmaceutical Application for Ischemic Brain Injury
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Insulin-Like Growth Factor-1 and its Derivatives: Potential Pharmaceutical Application for Ischemic Brain Injury

机译:胰岛素样生长因子-1及其衍生物:缺血性脑损伤的潜在药物应用。

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摘要

Brain ischemia induces the IGF-1 system in damaged regions, and exogenous administration of IGF-1 after injury is neuroprotective and improves long-term neurological function. The short treatment window can be extended by mild hypothermia, probably due to delayed apoptosis. Nevertheless, the poor central uptake of IGF-1 and its mitogenic potential preclude clinical application.nnThe N-terminal tripeptide of IGF-1 (glycine-proline-glutamate, GPE) is neuroprotective after central administration. Central uptake of GPE is injury dependent, and it is rapidly degraded in the plasma. Intravenous infusion of GPE prevents brain injury and improves long-term functional recovery, with a broad effective dose range and a 3-7 hour therapeutic window. GPE does not interact with IGF receptors. G-2meth-PE, a GPE analogue with improved stability, has a prolonged plasma half life and is neuroprotective after ischemic injury. Neuroprotection by GPE and its analogue may involve modulating inflammation, promoting astrocytosis and inhibiting apoptosis, and the analogue may have a vascular effect.nnCyclo-glycyl-proline (cGP) is an endogenous diketopiperazine possibly derived from GPE. Cyclic GP and its analogue cyclo-L-glycyl-L-2-allylproline (cG-2allylP) are neuroprotective after ischemic injury. cG-2allylP crosses the BBB independent of injury and remains detectable several hours after a single administration. Repeated peripheral administration of cG-2allyP improves somatosensory-motor function and long-term histological outcome.
机译:脑缺血可在受损区域诱导IGF-1系统,损伤后外源给予IGF-1具有神经保护作用,并改善长期神经功能。短暂的治疗窗口可通过温和的低温延长,可能是由于细胞凋亡延迟所致。然而,IGF-1的中枢摄取较差及其有丝分裂潜力阻碍了临床应用。nn中枢给药后,IGF-1的N端三肽(甘氨酸-脯氨酸-谷氨酸,GPE)具有神经保护作用。 GPE的中枢摄取与损伤有关,并且在血浆中迅速降解。静脉内输注GPE可预防脑损伤并改善长期功能恢复,并具有广泛的有效剂量范围和3-7小时的治疗窗口。 GPE不与IGF受体相互作用。 G-2meth-PE,一种具有改善的稳定性的GPE类似物,具有延长的血浆半衰期,并且在缺血性损伤后具有神经保护作用。 GPE及其类似物的神经保护作用可能涉及调节炎症,促进星形胶质细胞增多和抑制细胞凋亡,并且该类似物可能具有血管作用。nn-环糖基脯氨酸(cGP)是一种内源性二酮哌嗪,可能源自GPE。环GP及其类似物环-L-甘氨酰-L-2-烯丙基脯氨酸(cG-2allylP)在缺血性损伤后具有神经保护作用。 cG-2allylP不受损伤地穿过BBB,单次给药后数小时仍可检测到。重复外周施用cG-2allyP可改善体感运动功能和长期组织学结果。

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