选择性p38抑制剂SB - 239063可保护原代神经元免受轻度至中度兴奋性毒性损伤。

The selective p38 inhibitor SB-239063 protects primary neurons from mild to moderate excitotoxic injury.

作者信息

Legos Jeffrey J, McLaughlin BethAnn, Skaper Stephen D, Strijbos Paul J L M, Parsons Andrew A, Aizenman Elias, Herin Greta A, Barone Frank C, Erhardt Joseph A

机构信息

High Throughput Biology, Discovery Research, GlaxoSmithKline, PO Box 1539, Mail Code UW 2523, 709 Swedeland Road, 19406, King of Prussia, PA, USA.

出版信息

Eur J Pharmacol. 2002 Jun 28;447(1):37-42. doi: 10.1016/s0014-2999(02)01890-3.

DOI:10.1016/s0014-2999(02)01890-3

PMID:12106800

Abstract

Inhibition of the p38 mitogen-activated protein kinase (MAP Kinase) pathway reduces acute ischemic injury in vivo, suggesting a direct role for this signaling pathway in a number of neurodegenerative processes. The present study was designed to evaluate further the role of p38 MAP Kinase in acute excitotoxic neuronal injury using the selective p38 inhibitor SB-239063 (trans-1-(4hydroxycyclohexyl)-4-(fluorophenyl)-5-(2-methoxy-pyrimidin-4-yl) imidazole). Unlike the widely used p38 inhibitor, SB-203580 (4-(4-Fluorophenyl)-2-(4-methylsulfinylphenyl)-5-(4-pyridyl)1H-imidazole), this second generation p38 inhibitor more selectively inhibits p38 MAP Kinase without affecting the activity of other MAP Kinase signaling pathways and provides a more accurate means to selectively assess the role of p38 in excitotoxicity that has not been previously possible. SB-239063 provided substantial protection against cell death induced by either oxygen glucose deprivation (OGD) or magnesium deprivation in cultured neurons. The ability of this compound to block excitotoxicity was not due to direct inhibition of N-methyl-D-aspartate (NMDA) receptor-mediated currents as SB-239063 did not alter NMDA electrophysiological responses. SB-239063 did not protect against a severe excitotoxic insult induced by 60-min exposure to NMDA. However, when tested against a less severe, brief (5 min) NMDA exposure, p38 inhibition provided substantial protection. These data demonstrate that inhibition of p38 MAP Kinase can confer neuroprotection in vitro against mild but not severe excitotoxic exposure, and suggests that other additional pathways/mechanism(s) may be involved in severe excitotoxic cell death.

摘要

抑制p38丝裂原活化蛋白激酶（MAP激酶）信号通路可减轻体内急性缺血性损伤，提示该信号通路在多种神经退行性病变过程中发挥直接作用。本研究旨在使用选择性p38抑制剂SB - 239063（反式 - 1 -（4 - 羟基环己基）- 4 -（氟苯基）- 5 -（2 - 甲氧基嘧啶 - 4 - 基）咪唑）进一步评估p38 MAP激酶在急性兴奋性毒性神经元损伤中的作用。与广泛使用的p38抑制剂SB - 203580（4 -（4 - 氟苯基）- 2 -（4 - 甲基亚磺酰基苯基）- 5 -（4 - 吡啶基）- 1H - 咪唑）不同，这种第二代p38抑制剂能更选择性地抑制p38 MAP激酶，而不影响其他MAP激酶信号通路的活性，为选择性评估p38在兴奋性毒性中的作用提供了一种更准确的方法，这在以前是不可能的。SB - 239063为培养神经元中由氧葡萄糖剥夺（OGD）或镁剥夺诱导的细胞死亡提供了显著的保护作用。该化合物阻断兴奋性毒性的能力并非由于直接抑制N - 甲基 - D - 天冬氨酸（NMDA）受体介导的电流，因为SB - 239063并未改变NMDA的电生理反应。SB - 239063不能保护神经元免受60分钟NMDA诱导的严重兴奋性毒性损伤。然而，当针对较轻的、短暂（5分钟）的NMDA暴露进行测试时，p38抑制提供了显著的保护作用。这些数据表明，抑制p38 MAP激酶在体外可对轻度但非重度兴奋性毒性暴露起到神经保护作用，并提示其他额外的信号通路/机制可能参与了重度兴奋性毒性细胞死亡过程。