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首页> 外文期刊>Current Neuropharmacology >The ERK 1 and 2 Pathway in the Nervous System: From Basic Aspects to Possible Clinical Applications in Pain and Visceral Dysfunction
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The ERK 1 and 2 Pathway in the Nervous System: From Basic Aspects to Possible Clinical Applications in Pain and Visceral Dysfunction

机译:神经系统的ERK 1和2途径:从基本方面到疼痛和内脏功能障碍的可能临床应用

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摘要

The extracellular signal-regulated kinases 1 and 2 (ERK) cascade, member of the mitogen-activated protein kinases superfamily of signalling pathways, is one of the best characterized pathways as many protein interactions and phosphorylation events have been systematically studied. Traditionally, ERK are associated with the regulation of proliferation and differentiation as well as survival of various cell types. Their activity is controlled by phosphorylation on specific aminoacidic residues, which is induced by a variety of external cues, including growth-promoting factors.nnIn the nervous system, ERK phosphorylation is induced by binding of neurotrophins to their specific tyrosine kinase receptors or by neuronal activity leading to glutamate release and binding to its ionotropic and metabotropic receptors. Some studies have provided evidence of its importance in neuroplastic events. In particular, ERK phosphorylation in the spinal cord was shown to be nociceptive-specific and its upregulation, occurring in cases of chronic inflammatory and neuropathic pain, seems to be of the utmost importance to behavioural changes observed in those conditions. In fact, experiments using specific inhibitors of ERK phosphorylation have proved that ERK directly contributes to allodynia and hyperalgesia caused by spinal cord injury or chronic pain. Additionally, spinal ERK phosphorylation regulates the micturition reflex in experimental models of bladder inflammation and chronic spinal cord transection.nnIn this review we will address the main findings that suggest that ERK might be a future therapeutic target to treat pain and other complications arising from chronic pain or neuronal injury.
机译:细胞外信号调节激酶1和2(ERK)级联,信号通路的有丝分裂原活化蛋白激酶的超家族成员,是最有特色的途径之一,因为已经系统地研究了许多蛋白质相互作用和磷酸化事件。传统上,ERK与各种细胞类型的增殖和分化以及存活相关。它们的活性受特定氨基酸残基的磷酸化控制,而磷酸化是由多种外部线索(包括生长促进因子)诱导的。在神经系统中,ERK磷酸化是由于神经营养蛋白与特定酪氨酸激酶受体的结合或神经元活性引起的。导致谷氨酸释放并与其离子和代谢亲和受体结合。一些研究提供了其在神经塑性事件中重要性的证据。特别是,脊髓中的ERK磷酸化被证明具有伤害感受特异性,在慢性炎症和神经性疼痛的情况下,其上调似乎对于在这些情况下观察到的行为变化至关重要。实际上,使用ERK磷酸化特异性抑制剂的实验已证明ERK直接导致由脊髓损伤或慢性疼痛引起的异常性疼痛和痛觉过敏。此外,在膀胱炎症和慢性脊髓横断的实验模型中,脊柱ERK磷酸化调节排尿反射。或神经元损伤。

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