Research Institute for Reproduction, School of Medicine, University of Buenos Aires, Ciudad Autónoma de Buenos Aires, Beunos Aires, Argentina.
PLoS One. 2011;6(7):e22235. doi: 10.1371/journal.pone.0022235. Epub 2011 Jul 14.
In recent decades, astrocytes have emerged as key pieces in the maintenance of normal functioning of the central nervous system. Any impairment in astroglial function can ultimately lead to generalized disturbance in the brain, thus pharmacological targets associated with prevention of astrocyte death are actually promising. Subtype 3 of metabotropic glutamate receptors (mGluR3) is present in astrocytes, its activation exerting neuroprotective roles. In fact, we have previously demonstrated that mGluR3 selective agonists prevent nitric oxide (NO)-induced astrocyte death. However, mechanisms responsible for that cytoprotective property are still subject to study. Although inhibition of adenylyl cyclase by mGluR3 activation was extensively reported, the involvement of reduced cAMP levels in the effects of mGluR3 agonists and the association between cAMP decrease and the downstream pathways activated by mGluR3 remain neglected. Thus, we studied intracellular signaling mediating anti-apoptotic actions of mGluR3 in cultured rat astrocytes exposed to NO. In the present work, we showed that the cytoprotective effect of mGluR3 agonists (LY379268 and LY404039) requires both the reduction of intracellular cAMP levels and activation of Akt, as assessed by MTT and TUNEL techniques. Moreover, dibutyryl-cAMP impairs Akt phosphorylation induced by LY404039, indicating a relationship between mGluR3-reduced cAMP levels and PI3K/Akt pathway activation. We also demonstrated, by co-immunoprecipitation followed by western-blot, that the mGluR3 agonists not only induce per se survival-linked interaction between members of the NF-κB family p65 and c-Rel, but also impede reduction of levels of p65-c-Rel dimers caused by NO, suggesting a possible anti-apoptotic role for p65-c-Rel. All together, these data suggest that mGluR3 agonists may regulate cAMP/Akt/p65-c-Rel pathway, which would contribute to the protective effect of mGluR3 against NO challenge in astrocytes. Our results widen the knowledge about mechanisms of action of mGluR3, potential targets for the treatment of neurodegenerative disorders where a pathophysiological role for NO has been established.
在最近几十年中,星形胶质细胞已成为维持中枢神经系统正常功能的关键部分。星形胶质细胞功能的任何损伤最终都会导致大脑的普遍紊乱,因此与预防星形胶质细胞死亡相关的药理学靶标实际上很有前途。代谢型谷氨酸受体 3 型(mGluR3)存在于星形胶质细胞中,其激活发挥神经保护作用。实际上,我们之前已经证明,mGluR3 选择性激动剂可防止一氧化氮(NO)诱导的星形胶质细胞死亡。但是,负责这种细胞保护特性的机制仍在研究中。尽管 mGluR3 激活引起的腺苷酸环化酶抑制作用已被广泛报道,但 mGluR3 激动剂降低 cAMP 水平的作用以及 cAMP 降低与 mGluR3 激活的下游途径之间的关联仍被忽视。因此,我们研究了暴露于 NO 的培养的大鼠星形胶质细胞中 mGluR3 介导的抗凋亡作用的细胞内信号传导。在本工作中,我们表明 mGluR3 激动剂(LY379268 和 LY404039)的细胞保护作用需要降低细胞内 cAMP 水平和激活 Akt,如 MTT 和 TUNEL 技术所评估的那样。此外,二丁酰基-cAMP 会损害 LY404039 诱导的 Akt 磷酸化,表明 mGluR3 降低的 cAMP 水平与 PI3K/Akt 途径的激活之间存在关系。我们还通过免疫沉淀 followed by western-blot 证明,mGluR3 激动剂不仅诱导 NF-κB 家族成员 p65 和 c-Rel 之间本身就与生存相关的相互作用,而且还阻止了 NO 引起的 p65-c-Rel 二聚体水平的降低,表明 p65-c-Rel 可能具有抗凋亡作用。所有这些数据表明,mGluR3 激动剂可能调节 cAMP/Akt/p65-c-Rel 途径,这将有助于 mGluR3 抵抗星形胶质细胞中 NO 挑战的保护作用。我们的结果拓宽了 mGluR3 作用机制的知识,为已经建立了 NO 病理生理作用的神经退行性疾病的治疗提供了潜在的靶标。
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