星形细胞截断原肌球蛋白受体激酶 B 介导脑源性神经营养因子抗细胞凋亡作用,从而实现神经保护。
Astrocyte truncated tropomyosin receptor kinase B mediates brain-derived neurotrophic factor anti-apoptotic effect leading to neuroprotection.
机构信息
Instituto de Investigaciones Biomédicas (INBIOMED) UBA-CONICET, Paraguay 2155, Facultad de Medicina, Universidad de Buenos Aires, Buenos Aires, Argentina.
出版信息
J Neurochem. 2018 Sep;146(6):686-702. doi: 10.1111/jnc.14476. Epub 2018 Aug 9.
UNLABELLED
Astrocytes are glial cells that help maintain brain homeostasis and become reactive in neurodegenerative processes releasing both harmful and beneficial factors. We have demonstrated that brain-derived neurotrophic factor (BDNF) expression is induced by melanocortins in astrocytes but BDNF actions in astrocytes are largely unknown. We hypothesize that BDNF may prevent astrocyte death resulting in neuroprotection. We found that BDNF increased astrocyte viability, preventing apoptosis induced by serum deprivation by decreasing active caspase 3 and p53 expression. The anti-apoptotic action of BDNF was abolished by ANA-12 (a specific TrkB antagonist) and by K252a (a general Trk antagonist). Astrocytes only express the BDNF receptor TrkB-truncated isoform 1, TrkB-T1. BDNF induced ERK, Akt, and Src (a non-receptor tyrosine kinase) activation in astrocytes. Blocking ERK and Akt pathways abolished BDNF protection in serum deprivation-induced cell death. Moreover, BDNF protected astrocytes from death by 3-nitropropionic acid (3-NP), an effect also blocked by ANA-12, K252a, and inhibitors of ERK, calcium, and Src. BDNF reduced reactive oxygen species levels induced in astrocytes by 3-NP and increased xCT expression and glutathione levels. Astrocyte-conditioned medium (ACM) from untreated astrocytes partially protected PC12 neurons, whereas ACM from BDNF-treated astrocytes completely protected PC12 neurons from 3-NP-induced apoptosis. Both ACM from control and BDNF-treated astrocytes markedly reduced reactive oxygen species levels induced by 3-NP in PC12 cells. Our results demonstrate that BDNF protects astrocytes from cell death through TrkB-T1 signaling, exerts an antioxidant action, and induces release of neuroprotective factors from astrocytes.
OPEN PRACTICES
Open Science: This manuscript was awarded with the Open Materials Badge. For more information see: https://cos.io/our-services/open-science-badges/.
未标记
星形胶质细胞是神经胶质细胞,有助于维持大脑内环境平衡,并在神经退行性过程中产生反应,释放有害和有益的因素。我们已经证明,脑源性神经营养因子(BDNF)在星形胶质细胞中的表达是由黑色素细胞刺激素诱导的,但 BDNF 在星形胶质细胞中的作用在很大程度上尚不清楚。我们假设 BDNF 可能防止星形胶质细胞死亡,从而起到神经保护作用。我们发现,BDNF 通过降低活性 caspase 3 和 p53 的表达,增加了星形胶质细胞的活力,防止了血清剥夺诱导的细胞凋亡。BDNF 的抗凋亡作用被 ANA-12(一种特定的 TrkB 拮抗剂)和 K252a(一种通用的 Trk 拮抗剂)所阻断。星形胶质细胞仅表达 BDNF 受体 TrkB 截断型 1 异构体,即 TrkB-T1。BDNF 诱导星形胶质细胞中 ERK、Akt 和 Src(一种非受体酪氨酸激酶)的激活。阻断 ERK 和 Akt 通路可使 BDNF 在血清剥夺诱导的细胞死亡中失去保护作用。此外,BDNF 通过 3-硝基丙酸(3-NP)保护星形胶质细胞免于死亡,这一作用也被 ANA-12、K252a 和 ERK、钙和 Src 的抑制剂所阻断。BDNF 降低了 3-NP 诱导的星形胶质细胞中活性氧物质的水平,并增加了 xCT 的表达和谷胱甘肽的水平。未经处理的星形胶质细胞的星形胶质细胞条件培养基(ACM)部分保护 PC12 神经元,而经 BDNF 处理的星形胶质细胞的 ACM 则完全保护 PC12 神经元免受 3-NP 诱导的细胞凋亡。控制和 BDNF 处理的星形胶质细胞的 ACM 都明显降低了 3-NP 在 PC12 细胞中诱导的活性氧物质水平。我们的结果表明,BDNF 通过 TrkB-T1 信号通路保护星形胶质细胞免于死亡,发挥抗氧化作用,并诱导星形胶质细胞释放神经保护因子。
公开实践
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