组织金属蛋白酶抑制剂 3 通过 TNF-α/TACE 介导局灶性脑缺血小鼠未成熟少突胶质细胞的死亡。
Tissue inhibitor of metalloproteinases-3 mediates the death of immature oligodendrocytes via TNF-α/TACE in focal cerebral ischemia in mice.
机构信息
Department of Neurology, University of New Mexico Health Sciences Center, Albuquerque, NM 87131, USA.
出版信息
J Neuroinflammation. 2011 Aug 29;8:108. doi: 10.1186/1742-2094-8-108.
BACKGROUND AND PURPOSE
Oligodendrocyte (OL) death is important in focal cerebral ischemia. TIMP-3 promotes apoptosis in ischemic neurons by inhibiting proteolysis of TNF-α superfamily of death receptors. Since OLs undergo apoptosis during ischemia, we hypothesized that TIMP-3 contributes to OL death.
METHODS
Middle cerebral artery occlusion (MCAO) was induced in Timp-3 knockout (KO) and wild type (WT) mice with 24 or 72 h of reperfusion. Cell death in white matter was investigated by stereology and TUNEL. Mature or immature OLs were identified using antibodies against glutathione S-transferase-π (GST-π) and galactocerebroside (GalC), respectively. Expression and level of proteins were examined using immunohistochemistry and immunoblotting. Protein activities were determined using a FRET peptide.
RESULTS
Loss of OL-like cells was detected at 72 h only in WT ischemic white matter where TUNEL showed greater cell death. TIMP-3 expression was increased in WT reactive astrocytes. GST-π was reduced in ischemic white matter of WT mice compared with WT shams with no difference between KO and WT at 72 h. GalC level was significantly increased in both KO and WT ischemic white matter at 72 h. However, the increase in GalC in KO mice was significantly higher than WT; most TUNEL-positive cells in ischemic white matter expressed GalC, suggesting TIMP-3 deficiency protects the immature OLs from apoptosis. There were significantly higher levels of cleaved caspase-3 at 72 h in WT white matter than in KO. Greater expression of MMP-3 and -9 was seen in reactive astrocytes and/or microglia/macrophages in WT at 72 h. We found more microglia/macrophages in WT than in KO, which were the predominant source of increased TNF-α detected in the ischemic white matter. TACE activity was significantly increased in ischemic WT white matter, which was expressed in active microglia/macrophages and OLs.
CONCLUSIONS
Our results suggested that focal ischemia leads to proliferation of immature OLs in white matter and that TIMP-3 contributes to a caspase-3-dependent immature OL death via TNF-α-mediated neuroinflammation. Future studies will be needed to delineate the role of MMP-3 and MMP-9 that were increased in the Timp-3 wild type.
背景与目的
少突胶质细胞(OL)死亡在局灶性脑缺血中很重要。TIMP-3 通过抑制 TNF-α 超家族死亡受体的蛋白水解来促进缺血性神经元的凋亡。由于 OL 在缺血过程中发生凋亡,我们假设 TIMP-3 有助于 OL 死亡。
方法
通过大脑中动脉闭塞(MCAO)诱导 Timp-3 敲除(KO)和野生型(WT)小鼠 24 或 72 小时再灌注。通过立体学和 TUNEL 研究白质中的细胞死亡。使用针对谷胱甘肽 S-转移酶-π(GST-π)和半乳糖脑苷脂(GalC)的抗体分别鉴定成熟或不成熟的 OL。使用免疫组织化学和免疫印迹检查蛋白质的表达和水平。使用 FRET 肽测定蛋白质活性。
结果
仅在 WT 缺血性白质中观察到 72 小时时 OL 样细胞的丢失,TUNEL 显示细胞死亡更多。TIMP-3 在 WT 反应性星形胶质细胞中表达增加。与 WT 假手术相比,WT 缺血性白质中的 GST-π 减少,而 KO 和 WT 之间在 72 小时时没有差异。GalC 水平在 KO 和 WT 缺血性白质中均在 72 小时时显著增加;缺血性白质中大多数 TUNEL 阳性细胞表达 GalC,表明 TIMP-3 缺乏可保护不成熟的 OL 免于凋亡。WT 白质中的 cleaved caspase-3 水平在 72 小时时显著高于 KO。WT 中反应性星形胶质细胞和/或小胶质细胞/巨噬细胞中 MMP-3 和 MMP-9 的表达更高在 72 小时时。我们发现 WT 中的小胶质细胞/巨噬细胞比 KO 中的多,WT 缺血性白质中检测到的 TNF-α的主要来源是增加的小胶质细胞/巨噬细胞。TACE 活性在缺血性 WT 白质中显著增加,该活性在活性小胶质细胞/巨噬细胞和 OL 中表达。
结论
我们的结果表明,局灶性缺血导致白质中不成熟 OL 的增殖,并且 TIMP-3 通过 TNF-α 介导的神经炎症导致 caspase-3 依赖性不成熟 OL 死亡。需要进一步研究来阐明 MMP-3 和 MMP-9 的作用,这些因子在 Timp-3 野生型中增加。
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