1 Laboratory of Neurotrauma and Biomarkers, Federal University of Rio Grande do Sul, Porto Alegre, Brazil.
2 Department of Biochemistry, Federal University of Rio Grande do Sul, Porto Alegre, Brazil.
J Neurotrauma. 2019 Jul 15;36(14):2246-2259. doi: 10.1089/neu.2018.6266. Epub 2019 Apr 9.
Traumatic brain injury (TBI) increases Ca influx into neurons and desynchronizes mitochondrial function leading to energy depletion and apoptosis. This process may be influenced by brain testosterone (TS) levels, which are known to decrease after TBI. We hypothesized that a TS-based therapy could preserve mitochondrial neuroenergetics after TBI, thereby reducing neurodegeneration. C57BL/6J mice were submitted to sham treatment or severe parasagittal controlled cortical impact (CCI) and were subcutaneously injected with either vehicle (VEH-SHAM and VEH-CCI) or testosterone cypionate (15 mg/kg, TS-CCI) for 10 days. Cortical tissue homogenates ipsilateral to injury were used for neurochemical analysis. The VEH-CCI group displayed an increased Ca-induced mitochondrial swelling after the addition of metabolic substrates (pyruvate, malate, glutamate, succinate, and adenosine diphosphate [PMGSA]). The addition of Na stimulated mitochondrial Ca extrusion through Na/Ca/Li exchanger (NCLX) in VEH-SHAM and TS-CCI, but not in the VEH-CCI group. Reduction in Ca efflux post-injury was associated with impaired mitochondrial membrane potential formation/dissipation, and decreased mitochondrial adenosine triphosphate (ATP)-synthase coupling efficiency. Corroborating evidence of mitochondrial uncoupling was observed with an increase in HO production post-injury, but not in superoxide dismutase (SOD2) protein levels. TS administration significantly reduced these neuroenergetic alterations. At molecular level, TS prevented the increase in pTau and alpha-Spectrin fragmentation by the Cadependent calpain-2 activation, and decreased both caspase-3 activation and Bax/BCL-2 ratio, which suggests a downregulation of mitochondrial apoptotic signals. Search Tool for the Retrieval of Interacting Genes/Proteins database provided two distinct gene/protein clusters, "upregulated and downregulated," interconnected through SOD2. Therefore, TS administration after a severe CCI improves the mitochondrial Caextrusion through NCLX exchanger and ATP synthesis efficiency, ultimately downregulating the overexpression of molecular drivers of neurodegeneration.
创伤性脑损伤 (TBI) 会增加神经元内的 Ca 流入,并使线粒体功能失步,导致能量耗竭和细胞凋亡。这个过程可能会受到大脑睾酮 (TS) 水平的影响,TBI 后 TS 水平已知会下降。我们假设,基于 TS 的治疗可以在 TBI 后维持线粒体神经能量代谢,从而减少神经退行性变。将 C57BL/6J 小鼠进行假手术或严重矢状旁皮质控制撞击 (CCI) 处理,并皮下注射载体 (VEH-SHAM 和 VEH-CCI) 或睾酮 Cypionate (15mg/kg,TS-CCI) 治疗 10 天。损伤对侧皮质组织匀浆用于神经化学分析。VEH-CCI 组在加入代谢底物 (丙酮酸、苹果酸、谷氨酸、琥珀酸和二磷酸腺苷 [PMGSA]) 后显示出 Ca 诱导的线粒体肿胀增加。加入 Na 通过 Na/Ca/Li 交换器 (NCLX) 刺激线粒体 Ca 外排,而 VEH-SHAM 和 TS-CCI 组则没有。损伤后 Ca 外排减少与线粒体膜电位形成/耗散受损以及线粒体三磷酸腺苷 (ATP)-合成酶偶联效率降低有关。损伤后 HO 生成增加表明线粒体解偶联,而超氧化物歧化酶 (SOD2) 蛋白水平没有增加。TS 给药显著减轻了这些神经能量变化。在分子水平上,TS 通过 Cadependent 钙蛋白酶-2 激活来阻止 pTau 和 alpha-Spectrin 片段的增加,并降低 caspase-3 激活和 Bax/BCL-2 比值,这表明线粒体凋亡信号下调。检索相互作用基因/蛋白的工具数据库提供了两个不同的基因/蛋白簇,“上调和下调”,通过 SOD2 相互连接。因此,严重 CCI 后给予 TS 可通过 NCLX 交换器和 ATP 合成效率改善线粒体 Ca 外排,最终下调神经退行性变的分子驱动因子的过表达。
