Bellusci Lorenza, Laurino Annunziatina, Sabatini Martina, Sestito Simona, Lenzi Paola, Raimondi Laura, Rapposelli Simona, Biagioni Francesca, Fornai Francesco, Salvetti Alessandra, Rossi Leonardo, Zucchi Riccardo, Chiellini Grazia
Laboratory of Biochemistry, Department of Pathology, University of Pisa, Pisa, Italy.
Section of Pharmacology and Toxicology, Department of Psychology, Neurology, Drug Sciences, Health of the Child, Pharmacology, University of Florence, Florence, Italy.
Front Pharmacol. 2017 Dec 12;8:905. doi: 10.3389/fphar.2017.00905. eCollection 2017.
3-Iodothyronamine (T1AM) is an endogenous high-affinity ligand of the trace amine-associated receptor 1 (TAAR1), detected in mammals in many organs, including the brain. Recent evidence indicates that pharmacological TAAR1 activation may offer a novel therapeutic option for the treatment of a wide range of neuropsychiatric and metabolic disorders. To assess potential neuroprotection by TAAR1 agonists, in the present work, we initially investigated whether T1AM and its corresponding 3-methylbiaryl-methane analog SG-2 can improve learning and memory when systemically administered to mice at submicromolar doses, and whether these effects are modified under conditions of MAO inhibition by clorgyline. Our results revealed that when i.p. injected to mice, both T1AM and SG-2 produced memory-enhancing and hyperalgesic effects, while increasing ERK1/2 phosphorylation and expression of transcription factor -fos. Notably, both compounds appeared to rely on the action of ubiquitous enzymes MAO to produce the corresponding oxidative metabolites that were then able to activate the histaminergic system. Since autophagy is key for neuronal plasticity, in a second line of experiments we explored whether T1AM and synthetic TAAR1 agonists SG1 and SG2 were able to induce autophagy in human glioblastoma cell lines (U-87MG). After treatment of U-87MG cells with 1 μM T1AM, SG-1, SG-2 transmission electron microscopy (TEM) and immunofluorescence (IF) showed a significant time-dependent increase of autophagy vacuoles and microtubule-associated protein 1 light chain 3 (LC3). Consistently, Western blot analysis revealed a significant increase of the LC3II/LC3I ratio, with T1AM and SG-1 being the most effective agents. A decreased level of the p62 protein was also observed after treatment with T1AM and SG-1, which confirms the efficacy of these compounds as autophagy inducers in U-87MG cells. In the process to dissect which pathway induces ATG, the effects of these compounds were evaluated on the PI3K-AKT-mTOR pathway. We found that 1 μM T1AM, SG-1 and SG-2 decreased pAKT/AKT ratio at 0.5 and 4 h after treatment, suggesting that autophagy is induced by inhibiting mTOR phosphorylation by PI3K-AKT-mTOR pathway. In conclusion, our study shows that T1AM and thyronamine-like derivatives SG-1 and SG-2 might represent valuable tools to therapeutically intervene with neurological disorders.
3-碘甲腺原氨酸(T1AM)是痕量胺相关受体1(TAAR1)的内源性高亲和力配体,在包括大脑在内的哺乳动物的许多器官中都能检测到。最近的证据表明,药理学上激活TAAR1可能为治疗多种神经精神和代谢紊乱提供一种新的治疗选择。为了评估TAAR1激动剂的潜在神经保护作用,在本研究中,我们首先研究了T1AM及其相应的3-甲基联芳基甲烷类似物SG-2在以亚微摩尔剂量全身给药于小鼠时是否能改善学习和记忆,以及在氯吉兰抑制单胺氧化酶(MAO)的条件下这些作用是否会改变。我们的结果显示,当腹腔注射给小鼠时,T1AM和SG-2都产生了记忆增强和痛觉过敏作用,同时增加了细胞外信号调节激酶1/2(ERK1/2)的磷酸化和转录因子-fos的表达。值得注意的是,这两种化合物似乎都依赖于普遍存在的酶MAO的作用来产生相应的氧化代谢产物,然后这些代谢产物能够激活组胺能系统。由于自噬是神经元可塑性的关键,在另一系列实验中,我们探究了T1AM和合成的TAAR1激动剂SG1和SG2是否能够在人胶质母细胞瘤细胞系(U-87MG)中诱导自噬。用1μM T1AM、SG-1、SG-2处理U-87MG细胞后,透射电子显微镜(TEM)和免疫荧光(IF)显示自噬泡和微管相关蛋白1轻链3(LC3)有显著的时间依赖性增加。一致地,蛋白质免疫印迹分析显示LC3II/LC3I比值显著增加,其中T1AM和SG-1是最有效的药物。在用T1AM和SG-1处理后,还观察到p62蛋白水平降低,这证实了这些化合物作为U-87MG细胞自噬诱导剂的有效性。在剖析哪种途径诱导自噬相关基因(ATG)的过程中,评估了这些化合物对磷脂酰肌醇-3-激酶-蛋白激酶B-哺乳动物雷帕霉素靶蛋白(PI3K-AKT-mTOR)途径的影响。我们发现,1μM T1AM、SG-1和SG-2在处理后0.5小时和4小时降低了磷酸化蛋白激酶B(pAKT)/蛋白激酶B(AKT)的比值,表明自噬是通过PI3K-AKT-mTOR途径抑制mTOR磷酸化来诱导的。总之,我们的研究表明,T1AM和甲状腺原氨酸样衍生物SG-1和SG-2可能是治疗神经系统疾病的有价值的工具。
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