Departments of Pharmacology and Experimental Therapeutics, Boston University School of Medicine, Boston, MA, USA.
Department of Cell Pharmacology, Graduate School of Medicine, Nagoya University School of Medicine, Aichi, Japan.
Acta Neuropathol Commun. 2020 Feb 4;8(1):12. doi: 10.1186/s40478-020-0890-4.
The accumulation of phosphorylated tau protein (pTau) in the entorhinal cortex (EC) is the earliest tau pathology in Alzheimer's disease (AD). Tau tubulin kinase-1 (TTBK1) is a neuron-specific tau kinase and expressed in the EC and hippocampal regions in both human and mouse brains. Here we report that collapsin response mediator protein-2 (CRMP2), a critical mediator of growth cone collapse, is a new downstream target of TTBK1 and is accumulated in the EC region of early stage AD brains. TTBK1 transgenic mice show severe axonal degeneration in the perforant path, which is exacerbated by crossing with Tg2576 mice expressing Swedish familial AD mutant of amyloid precursor protein (APP). TTBK1 mice show accumulation of phosphorylated CRMP2 (pCRMP2), in the EC at 10 months of age, whereas age-matched APP/TTBK1 bigenic mice show pCRMP2 accumulation in both the EC and hippocampal regions. Amyloid-β peptide (Aβ) and TTBK1 suppress the kinetics of microtubule polymerization and TTBK1 reduces the neurite length of primary cultured neurons in Rho kinase-dependent manner in vitro. Silencing of TTBK1 or expression of dominant-negative Rho kinase demonstrates that Aβ induces CRMP2 phosphorylation at threonine 514 in a TTBK1-dependent manner, and TTBK1 enhances Aβ-induced CRMP2 phosphorylation in Rho kinase-dependent manner in vitro. Furthermore, TTBK1 expression induces pCRMP2 complex formation with pTau in vitro, which is enhanced upon Aβ stimulation in vitro. Finally, pCRMP2 forms a complex with pTau in the EC tissue of TTBK1 mice in vivo, which is exacerbated in both the EC and hippocampal tissues in APP/TTBK1 mice. These results suggest that TTBK1 and Aβ induce phosphorylation of CRMP2, which may be causative for the neurite degeneration and somal accumulation of pTau in the EC neurons, indicating critical involvement of TTBK1 and pCRMP2 in the early AD pathology.
磷酸化tau 蛋白 (pTau) 在海马旁回皮层 (EC) 的积累是阿尔茨海默病 (AD) 中最早的 tau 病理学。Tau 微管激酶-1 (TTBK1) 是一种神经元特异性 tau 激酶,在人和鼠脑的 EC 和海马区均有表达。在这里,我们报告说, collapsin 反应介质蛋白-2 (CRMP2),生长锥塌陷的关键介质,是 TTBK1 的一个新的下游靶标,并在早期 AD 大脑的 EC 区域积累。TTBK1 转基因小鼠在穿通纤维通路中表现出严重的轴突退化,而与表达淀粉样前体蛋白 (APP) 瑞典家族 AD 突变体的 Tg2576 小鼠杂交后,这种退化更为严重。TTBK1 小鼠在 10 个月大时,在 EC 中积累磷酸化的 CRMP2 (pCRMP2),而年龄匹配的 APP/TTBK1 双基因小鼠在 EC 和海马区均积累 pCRMP2。淀粉样β肽 (Aβ) 和 TTBK1 抑制微管聚合动力学,体外 TTBK1 以 Rho 激酶依赖性方式降低原代培养神经元的神经突长度。沉默 TTBK1 或表达显性负性 Rho 激酶表明,Aβ 以 TTBK1 依赖的方式诱导 CRMP2 丝氨酸 514 磷酸化,而 TTBK1 以 Rho 激酶依赖的方式增强 Aβ诱导的 CRMP2 磷酸化。此外,TTBK1 在体外与 pTau 形成 pCRMP2 复合物,体外 Aβ刺激后增强。最后,pCRMP2 在体内 TTBK1 小鼠的 EC 组织中与 pTau 形成复合物,在 APP/TTBK1 小鼠的 EC 和海马组织中加剧。这些结果表明,TTBK1 和 Aβ诱导 CRMP2 磷酸化,这可能是导致 EC 神经元中 pTau 的神经突退化和体部积累的原因,表明 TTBK1 和 pCRMP2 对 AD 早期病理学的关键作用。
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