载脂蛋白E4上调糖原合成酶激酶-3β以加重2型糖尿病小鼠的阿尔茨海默病样病理改变和认知障碍。
ApoE4 Upregulates GSK-3β to Aggravate Alzheimer-Like Pathologies and Cognitive Impairment in Type 2 Diabetic Mice.
作者信息
Wang Yuying, Gao Yang, Wang Yarong, Zhang Fuqiang, Sun Fei, Wang Xin, Xie Jiazhao, Xu Zhipeng, Zhang Junjian, Xu Haibo, Zhang Yao, Wang Jian-Zhi
机构信息
Key Laboratory of Ministry of Education for Neurological Disorders, Department of Pathophysiology, School of Basic Medicine, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, China.
Department of Neurology, Zhongnan Hospital of Wuhan University, Wuhan University, Wuhan, China.
出版信息
CNS Neurosci Ther. 2025 Sep;31(9):e70575. doi: 10.1111/cns.70575.
BACKGROUND
The apolipoprotein E (ApoE) ε4 allele and type 2 diabetes mellitus (T2DM) are independent risk factors for Alzheimer's disease (AD), the most prevalent neurodegenerative disorder in the elderly. The T2DM patients carrying the ApoE ε4 allele exhibit heightened activation of platelet glycogen synthase kinase-3β (GSK-3β), a key downstream kinase in the insulin signaling pathway, along with more severe cognitive deficits. This observation suggests an intrinsic link between ApoE ε4, GSK-3β, and cognitive dysfunction. However, the precise mechanisms by which ApoE ε4 influences GSK-3β activity and exacerbates brain pathology and cognitive decline in T2DM patients remain poorly understood.
METHODS
To investigate these mechanisms, we developed T2DM mouse models by generating humanized ApoE ε3/ε3 and ε4/ε4 knock-in mice. The mice were subjected to a high-fat diet combined with multiple low-dose intraperitoneal streptozotocin injections to induce T2DM. We then assessed GSK-3β expression, AD-like pathologies, and cognitive functions in these models.
RESULTS
We observed that GSK-3β activity was significantly upregulated in ApoE4 mice, accompanied by disruption of the insulin signaling pathway. Notably, ApoE4-T2DM mice exhibited exacerbated AD-related pathologies, including increased accumulation of hyperphosphorylated tau, neuroinflammation, and synaptic loss. These changes were correlated with more severe cognitive impairments compared with ApoE3-T2DM or ApoE4 mice. Furthermore, inhibition of GSK-3β activity using the selective inhibitor 9-ING-41 effectively ameliorated both AD-like pathologies and cognitive deficits in ApoE4-T2DM mice.
CONCLUSIONS
Our findings suggest that ApoE4 exacerbates AD pathogenesis by activating GSK-3β. Furthermore, targeting GSK-3β may offer a promising therapeutic strategy to halt the progression from T2DM to AD, providing new insights into potential interventions for patients at risk.
背景
载脂蛋白E(ApoE)ε4等位基因和2型糖尿病(T2DM)是阿尔茨海默病(AD)的独立危险因素,AD是老年人中最常见的神经退行性疾病。携带ApoE ε4等位基因的T2DM患者表现出血小板糖原合酶激酶-3β(GSK-3β)的激活增强,GSK-3β是胰岛素信号通路中的关键下游激酶,同时伴有更严重的认知缺陷。这一观察结果表明ApoE ε4、GSK-3β和认知功能障碍之间存在内在联系。然而,ApoE ε4影响GSK-3β活性并加剧T2DM患者脑病理和认知衰退的确切机制仍知之甚少。
方法
为了研究这些机制,我们通过构建人源化ApoE ε3/ε3和ε4/ε4基因敲入小鼠建立了T2DM小鼠模型。对小鼠进行高脂饮食并多次低剂量腹腔注射链脲佐菌素以诱导T2DM。然后我们评估了这些模型中GSK-3β的表达、AD样病理变化和认知功能。
结果
我们观察到ApoE4小鼠中GSK-3β活性显著上调,同时胰岛素信号通路受到破坏。值得注意的是,ApoE4-T2DM小鼠表现出AD相关病理变化加剧,包括过度磷酸化tau蛋白的积累增加、神经炎症和突触丧失。与ApoE3-T2DM或ApoE4小鼠相比,这些变化与更严重的认知障碍相关。此外,使用选择性抑制剂9-ING-41抑制GSK-3β活性可有效改善ApoE4-T2DM小鼠的AD样病理变化和认知缺陷。
结论
我们的研究结果表明,ApoE4通过激活GSK-3β加剧AD发病机制。此外,靶向GSK-3β可能为阻止从T2DM进展到AD提供一种有前景的治疗策略,为有风险的患者提供潜在干预措施的新见解。
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