UK Dementia Research Institute at University College London, UCL Queen Square Institute of Neurology, University College London, London, UK.
Dementia Research Centre, Department of Neurodegenerative Disease, UCL Queen Square Institute of Neurology, University College London, London, WC1N 3BG, UK.
J Neuroinflammation. 2021 Oct 3;18(1):224. doi: 10.1186/s12974-021-02247-3.
The primary progressive aphasias (PPA) represent a group of usually sporadic neurodegenerative disorders with three main variants: the nonfluent or agrammatic variant (nfvPPA), the semantic variant (svPPA), and the logopenic variant (lvPPA). They are usually associated with a specific underlying pathology: nfvPPA with a primary tauopathy, svPPA with a TDP-43 proteinopathy, and lvPPA with underlying Alzheimer's disease (AD). Little is known about their cause or pathophysiology, but prior studies in both AD and svPPA have suggested a role for neuroinflammation. In this study, we set out to investigate the role of chemokines across the PPA spectrum, with a primary focus on central changes in cerebrospinal fluid (CSF) METHODS: Thirty-six participants with sporadic PPA (11 svPPA, 13 nfvPPA, and 12 lvPPA) as well as 19 healthy controls were recruited to the study and donated CSF and plasma samples. All patients with lvPPA had a tau/Aβ42 biomarker profile consistent with AD, whilst this was normal in the other PPA groups and controls. We assessed twenty chemokines in CSF and plasma using Proximity Extension Assay technology: CCL2 (MCP-1), CCL3 (MIP-1a), CCL4 (MIP-1β), CCL7 (MCP-3), CCL8 (MCP-2), CCL11 (eotaxin), CCL13 (MCP-4), CCL19, CCL20, CCL23, CCL25, CCL28, CX3CL1 (fractalkine), CXCL1, CXCL5, CXCL6, CXCL8 (IL-8), CXCL9, CXCL10, and CXCL11.
In CSF, CCL19 and CXCL6 were decreased in both svPPA and nfvPPA compared with controls whilst CXCL5 was decreased in the nfvPPA group with a borderline significant decrease in the svPPA group. In contrast, CCL2, CCL3 and CX3CL1 were increased in lvPPA compared with controls and nfvPPA (and greater than svPPA for CX3CL1). CXCL1 was also increased in lvPPA compared with nfvPPA but not the other groups. CX3CL1 was significantly correlated with CSF total tau concentrations in the controls and each of the PPA groups. Fewer significant differences were seen between groups in plasma, although in general, results were in the opposite direction to CSF, i.e. decreased in lvPPA compared with controls (CCL3 and CCL19), and increased in svPPA (CCL8) and nfvPPA (CCL13).
Differential alteration of chemokines across the PPA variants is seen in both CSF and plasma. Importantly, these results suggest a role for neuroinflammation in these poorly understood sporadic disorders, and therefore also a potential future therapeutic target.
原发性进行性失语症(PPA)代表一组通常为散发性神经退行性疾病,有三个主要变体:非流利或语法障碍变体(nfvPPA)、语义变体(svPPA)和失读症变体(lvPPA)。它们通常与特定的潜在病理学有关:nfvPPA 与原发性 tau 病理学有关,svPPA 与 TDP-43 蛋白病有关,lvPPA 与潜在的阿尔茨海默病(AD)有关。关于它们的病因或病理生理学知之甚少,但在 AD 和 svPPA 中的先前研究表明神经炎症起作用。在这项研究中,我们着手研究 PPA 谱中趋化因子的作用,主要关注脑脊液(CSF)中的中枢变化。
36 名患有散发性 PPA(11 名 svPPA、13 名 nfvPPA 和 12 名 lvPPA)的参与者以及 19 名健康对照者被招募到该研究中,并捐献了 CSF 和血浆样本。所有 lvPPA 患者的 tau/Aβ42 生物标志物谱与 AD 一致,而其他 PPA 组和对照组则正常。我们使用邻近延伸测定法(Proximity Extension Assay)技术评估 CSF 和血浆中的 20 种趋化因子:CCL2(MCP-1)、CCL3(MIP-1a)、CCL4(MIP-1β)、CCL7(MCP-3)、CCL8(MCP-2)、CCL11(eotaxin)、CCL13(MCP-4)、CCL19、CCL20、CCL23、CCL25、CCL28、CX3CL1( fractalkine)、CXCL1、CXCL5、CXCL6、CXCL8(IL-8)、CXCL9、CXCL10 和 CXCL11。
在 CSF 中,与对照组相比,svPPA 和 nfvPPA 中的 CCL19 和 CXCL6 降低,而 nfvPPA 中的 CXCL5 降低,svPPA 组有边缘显著降低。相比之下,与对照组和 nfvPPA 相比,lvPPA 中的 CCL2、CCL3 和 CX3CL1 增加(而 CX3CL1 与 svPPA 相比增加)。与 nfvPPA 相比,lvPPA 中的 CXCL1 也增加,但与其他组相比没有增加。CX3CL1 与对照组和各 PPA 组的 CSF 总 tau 浓度显著相关。与 CSF 相比,组间差异较小,尽管一般来说,结果与 CSF 相反,即与对照组相比,lvPPA 中 CCL3 和 CCL19 降低(与 svPPA 相比,CCL8 增加),svPPA 和 nfvPPA 中 CCL13 增加。
在 PPA 变体中,趋化因子的差异改变同时出现在 CSF 和血浆中。重要的是,这些结果表明神经炎症在这些理解甚少的散发性疾病中起作用,因此也是潜在的未来治疗靶点。
Zotero 插件