阿尔茨海默病早期 Aβ 沉积与区域突触密度的相关性:一项使用 [C]UCB-J 的 PET 成像研究。
Association of Aβ deposition and regional synaptic density in early Alzheimer's disease: a PET imaging study with [C]UCB-J.
机构信息
Alzheimer's Disease Research Unit, Yale University School of Medicine, One Church Street, 8th Floor, New Haven, CT, 06510, USA.
Department of Psychiatry, Yale University School of Medicine, 300 George Street, New Haven, CT, 06510, USA.
出版信息
Alzheimers Res Ther. 2021 Jan 5;13(1):11. doi: 10.1186/s13195-020-00742-y.
BACKGROUND
Attempts to associate amyloid-β (Aβ) pathogenesis with synaptic loss in Alzheimer's disease (AD) have thus far been limited to small numbers of postmortem studies. Aβ plaque burden is not well-correlated with indices of clinical severity or neurodegeneration-at least in the dementia stage-as deposition of Aβ reaches a ceiling. In this study, we examined in vivo the association between fibrillar Aβ deposition and synaptic density in early AD using positron emission tomography (PET). We hypothesized that global Aβ deposition would be more strongly inversely associated with hippocampal synaptic density in participants with amnestic mild cognitive impairment (aMCI; a stage of continued Aβ accumulation) compared to those with dementia (a stage of relative Aβ plateau).
METHODS
We measured SV2A binding ([C]UCB-J) and Aβ deposition ([C]PiB) in 14 participants with aMCI due to AD and 24 participants with mild AD dementia. Distribution volume ratios (DVR) with a cerebellar reference region were calculated for both tracers to investigate the association between global Aβ deposition and SV2A binding in hippocampus. Exploratory analyses examined correlations between both global and regional Aβ deposition and SV2A binding across a broad range of brain regions using both ROI- and surface-based approaches.
RESULTS
We observed a significant inverse association between global Aβ deposition and hippocampal SV2A binding in participants with aMCI (r = - 0.55, P = 0.04), but not mild dementia (r = 0.05, P = 0.82; difference statistically significant by Fisher z = - 1.80, P = 0.04). Exploratory analyses across other ROIs and whole brain analyses demonstrated no broad or consistent associations between global Aβ deposition and regional SV2A binding in either diagnostic group. ROI-based analyses of the association between regional Aβ deposition and SV2A binding also revealed no consistent pattern but suggested a "paradoxical" positive association between local Aβ deposition and SV2A binding in the hippocampus.
CONCLUSIONS
Our findings lend support to a model in which fibrillar Aβ is still accumulating in the early stages of clinical disease but approaching a relative plateau, a point at which Aβ may uncouple from neurodegenerative processes including synaptic loss. Future research should investigate the relationship between Aβ deposition and synaptic loss in larger cohorts beginning preclinically and followed longitudinally in conjunction with other biomarkers.
背景
目前,尝试将淀粉样蛋白-β(Aβ)发病机制与阿尔茨海默病(AD)中的突触丢失联系起来的研究,仅限于少数尸检研究。淀粉样斑块负担与临床严重程度或神经退行性变的指标相关性较差-至少在痴呆阶段,因为 Aβ的沉积达到了一个上限。在这项研究中,我们使用正电子发射断层扫描(PET)检查了早期 AD 中纤维状 Aβ沉积与突触密度之间的体内关联。我们假设,与痴呆(Aβ相对平台阶段)参与者相比,在有遗忘性轻度认知障碍(aMCI;持续 Aβ积累阶段)的参与者中,全局 Aβ沉积与海马突触密度的负相关性更强。
方法
我们测量了 14 名 AD 所致 aMCI 患者和 24 名轻度 AD 痴呆患者的 SV2A 结合物([C]UCB-J)和 Aβ沉积([C]PiB)。使用小脑参考区域计算了两种示踪剂的分布容积比(DVR),以研究全局 Aβ沉积与海马 SV2A 结合之间的关系。通过 ROI 和表面方法,对广泛的脑区进行了全局和局部 Aβ沉积与 SV2A 结合之间的相关性分析。
结果
我们观察到,在 aMCI 患者中,全局 Aβ沉积与海马 SV2A 结合之间存在显著的负相关(r=-0.55,P=0.04),但在轻度痴呆患者中则没有(r=0.05,P=0.82;Fisher z 差异有统计学意义,z=-1.80,P=0.04)。在其他 ROI 和全脑分析中,在两个诊断组中,均未发现全局 Aβ沉积与局部 SV2A 结合之间存在广泛或一致的相关性。基于 ROI 的分析也揭示了局部 Aβ沉积与 SV2A 结合之间没有一致的模式,但提示在海马区局部 Aβ沉积与 SV2A 结合之间存在“矛盾”的正相关。
结论
我们的研究结果支持这样一种模型,即在临床疾病的早期阶段,纤维状 Aβ仍在积累,但已接近相对平台期,此时 Aβ可能与包括突触丢失在内的神经退行性过程脱耦。未来的研究应在更大的队列中,在临床前期开始并进行纵向随访,同时结合其他生物标志物,调查 Aβ沉积与突触丢失之间的关系。
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