Experimental Neuropsychophysiology Lab, Santa Lucia Foundation, IRCCS, Rome, Italy.
UOSD Centro Demenze, Policlinico Tor Vergata, Rome, Italy.
J Alzheimers Dis. 2022;86(2):773-778. doi: 10.3233/JAD-215218.
Long-term potentiation (LTP) like-cortical plasticity impairment and cholinergic neurotransmission deficits have been widely demonstrated in Alzheimer's disease (AD) patients.
In this study we aim to investigate the neurophysiological features underlying cognitive decline in AD patients according to the National Institute on Aging-Alzheimer's Association (NIA-AA) classification and APOE genotype.
65 newly diagnosed AD patients were enrolled. APOE genotype and lumbar puncture for the analysis of cerebrospinal fluid biomarkers were performed for diagnostic purposes. Patients were subdivided upon NIA-AA criteria, according to the presence of biomarkers of amyloid-β (Aβ) deposition (A) and fibrillar tau (T), in four groups: A+/T-E4 (n = 9), A+/T-E3 (n = 18), A+/T+ E4 (n = 21), and A+/T+ E3 (n = 17). We applied intermittent theta burst stimulation protocol over the primary motor cortex to assess LTP-like cortical plasticity and short latency afferent inhibition (SAI) protocol to investigate central cholinergic activity. Patients were followed over 24 months. Cognitive decline was evaluated considering changes in Mini-Mental State Examination (MMSE) scores respect to the baseline.
A+/T-E4 patients showed preserved LTP-like cortical plasticity as compared to A+/T-E3 and to A+/T+ patients independently from genotype (p < 0.001). In addition, A+/T-E4 patients showed a slower cognitive decline with respect to A+/T+ E4 (delta MMSE -0.5±2.12 versus -6.05±4.95; post-hocp = 0.004) and to A+/T+ E3 patients (-4.12±4.14; post-hoc p = 0.028). No differences were found for SAI protocol (p > 0.05).
Our results suggest that APOE4 in patients with isolated Aβ pathology could exert positive effects on LTP-like cortical plasticity with a consequent slower cognitive decline.
长时程增强(LTP)样皮质可塑性损伤和胆碱能神经递质传递缺陷已在阿尔茨海默病(AD)患者中广泛证实。
本研究旨在根据美国国家老龄化研究所-阿尔茨海默病协会(NIA-AA)分类和 APOE 基因型,研究 AD 患者认知能力下降的神经生理特征。
共纳入 65 例新诊断的 AD 患者。进行 APOE 基因型和腰椎穿刺以分析脑脊液生物标志物,以进行诊断。根据 Aβ 沉积(A)和纤维状 tau(T)生物标志物的存在,根据 NIA-AA 标准将患者分为四组:A+/T-E4(n=9)、A+/T-E3(n=18)、A+/T+E4(n=21)和 A+/T+E3(n=17)。我们应用间歇性 theta 爆发刺激方案刺激初级运动皮层,以评估 LTP 样皮质可塑性和短潜伏期传入抑制(SAI)方案,以研究中枢胆碱能活性。患者随访 24 个月。考虑到与基线相比,Mini-Mental State Examination(MMSE)评分的变化,评估认知能力下降。
与 A+/T-E3 和 A+/T+患者相比,A+/T-E4 患者表现出保留的 LTP 样皮质可塑性,而与基因型无关(p<0.001)。此外,与 A+/T+ E4 患者(delta MMSE-0.5±2.12 与-6.05±4.95;post-hoc p=0.004)和 A+/T+ E3 患者(-4.12±4.14;post-hoc p=0.028)相比,A+/T-E4 患者的认知衰退速度较慢。在 SAI 方案中未发现差异(p>0.05)。
我们的结果表明,在仅有 Aβ 病理的患者中,APOE4 可能对 LTP 样皮质可塑性产生积极影响,从而导致认知衰退速度较慢。
