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体内 tau 与早老素 1 变异型 Met146Leu 相关神经退行性变的影像学研究

In Vivo Tau and Neurodegeneration Imaging in a Family With the Presenilin 1 Met146Leu Pathogenic Variant.

机构信息

From the Laboratory of Neuroimaging and Innovative Molecular Tracers (NIMTlab) (C.B.), Geneva University Neurocenter and Faculty of Medicine, University of Geneva, Switzerland; Center for Mind/Brain Sciences (A.D.), CIMeC, University of Trento, Italy; Division of Radiology (M.S.), Geneva University Hospitals, Switzerland; Department of Primary Care (V.L., A.C.B., R.C.), Regional Neurogenetic Centre, ASP Catanzaro, Lamezia Terme; Institute of Neurology (E.F.), Department of Medical and Surgical Sciences, Magna Graecia University, Catanzaro, Italy; Geneva Memory Center (G.B.F.), Geneva University Hospitals, Switzerland; Nuclear Medicine Unit (D.P.), San Raffaele Hospital, Milan; Vita-Salute San Raffaele University (D.P.), Milan, Italy; and Division of Nuclear Medicine and Molecular Imaging (V.G.), Geneva University Hospitals, Switzerland.

出版信息

Neurology. 2024 Dec 24;103(12):e210103. doi: 10.1212/WNL.0000000000210103. Epub 2024 Nov 25.

Abstract

OBJECTIVES

We investigated tau and neurodegeneration patterns and clinical phenotypes in carriers of a specific pathogenic variant in the PSEN1 gene and 1 nonaffected relative.

METHODS

We included 3 symptomatic carriers of the c.436 A>C, p.Met146Leu, NM_000021.4, rs63750306 variant in the PSEN1 gene, pathogenic for autosomal dominant Alzheimer disease (AD), 1 asymptomatic carrier of the same variant, and 1 noncarrier, all belonging to the same "N" family. All subjects underwent clinical evaluations, F-flortaucipir-PET, and MRI. F-fludeoxyglucose-PET was available for 3 cases.

RESULTS

All symptomatic carriers showed advanced AD tau patterns. Symptomatic female carriers presented an earlier age at onset and more pronounced tau pathology in temporoparietal and frontal regions than male carriers, at comparable disease severity and duration. The presymptomatic male carrier showed a negative tau scan 4 years before symptom onset. MRI showed no severe cortical and hippocampal atrophy in all individuals. Brain metabolism showed neurodegeneration patterns typical of AD in symptomatic carriers.

DISCUSSION

In PSEN1 Met146Leu variant carriers, high cortical tau load, without significant atrophy, was present during early memory deficits. In the asymptomatic phase, all biomarkers were negative. More pronounced tau pathology in female than male individuals highlights the need to investigate sex differences in autosomal dominant AD.

摘要

目的

我们研究了载有特定 PSEN1 基因致病性变异体的个体以及 1 名无相关个体中的 tau 和神经退行性变模式及临床表型。

方法

我们纳入了 3 名载有 PSEN1 基因 c.436 A>C,p.Met146Leu,NM_000021.4,rs63750306 变异体的有症状携带者,该变异体致病性为常染色体显性阿尔茨海默病(AD),1 名无症状携带者和 1 名非携带者,均属于同一个“N”家族。所有受试者均接受了临床评估、F-氟脱氧葡萄糖-PET 和 MRI 检查。3 例受试者可进行 F-氟托西匹啶-PET 检查。

结果

所有有症状携带者均表现出严重的 AD tau 模式。有症状的女性携带者在颞顶和额区的 tau 病理比男性携带者更早出现,且更为显著,尽管疾病严重程度和持续时间相当。在症状出现前 4 年,处于无症状期的男性携带者的 tau 扫描结果为阴性。MRI 显示所有个体均无严重的皮质和海马萎缩。脑代谢显示出与 AD 典型的神经退行性变模式。

讨论

在 PSEN1 Met146Leu 变异携带者中,在早期记忆障碍时即存在高皮质 tau 负荷,但无明显萎缩。在无症状期,所有生物标志物均为阴性。女性个体比男性个体的 tau 病理更为显著,这突显了需要研究常染色体显性 AD 中的性别差异。

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