Stocks Jane, Behn Jordan, Barbieri Elena, Mesulam M-Marsel
Department of Psychiatry and Behavioral Sciences, Feinberg School of Medicine, Northwestern University, Chicago, IL, USA 60611.
Mesulam Center for Cognitive Neurology and Alzheimer's Disease, Feinberg School of Medicine, Northwestern University, Chicago IL, USA 60611.
Imaging Neurosci (Camb). 2025;3. doi: 10.1162/imag.a.83. Epub 2025 Jul 16.
The delineation of disease progression in neurodegenerative entities offers neurobiological insights into pathophysiology as well as practical information on natural progression that can be used to gauge the benefits of treatment. In AD, FTLD-tau and FTLD-TDP types A and B such advances have been achieved based on the investigation of presymptomatic mutation carriers. In the absence of dominant mutations, this approach is not feasible in FTLD-TDP type C (TDP-C). Considering the subtlety of the initial symptoms, it is almost certain that the disease had been progressing for years before the first investigations are obtained. We addressed this limitation through an indirect approach based on the fact that neurodegeneration in TDP-C can be asymmetric for 5-6 years after symptom onset. In time, the contralateral hemisphere starts to show the onset of atrophy, the spread of which mirrors the pattern in the affected hemisphere. The unaffected hemisphere therefore offers an opportunity for capturing the very first emergence of atrophy. To that end, we traced the onset and progression of neurodegeneration in TDP-C by analyzing the right hemisphere longitudinally in cases of asymmetric left anterior temporal atrophy. In these cases, TDP-C was either confirmed at autopsy or suspected based on the clinical features and anatomy of atrophy. Structural MRIs were processed using voxel-based morphometry and parcellated into cortical and subcortical regions. W-scores were computed to identify volume loss relative to age-matched controls. Linear mixed-effects models assessed disease progression across regions of interest (ROIs). Results of our analyses reveal that atrophy in TDP-C follows a stereotyped progression within the right hemisphere, beginning in the ventromedial anterior temporal lobe and extending posteriorly and laterally over time. Early atrophy was most prominent in the medial temporal pole (planum polare), perirhinal cortex, entorhinal cortex, and anterior fusiform cortex, with subcortical involvement initially limited to the amygdala. Voxelwise and ROI-based analyses confirmed that cortical atrophy preceded and exceeded amygdala atrophy in most cases, suggesting greater neocortical vulnerability. Longitudinal linear mixed-effects models identified the greatest volume loss in medial temporal ROIs and the amygdala, following a consistent anterior-to-posterior gradient over time. These findings reconstruct the spatial and temporal progression of TDP-C pathology using the initially unaffected hemisphere as a proxy for early disease stages. The stereotyped trajectory of atrophy aligns with neuropathological patterns and offers critical insights into disease progression, aiding therapeutic evaluation.
神经退行性疾病实体中疾病进展的描绘,为病理生理学提供了神经生物学见解,以及关于自然进展的实用信息,可用于评估治疗效果。在阿尔茨海默病(AD)、额颞叶痴呆- tau型(FTLD-tau)以及A型和B型额颞叶痴呆-TDP型(FTLD-TDP)中,基于对症状前突变携带者的研究已取得了这样的进展。在没有显性突变的情况下,这种方法在C型额颞叶痴呆-TDP型(TDP-C)中不可行。考虑到初始症状的细微性,几乎可以肯定的是,在首次进行检查之前,疾病已经进展了数年。我们通过一种间接方法解决了这一局限性,该方法基于这样一个事实,即TDP-C中的神经退行性变在症状出现后的5 - 6年内可能是不对称的。随着时间的推移,对侧半球开始出现萎缩,其蔓延模式与受影响半球的模式相似。因此,未受影响的半球为捕捉萎缩的最初出现提供了机会。为此,我们通过纵向分析不对称性左前颞叶萎缩病例的右半球,追踪了TDP-C中神经退行性变的发生和进展。在这些病例中,TDP-C要么在尸检时得到证实,要么根据临床特征和萎缩的解剖结构被怀疑。使用基于体素的形态测量法对结构磁共振成像(MRI)进行处理,并将其分割为皮质和皮质下区域。计算W分数以确定相对于年龄匹配对照组的体积损失。线性混合效应模型评估了感兴趣区域(ROI)的疾病进展。我们的分析结果表明,TDP-C中的萎缩在右半球内遵循一种刻板的进展模式,始于腹内侧前颞叶,并随着时间向后和向外扩展。早期萎缩在颞极内侧(极平面)、嗅周皮质、内嗅皮质和前梭状回最为明显,皮质下受累最初仅限于杏仁核。基于体素和基于ROI的分析证实,在大多数情况下,皮质萎缩先于并超过杏仁核萎缩,表明新皮质更易受损。纵向线性混合效应模型确定颞叶内侧ROI和杏仁核的体积损失最大,且随着时间推移呈现出一致的从前到后的梯度。这些发现利用最初未受影响的半球作为疾病早期阶段的替代物,重建了TDP-C病理的空间和时间进展。萎缩的刻板轨迹与神经病理学模式一致,并为疾病进展提供了关键见解,有助于治疗评估。
