在常见痴呆症和渐冻症中,前脑岛比后脑岛更容易受到 TDP-43 病理学的影响

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-04-09 DOI:10.1093/jnen/nlae027
Riley H Lochner, Anithachristy S Arumanayagam, Suzanne Z Powell, Joseph C Masdeu, Belen Pascual, Matthew D Cykowski
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引用次数: 0

摘要

基于前脑岛和杏仁核在解剖学上的邻近性、连接性和功能上的相似性,我们检验了前脑岛是晚期老年痴呆症患者TDP-43病理发展过程中的一个重要病灶这一假设。在对临床和神经病理学数据保密的情况下,我们对105名阿尔茨海默病、路易体病、LATE-NC和海马硬化症(HS)、肌萎缩侧索硬化症(ALS)及其他疾病的尸检患者的岛叶前后配对样本进行了磷酸化TDP(pTDP)包涵体病理学评估。34.3%的研究对象存在岛叶 pTDP 病变,最常见的是神经元包涵体和/或 II 层的短神经元,较少见的是类似杏仁核区域的皮下过程。在阳性样本中,pTDP病理变化仅限于岛叶前部(41.7%),或同时发生在岛叶前部和后部(58.3%);在所有疾病中,岛叶前部的包涵体密度更大(p &p;lt;.001)。46.7%的ALS样本出现pTDP病理变化,通常没有广泛的TDP-43蛋白病变。在晚期脊髓灰质炎中,30.4%的样本(主要是晚期脊髓灰质炎2期和3期)出现了pTDP病变,通常与基底前脑病变和合并HS同时出现,这表明这是这种病变向颞叶内侧以外发展的重要一步。
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Anterior insula is more vulnerable than posterior insula to TDP-43 pathology in common dementias and ALS
Based on the anatomic proximity, connectivity, and functional similarities between the anterior insula and amygdala, we tested the hypothesis that the anterior insula is an important focus in the progression of TDP-43 pathology in LATE-NC. Blinded to clinical and neuropathologic data, phospho-TDP (pTDP) inclusion pathology was assessed in paired anterior and posterior insula samples in 105 autopsied patients with Alzheimer disease, Lewy body disease, LATE-NC and hippocampal sclerosis (HS), amyotrophic lateral sclerosis (ALS), and other conditions. Insular pTDP pathology was present in 34.3% of the study cohort, most commonly as neuronal inclusions and/or short neurites in lamina II, and less commonly as subpial processes resembling those described in the amygdala region. Among positive samples, pTDP pathology was limited to the anterior insula (41.7%), or occurred in both anterior and posterior insula (58.3%); inclusion density was greater in anterior insula across all diseases (p < .001). pTDP pathology occurred in 46.7% of ALS samples, typically without a widespread TDP-43 proteinopathy. In LATE-NC, it was seen in 30.4% of samples (mostly LATE-NC stages 2 and 3), often co-occurring with basal forebrain pathology and comorbid HS, suggesting this is an important step in the evolution of this pathology beyond the medial temporal lobe.
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4.30%
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