Sierra Jaye, U. Sandau, Trevor J. McFarland, Randy L. Woltjer, J. Saugstad
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Thus, we used immunoblots to evaluate human post-mortem AD and control (CTL) frontal cortex (FC; AD n = 22, CTL n = 23) and hippocampus (HP; AD n = 34, CTL n = 22) for changes in Intersectin 1 (ITSN1), Phosphatidylinositol Binding Clathrin Assembly Protein gene (PICALM), Clathrin Light Chain (CLT), FCH and Mu Domain Containing Endocytic Adaptor 1 (FCHO1), Adaptor Related Protein Complex 2 (AP2) Subunit Alpha 1 (AP2A1), and Dynamin 2 (DNM2). Of these, we found that in AD, ITSN1-long (ITSN1-L) was decreased in the FC of males and HP of females, while ITSN1-short was increased in the HP of both males and females. We further evaluated ITSN1-L levels in cortex (CTX) and HP of the 5xFAD mouse model of Aβ pathology at different timepoints during aging and disease progression by immunoblot (n = 5–8 per group). At 3 months, female 5xFAD exhibited an increase of ITSN1-L in CTX but a decrease at 6 and 9 months. Additionally, immunofluorescent staining of 5xFAD primary HP neurons showed an increase of ITSN1-L in matured 5xFAD neurons at 21 and 28 days in vitro. Together, our studies show that in AD, isoforms of ITSN1 change in a brain region-and sex-dependent manner. Further, changes in ITSN1-L are transient with levels increasing during early Aβ accumulation and decreasing during later progression. 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We previously identified a set of candidate AD microRNAs (miRNAs) in human cerebrospinal fluid (CSF) and used a target prediction pipeline to identify mRNAs and pathways that could potentially be regulated by the miRNAs. Of these pathways, clathrin mediated endocytosis (CME) was selected for further investigation. CME is altered in multiple brain cell types in AD and is implicated in early cellular phenotypes such as enlarged early endosomes and pathogenic processing of Aβ. However, a comprehensive evaluation of major CME hub proteins in humans with AD across multiple brain regions is lacking. Thus, we used immunoblots to evaluate human post-mortem AD and control (CTL) frontal cortex (FC; AD n = 22, CTL n = 23) and hippocampus (HP; AD n = 34, CTL n = 22) for changes in Intersectin 1 (ITSN1), Phosphatidylinositol Binding Clathrin Assembly Protein gene (PICALM), Clathrin Light Chain (CLT), FCH and Mu Domain Containing Endocytic Adaptor 1 (FCHO1), Adaptor Related Protein Complex 2 (AP2) Subunit Alpha 1 (AP2A1), and Dynamin 2 (DNM2). Of these, we found that in AD, ITSN1-long (ITSN1-L) was decreased in the FC of males and HP of females, while ITSN1-short was increased in the HP of both males and females. We further evaluated ITSN1-L levels in cortex (CTX) and HP of the 5xFAD mouse model of Aβ pathology at different timepoints during aging and disease progression by immunoblot (n = 5–8 per group). At 3 months, female 5xFAD exhibited an increase of ITSN1-L in CTX but a decrease at 6 and 9 months. 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引用次数: 0
摘要
阿尔茨海默病(AD)是最常见的痴呆症,其特征是大脑中淀粉样β(Aβ)斑块和神经纤维Tau缠结的积累。我们先前在人类脑脊液(CSF)中发现了一组候选的AD microRNA(miRNA),并利用目标预测管道确定了可能受miRNA调控的mRNA和通路。在这些通路中,选择了凝集素介导的内吞(CME)进行进一步研究。CME在AD患者的多种脑细胞类型中发生改变,并与早期细胞表型有关,如早期内体增大和Aβ的致病处理。然而,目前还缺乏对AD患者多个脑区主要CME中枢蛋白的全面评估。因此,我们使用免疫印迹法评估了人类死后AD和对照组(CTL)的额叶皮层(FC;AD n = 22,CTL n = 23)和海马(HP;AD n = 34,CTL n = 22)中交联蛋白 1 (ITSN1)、磷脂酰肌醇结合鞘磷脂组装蛋白基因 (PICALM)、鞘磷脂轻链 (CLT)、FCH 和 Mu 域包含内吞适配体 1 (FCHO1)、适配体相关蛋白复合物 2 (AP2) 亚基 Alpha 1 (AP2A1) 和 Dynamin 2 (DNM2) 的变化。其中,我们发现在 AD 中,男性 FC 和女性 HP 中的 ITSN1-长(ITSN1-L)减少,而男性和女性 HP 中的 ITSN1-短增加。我们通过免疫印迹进一步评估了5xFAD小鼠Aβ病理模型在衰老和疾病进展过程中不同时间点皮层(CTX)和HP中的ITSN1-L水平(n = 5-8/组)。3 个月时,雌性 5xFAD CTX 中的 ITSN1-L 有所增加,但在 6 个月和 9 个月时有所减少。此外,对 5xFAD 初级 HP 神经元的免疫荧光染色显示,在体外 21 天和 28 天时,成熟的 5xFAD 神经元中的 ITSN1-L 有所增加。总之,我们的研究表明,在 AD 中,ITSN1 的同工型以脑区和性别依赖的方式发生变化。此外,ITSN1-L的变化是短暂的,其水平在早期Aβ积累时升高,而在后期发展时降低。这些研究结果表明,ITSN1的表达以及由此产生的CME活性可能会随着疾病的进展阶段而发生变化。
A clathrin mediated endocytosis scaffolding protein, Intersectin 1, changes in an isoform, brain region, and sex specific manner in Alzheimer’s disease
Alzheimer’s disease (AD) is the most common form of dementia and is characterized by the accumulation of amyloid-beta (Aβ) plaques and neurofibrillary Tau tangles in the brain. We previously identified a set of candidate AD microRNAs (miRNAs) in human cerebrospinal fluid (CSF) and used a target prediction pipeline to identify mRNAs and pathways that could potentially be regulated by the miRNAs. Of these pathways, clathrin mediated endocytosis (CME) was selected for further investigation. CME is altered in multiple brain cell types in AD and is implicated in early cellular phenotypes such as enlarged early endosomes and pathogenic processing of Aβ. However, a comprehensive evaluation of major CME hub proteins in humans with AD across multiple brain regions is lacking. Thus, we used immunoblots to evaluate human post-mortem AD and control (CTL) frontal cortex (FC; AD n = 22, CTL n = 23) and hippocampus (HP; AD n = 34, CTL n = 22) for changes in Intersectin 1 (ITSN1), Phosphatidylinositol Binding Clathrin Assembly Protein gene (PICALM), Clathrin Light Chain (CLT), FCH and Mu Domain Containing Endocytic Adaptor 1 (FCHO1), Adaptor Related Protein Complex 2 (AP2) Subunit Alpha 1 (AP2A1), and Dynamin 2 (DNM2). Of these, we found that in AD, ITSN1-long (ITSN1-L) was decreased in the FC of males and HP of females, while ITSN1-short was increased in the HP of both males and females. We further evaluated ITSN1-L levels in cortex (CTX) and HP of the 5xFAD mouse model of Aβ pathology at different timepoints during aging and disease progression by immunoblot (n = 5–8 per group). At 3 months, female 5xFAD exhibited an increase of ITSN1-L in CTX but a decrease at 6 and 9 months. Additionally, immunofluorescent staining of 5xFAD primary HP neurons showed an increase of ITSN1-L in matured 5xFAD neurons at 21 and 28 days in vitro. Together, our studies show that in AD, isoforms of ITSN1 change in a brain region-and sex-dependent manner. Further, changes in ITSN1-L are transient with levels increasing during early Aβ accumulation and decreasing during later progression. These findings suggest that ITSN1 expression, and consequently CME activity, may change depending on the stage of disease progression.
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