脑脊液中的可溶性SorLA,一种用于探索阿尔茨海默病中SorLA蛋白转运受损的新型生物标志物。
Soluble SorLA in CSF, a novel biomarker to explore disrupted trafficking of SorLA protein in Alzheimer disease.
作者信息
Castelot Romain, Zarea Aline, Wallon David, Rovelet-Lecrux Anne, Schramm Catherine, Quillard-Muraine Muriel, Beaume Anne, Blanc Frédéric, Bousiges Olivier, Dumurgier Julien, Formaglio Maïté, Leguyader Gwenael, Lehmann Sylvain, Marelli Cecilia, Martinet Matthieu, Nogueira Leonor, Pariente Jérémie, Quadrio Isabelle, Rollin-Sillaire Adeline, Schraen Susanna, Nicolas Gaël, Lecourtois Magalie
机构信息
Univ Rouen Normandie, Inserm U1245 and CHU Rouen, Department of Genetics and CNRMAJ, Rouen, F-76000, France.
Department of Neurology and CNRMAJ, Univ Rouen Normandie, Inserm U1245 and CHU Rouen, Rouen, F-76000, France.
出版信息
Alzheimers Res Ther. 2025 May 7;17(1):100. doi: 10.1186/s13195-025-01748-0.
BACKGROUND
The SorLA protein, encoded by the Sortilin-related receptor 1 (SORL1) gene, is a major player in Alzheimer's disease (AD) pathophysiology. Functional studies demonstrated that SorLA deficiency results in increased production of Aβ peptide, and thus a higher risk of AD. SorLA can be subject to proteolytic shedding at the cell surface, leading to the release of the soluble ectodomain of the protein (sSorLA) in the extracellular space. Recently, we demonstrated that a large proportion (~25%) of rare SORL1 missense variants found in AD patients alter SorLA trafficking along the constitutive secretory pathway, resulting in reduced delivery of SorLA to the plasma membrane and thus a loss of function. Here, we aimed to determine if CSF levels of sSORLA in AD patients carrying SORL1 rare variants that impact or not the trafficking of the protein can be used as a novel biomarker to explore disrupted trafficking of SorLA protein in AD.
METHODS
A total of 151 participants were categorized into 5 study groups: controls without any neurodegenerative disease (n=30), patients suffering from Fronto-Temporal Lobar Degeneration (FTLD, n=34), AD patients not carrying a SORL1 rare variant (AD , n=40), AD patients carrying SORL1 trafficking-defective variants or a protein-truncating variant (PTV) (AD, n=16), and AD patients carrying a SORL1 variant with no evidence of trafficking defect (AD n=31). Thirty-three unique rare variants of SORL1 were included for this study: 3 PTVs, 13 missense variants that impact SorLA protein trafficking in in vitro cellular assays, and 17 variants with no detectable effect on SorLA protein trafficking. We measured amounts of cleaved sSorLA by western blot in CSF samples.
RESULTS
We found significantly decreased levels of sSorLA in AD, compared to all other groups. According to ROC curve analysis, levels of sSorLA showed good performances to distinguish AD patients from other AD patients (AUC=0.89 [95%CI: 0.81-0.97]).
CONCLUSIONS
Our results suggest that differential levels of sSorLA in CSF could be used as a novel marker to explore disrupted trafficking of SorLA protein in Alzheimer disease. This could help solve some proportion of variants of uncertain significance in SORL1.
背景
由Sortilin相关受体1(SORL1)基因编码的SorLA蛋白是阿尔茨海默病(AD)病理生理学中的主要参与者。功能研究表明,SorLA缺乏会导致Aβ肽产生增加,从而增加患AD的风险。SorLA在细胞表面可能会发生蛋白水解切割,导致该蛋白的可溶性胞外域(sSorLA)释放到细胞外空间。最近,我们证明,在AD患者中发现的很大一部分(约25%)罕见SORL1错义变体改变了SorLA沿组成型分泌途径的运输,导致SorLA向质膜的递送减少从而功能丧失。在此,我们旨在确定携带影响或不影响该蛋白运输的SORL1罕见变体的AD患者脑脊液中sSORLA水平是否可作为一种新型生物标志物,以探索AD中SorLA蛋白运输的破坏情况。
方法
总共151名参与者被分为5个研究组:无任何神经退行性疾病的对照组(n = 30)、患有额颞叶痴呆(FTLD,n = 34)的患者、不携带SORL1罕见变体的AD患者(AD,n = 40)、携带SORL1运输缺陷变体或蛋白截短变体(PTV)的AD患者(AD,n = 16)以及携带无运输缺陷证据的SORL1变体的AD患者(AD,n = 31)。本研究纳入了33个独特的SORL1罕见变体:3个PTV、13个在体外细胞试验中影响SorLA蛋白运输的错义变体以及17个对SorLA蛋白运输无可检测影响的变体。我们通过蛋白质印迹法测量脑脊液样本中切割后的sSorLA的量。
结果
与所有其他组相比,我们发现AD患者中sSorLA水平显著降低。根据ROC曲线分析,sSorLA水平在区分AD患者与其他AD患者方面表现良好(AUC = 0.89 [95%CI:0.81 - 0.97])。
结论
我们的结果表明,脑脊液中sSorLA的差异水平可作为一种新型标志物,用于探索阿尔茨海默病中SorLA蛋白运输的破坏情况。这可能有助于解决SORL1中一定比例的意义未明变体问题。
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