Samanta Mazzetti, Elena Contaldi, Milo Jarno Basellini, Claudia Novello, Alessandra Maria Calogero, Letizia Straniero, Federica Garrì, Valentina Ferri, Daniela Calandrella, Francesca Del Sorbo, Rosanna Asselta, Emanuele Cereda, Graziella Cappelletti, Ioannis Ugo Isaias, Gianni Pezzoli
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We previously demonstrated that α-synuclein oligomers expressed as proximity ligation assay (PLA) score in synaptic terminals of skin biopsy are a reliable biomarker for distinguishing idiopathic PD (iPD) from healthy controls (HC). This cross-sectional study investigates an unexplored cohort of <i>GBA1</i>-PD (<i>n</i> = 27) compared to 28 HC, and 36 iPD cases to (i) analyze α-synuclein oligomers and quantify them throughout PLA score, (ii) investigate GCase expression in brain and synaptic terminals targeting the sweat gland, (iii) unravel indicators that could differentiate patients with specific <i>GBA1</i> mutations. PLA score discriminates <i>GBA1</i>-PD from HC with sensitivity = 88.9% (95% CI 70.84–97.65), specificity = 88.5% (95% CI 69.85–97.55), and PPV = 88.9% (95% CI 73.24–95.90), AUC value = 0.927 (95% CI 0.859–0.996). No difference was found between <i>GBA1</i>-PD patients and iPD, suggesting a common pathological pathway based on α-synuclein oligomers. GCase score did not differ in <i>GBA1</i>-PD, iPD, and HC in the synaptic terminals, whereas a positive correlation was found between PLA score and GCase score. Moreover, a significant increase in synaptic density was observed in <i>GBA1</i>-PD compared to iPD and HC (<i>P</i> < 0.0001). Employing ROC curve to discriminate <i>GBA1</i>-PD from iPD, we found an AUC value for synaptic density = 0.855 (95% CI 0.749–0.961) with sensitivity = 85.2% (95% CI 66.27%–95.81%), specificity = 77.1% (95% CI 59.86%–89.58%), and PPV = 74.19% (60.53%–84.35%). The highest synaptic density values were observed in p.N409S patients. This work points out to the value of both PLA score and synaptic density in distinguishing <i>GBA1</i>-PD from iPD and to their potential to stratify and monitor patients in the context of new pathway-specific therapeutic options.</p>","PeriodicalId":9290,"journal":{"name":"Brain Pathology","volume":"34 6","pages":""},"PeriodicalIF":5.8000,"publicationDate":"2024-09-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://onlinelibrary.wiley.com/doi/epdf/10.1111/bpa.13284","citationCount":"0","resultStr":"{\"title\":\"Comparing GBA1-Parkinson's disease and idiopathic Parkinson's disease: α-Synuclein oligomers and synaptic density as biomarkers in the skin biopsy\",\"authors\":\"Samanta Mazzetti, Elena Contaldi, Milo Jarno Basellini, Claudia Novello, Alessandra Maria Calogero, Letizia Straniero, Federica Garrì, Valentina Ferri, Daniela Calandrella, Francesca Del Sorbo, Rosanna Asselta, Emanuele Cereda, Graziella Cappelletti, Ioannis Ugo Isaias, Gianni Pezzoli\",\"doi\":\"10.1111/bpa.13284\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p>The main genetic risk factors for Parkinson's disease (PD) are presently represented by variants in <i>GBA1</i> gene encoding for the β-glucocerebrosidase (GCase). Searching for a peripheral biomarker that can be used for selecting and monitoring patients in clinical trials targeting <i>GBA1</i>-associated PD (<i>GBA1</i>-PD) is a current challenge. We previously demonstrated that α-synuclein oligomers expressed as proximity ligation assay (PLA) score in synaptic terminals of skin biopsy are a reliable biomarker for distinguishing idiopathic PD (iPD) from healthy controls (HC). This cross-sectional study investigates an unexplored cohort of <i>GBA1</i>-PD (<i>n</i> = 27) compared to 28 HC, and 36 iPD cases to (i) analyze α-synuclein oligomers and quantify them throughout PLA score, (ii) investigate GCase expression in brain and synaptic terminals targeting the sweat gland, (iii) unravel indicators that could differentiate patients with specific <i>GBA1</i> mutations. PLA score discriminates <i>GBA1</i>-PD from HC with sensitivity = 88.9% (95% CI 70.84–97.65), specificity = 88.5% (95% CI 69.85–97.55), and PPV = 88.9% (95% CI 73.24–95.90), AUC value = 0.927 (95% CI 0.859–0.996). No difference was found between <i>GBA1</i>-PD patients and iPD, suggesting a common pathological pathway based on α-synuclein oligomers. GCase score did not differ in <i>GBA1</i>-PD, iPD, and HC in the synaptic terminals, whereas a positive correlation was found between PLA score and GCase score. Moreover, a significant increase in synaptic density was observed in <i>GBA1</i>-PD compared to iPD and HC (<i>P</i> < 0.0001). Employing ROC curve to discriminate <i>GBA1</i>-PD from iPD, we found an AUC value for synaptic density = 0.855 (95% CI 0.749–0.961) with sensitivity = 85.2% (95% CI 66.27%–95.81%), specificity = 77.1% (95% CI 59.86%–89.58%), and PPV = 74.19% (60.53%–84.35%). The highest synaptic density values were observed in p.N409S patients. 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引用次数: 0
摘要
帕金森病(PD)的主要遗传风险因素目前以编码β-葡糖脑苷脂(GCase)的GBA1基因变异为代表。在针对 GBA1 相关帕金森病(GBA1-PD)的临床试验中,寻找一种可用于选择和监测患者的外周生物标记物是目前面临的一项挑战。我们以前曾证实,在皮肤活检的突触末端中以邻近结扎法(PLA)评分表达的α-突触核蛋白寡聚体是区分特发性帕金森病(iPD)和健康对照组(HC)的可靠生物标记物。这项横断面研究调查了一组尚未研究过的GBA1-PD患者(n = 27),与28例HC患者和36例iPD病例进行了比较,目的是:(i) 分析α-突触核蛋白寡聚体,并通过PLA评分对其进行量化;(ii) 调查GCase在大脑和以汗腺为目标的突触末端的表达;(iii) 揭示可区分特定GBA1突变患者的指标。PLA 评分能将 GBA1-PD 与 HC 区分开来,灵敏度 = 88.9% (95% CI 70.84-97.65),特异度 = 88.5% (95% CI 69.85-97.55),PPV = 88.9% (95% CI 73.24-95.90),AUC 值 = 0.927 (95% CI 0.859-0.996)。GBA1-PD患者和iPD患者之间没有发现差异,这表明基于α-突触核蛋白寡聚体的病理途径是相同的。在突触末端,GBA1-PD、iPD 和 HC 的 GCase 评分没有差异,而 PLA 评分与 GCase 评分呈正相关。此外,与 iPD 和 HC 相比,GBA1-PD 的突触密度明显增加(P
Comparing GBA1-Parkinson's disease and idiopathic Parkinson's disease: α-Synuclein oligomers and synaptic density as biomarkers in the skin biopsy
The main genetic risk factors for Parkinson's disease (PD) are presently represented by variants in GBA1 gene encoding for the β-glucocerebrosidase (GCase). Searching for a peripheral biomarker that can be used for selecting and monitoring patients in clinical trials targeting GBA1-associated PD (GBA1-PD) is a current challenge. We previously demonstrated that α-synuclein oligomers expressed as proximity ligation assay (PLA) score in synaptic terminals of skin biopsy are a reliable biomarker for distinguishing idiopathic PD (iPD) from healthy controls (HC). This cross-sectional study investigates an unexplored cohort of GBA1-PD (n = 27) compared to 28 HC, and 36 iPD cases to (i) analyze α-synuclein oligomers and quantify them throughout PLA score, (ii) investigate GCase expression in brain and synaptic terminals targeting the sweat gland, (iii) unravel indicators that could differentiate patients with specific GBA1 mutations. PLA score discriminates GBA1-PD from HC with sensitivity = 88.9% (95% CI 70.84–97.65), specificity = 88.5% (95% CI 69.85–97.55), and PPV = 88.9% (95% CI 73.24–95.90), AUC value = 0.927 (95% CI 0.859–0.996). No difference was found between GBA1-PD patients and iPD, suggesting a common pathological pathway based on α-synuclein oligomers. GCase score did not differ in GBA1-PD, iPD, and HC in the synaptic terminals, whereas a positive correlation was found between PLA score and GCase score. Moreover, a significant increase in synaptic density was observed in GBA1-PD compared to iPD and HC (P < 0.0001). Employing ROC curve to discriminate GBA1-PD from iPD, we found an AUC value for synaptic density = 0.855 (95% CI 0.749–0.961) with sensitivity = 85.2% (95% CI 66.27%–95.81%), specificity = 77.1% (95% CI 59.86%–89.58%), and PPV = 74.19% (60.53%–84.35%). The highest synaptic density values were observed in p.N409S patients. This work points out to the value of both PLA score and synaptic density in distinguishing GBA1-PD from iPD and to their potential to stratify and monitor patients in the context of new pathway-specific therapeutic options.
期刊介绍:
Brain Pathology is the journal of choice for biomedical scientists investigating diseases of the nervous system. The official journal of the International Society of Neuropathology, Brain Pathology is a peer-reviewed quarterly publication that includes original research, review articles and symposia focuses on the pathogenesis of neurological disease.