探究血浆游离循环核DNA和游离循环线粒体DNA对帕金森病和多系统萎缩的诊断价值。
Probing the diagnostic values of plasma cf-nDNA and cf-mtDNA for Parkinson's disease and multiple system atrophy.
作者信息
Ying Chao, Li Yuan, Zhang Hui, Pang Shimin, Hao Shuwen, Hu Songnian, Zhao Lifang
机构信息
Department of Neurobiology, Xuanwu Hospital, Capital Medical University, Beijing, China.
Beijing Municipal Geriatric Medical Research Center, Beijing, China.
出版信息
Front Neurosci. 2024 Dec 2;18:1488820. doi: 10.3389/fnins.2024.1488820. eCollection 2024.
BACKGROUND
Cell loss and mitochondrial dysfunction are key pathological features of idiopathic Parkinson's disease (PD) and multiple system atrophy (MSA). It remains unclear whether disease-specific changes in plasma circulating cell-free nuclear DNA (cf-nDNA) and mitochondrial DNA (cf-mtDNA) occur in patients with PD and MSA. In this study, we investigated whether plasma cf-nDNA, cf-mtDNA levels, as well as cf-mtDNA integrity, are altered in patients with PD and MSA.
METHODS
TaqMan probe-based quantitative PCR was employed to measure plasma cf-nDNA levels, cf-mtDNA copy numbers, and cf-mtDNA deletion levels in 171 participants, including 76 normal controls (NC), 62 PD patients, and 33 MSA patients. A generalized linear model was constructed to analyze differences in circulating cell-free DNA (cfDNA) biomarkers across clinical groups, while a logistic regression model was applied to assess the predictive values of these biomarkers for developing PD or MSA. Spearman correlations were used to explore associations between the three cfDNA biomarkers, demographic data, and clinical scales.
RESULTS
No significant differences in plasma cf-nDNA levels, cf-mtDNA copy numbers, or cf-mtDNA deletion levels were observed among the PD, MSA, and NC groups (all > 0.05). Additionally, these measures were not associated with the risk of developing PD or MSA. In PD patients, cf-nDNA levels were positively correlated with Hamilton Anxiety Rating Scale scores (Rho = 0.382, FDR adjusted = 0.027). In MSA patients, cf-nDNA levels were positively correlated with International Cooperative Ataxia Rating Scale scores (Rho = 0.588, FDR adjusted = 0.011) and negatively correlated with Montreal Cognitive Assessment scores (Rho = -0.484, FDR adjusted = 0.044). Subgroup analysis showed that PD patients with constipation had significantly lower plasma cf-mtDNA copy numbers than those without constipation ( = 0.049). MSA patients with cognitive impairment had significantly higher cf-nDNA levels compared to those without ( = 0.008).
CONCLUSION
Plasma cf-nDNA level, cf-mtDNA copy number, and cf-mtDNA deletion level have limited roles as diagnostic biomarkers for PD and MSA. However, their correlations with clinical symptoms support the hypothesis that cell loss and mitochondrial dysfunction are involved in PD and MSA development.
背景
细胞丢失和线粒体功能障碍是特发性帕金森病(PD)和多系统萎缩(MSA)的关键病理特征。目前尚不清楚PD和MSA患者血浆中循环游离核DNA(cf-nDNA)和线粒体DNA(cf-mtDNA)是否存在疾病特异性变化。在本研究中,我们调查了PD和MSA患者血浆cf-nDNA、cf-mtDNA水平以及cf-mtDNA完整性是否发生改变。
方法
采用基于TaqMan探针的定量PCR技术,检测了171名参与者的血浆cf-nDNA水平、cf-mtDNA拷贝数和cf-mtDNA缺失水平,其中包括76名正常对照(NC)、62名PD患者和33名MSA患者。构建广义线性模型分析不同临床组循环游离DNA(cfDNA)生物标志物的差异,同时应用逻辑回归模型评估这些生物标志物对发生PD或MSA的预测价值。采用Spearman相关性分析探索三种cfDNA生物标志物、人口统计学数据和临床量表之间的关联。
结果
在PD组、MSA组和NC组之间,血浆cf-nDNA水平、cf-mtDNA拷贝数或cf-mtDNA缺失水平均未观察到显著差异(均>0.05)。此外,这些指标与发生PD或MSA的风险无关。在PD患者中,cf-nDNA水平与汉密尔顿焦虑量表评分呈正相关(Rho = 0.382,FDR校正 = 0.027)。在MSA患者中,cf-nDNA水平与国际合作共济失调量表评分呈正相关(Rho = 0.588,FDR校正 = 0.011),与蒙特利尔认知评估量表评分呈负相关(Rho = -0.484,FDR校正 = 0.044)。亚组分析显示,便秘的PD患者血浆cf-mtDNA拷贝数显著低于无便秘的患者(P = 0.049)。有认知障碍的MSA患者cf-nDNA水平显著高于无认知障碍的患者(P = 0.008)。
结论
血浆cf-nDNA水平、cf-mtDNA拷贝数和cf-mtDNA缺失水平作为PD和MSA的诊断生物标志物作用有限。然而,它们与临床症状的相关性支持了细胞丢失和线粒体功能障碍参与PD和MSA发病机制的假说。
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