分子、表型和功能性衰老生物标志物在痴呆症预测中的互补价值

IF 5.3 2区 医学 Q1 GERIATRICS & GERONTOLOGY GeroScience Pub Date : 2024-10-24 DOI:10.1007/s11357-024-01376-w
Andreas Engvig, Karl Trygve Kalleberg, Lars T. Westlye, Esten Høyland Leonardsen
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引用次数: 0

摘要

DNA甲基化年龄(MA)、脑年龄(BA)和虚弱指数(FI)是与痴呆症风险相关的假定衰老生物标志物。我们利用 ADNI 数据库研究了它们之间的关系以及预测认知障碍和未来痴呆症风险的综合潜力。在几种MA算法中,与记忆相关的DunedinPACE和GrimAge2与BA和数据驱动的FI一起被组合成复合MA进行预测分析。年龄和性别调整后的 MA(aMA)、aBA 和 aFI 测量值之间的配对相关性较低。在所有诊断任务中,FI的表现均优于BA和MA。包括年龄、性别和 aFI 在内的一个模型的曲线下面积(AUC)达到了 0.94,可用于在保持不变的测试集中区分认知正常对照组(CN)和痴呆症患者。当与临床生物标记物(载脂蛋白 E ε4等位基因数量、记忆力、执行功能)相结合时,包括 aBA 和 aFI 的模型可以预测 MCI 患者 5 年的痴呆风险,样本外 AUC 为 0.88。在预后模型中,BA 和 FI 具有互补价值(β均为 0.50)。测试的 MA 并未提高预测效果。各种 FI 算法的结果是一致的,数据驱动的健康缺陷选择性能最佳。FI 对男性预后的不利影响更大,而 BA 对女性的影响更大。我们的研究结果凸显了 BA 和 FI 在痴呆症预测中的互补价值。研究结果支持从多维度看待痴呆症,包括生物标志物、性别和预后之间相互交织的关系。所测试的 MA 的作用有限,因此在将其用于痴呆症的个体风险评估时应谨慎。
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Complementary value of molecular, phenotypic, and functional aging biomarkers in dementia prediction

DNA methylation age (MA), brain age (BA), and frailty index (FI) are putative aging biomarkers linked to dementia risk. We investigated their relationship and combined potential for prediction of cognitive impairment and future dementia risk using the ADNI database. Of several MA algorithms, DunedinPACE and GrimAge2, associated with memory, were combined in a composite MA alongside BA and a data-driven FI in predictive analyses. Pairwise correlations between age- and sex-adjusted measures for MA (aMA), aBA, and aFI were low. FI outperformed BA and MA in all diagnostic tasks. A model including age, sex, and aFI achieved an area under the curve (AUC) of 0.94 for differentiating cognitively normal controls (CN) from dementia patients in a held-out test set. When combined with clinical biomarkers (apolipoprotein E ε4 allele count, memory, executive function), a model including aBA and aFI predicted 5-year dementia risk among MCI patients with an out-of-sample AUC of 0.88. In the prognostic model, BA and FI offered complementary value (both βs 0.50). The tested MAs did not improve predictions. Results were consistent across FI algorithms, with data-driven health deficit selection yielding the best performance. FI had a stronger adverse effect on prognosis in males, while BA’s impact was greater in females. Our findings highlight the complementary value of BA and FI in dementia prediction. The results support a multidimensional view of dementia, including an intertwined relationship between the biomarkers, sex, and prognosis. The tested MA’s limited contribution suggests caution in their use for individual risk assessment of dementia.

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来源期刊
GeroScience
GeroScience Medicine-Complementary and Alternative Medicine
CiteScore
10.50
自引率
5.40%
发文量
182
期刊介绍: GeroScience is a bi-monthly, international, peer-reviewed journal that publishes articles related to research in the biology of aging and research on biomedical applications that impact aging. The scope of articles to be considered include evolutionary biology, biophysics, genetics, genomics, proteomics, molecular biology, cell biology, biochemistry, endocrinology, immunology, physiology, pharmacology, neuroscience, and psychology.
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