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Blood-based systems biology biomarkers fornext-generation clinical trials in Alzheimer’s disease

机译:基于血液的系统生物学生物标志物阿尔茨海默氏病的下一代临床试验

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摘要

Alzheimer’s disease (AD)—a complex disease showing multiple pathomechanistic alterations—is triggered by nonlinear dynamic interactions of genetic/epigenetic and environmental risk factors, which, ultimately, converge into a biologically heterogeneous disease. To tackle the burden of AD during early preclinical stages, accessible blood-based biomarkers are currently being developed. Specifically, next-generation clinical trials are expected to integrate positive and negative predictive blood-based biomarkers into study designs to evaluate, at the individual level, target druggability and potential drug resistance mechanisms. In this scenario, systems biology holds promise to accelerate validation and qualification for clinical trial contexts of use—including proof-of-mechanism, patient selection, assessment of treatment efficacy and safety rates, and prognostic evaluation. Albeit in their infancy, systems biology-based approaches are poised to identify relevant AD “signatures” through multifactorial and interindividual variability, allowing us to decipher disease pathophysiology and etiology. Hopefully, innovative biomarker-drug codevelopment strategies will be the road ahead towards effective disease-modifying drugs.

机译:阿尔茨海默氏病(AD)是一种显示多种病理机制改变的复杂疾病,是由遗传/表观遗传因素和环境风险因素的非线性动态相互作用触发的,最终,这些疾病会聚为生物异质性疾病。为了在临床前早期解决AD的负担,目前正在开发可利用的基于血液的生物标记。具体而言,下一代临床试验有望将阳性和阴性的基于血液的预测生物标记物整合到研究设计中,以在个体水平上评估目标药物可及性和潜在的耐药性机制。在这种情况下,系统生物学有望加快临床试验使用环境的验证和鉴定,包括机理证明,患者选择,治疗疗效和安全性评估以及预后评估。尽管处于起步阶段,但基于系统生物学的方法已准备好通过多因素和个体间的可变性来识别相关的AD“特征”,从而使我们能够了解疾病的病理生理和病因。希望创新的生物标志物-药物联合开发策略将成为通往有效的疾病缓解药物的道路。

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