Biological effects of pathologies in Lewy body diseases: why timing matters

Elie Matar, Glenda M Halliday
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Abstract

The emergence of promising biomarkers of α-synuclein Lewy pathology has led to new biological definitions and staging systems for Parkinson's disease and dementia with Lewy bodies. These research frameworks aim to enhance patient selection for studies of biomarkers and disease-modifying therapies. Building on approaches developed for Alzheimer's disease, these new frameworks focus on hallmark neuropathological findings in Lewy body diseases, including abnormal α-synuclein aggregates and neurodegeneration, particularly nigrostriatal dopaminergic loss. Understanding the temporal inter-relationships between Lewy pathology, Alzheimer's disease, and other co-pathologies and symptom manifestation is central to any biological staging system. Neuropathological and in vivo evidence demonstrates substantial temporal and biological heterogeneity in the progression of clinical and pathological events across Lewy body disorders, highlighting knowledge gaps. Staging systems must incorporate this evidence into a nuanced conceptual framework of biological progression. Such revision will be crucial for the appropriate selection of participants and correct timing of targeted interventions in clinical research.
路易体疾病病理的生物学效应:为什么时间很重要
α-突触核蛋白路易体病理学生物标志物的出现为帕金森病和路易体痴呆带来了新的生物学定义和分期系统。这些研究框架旨在加强对生物标志物和疾病修饰疗法研究的患者选择。在针对阿尔茨海默病开发的方法的基础上,这些新框架关注路易体疾病的标志性神经病理学发现,包括异常α-突触核蛋白聚集和神经变性,特别是黑质纹状体多巴胺能丧失。了解路易氏病、阿尔茨海默病和其他共病和症状表现之间的时间相互关系是任何生物学分期系统的核心。神经病理学和体内证据表明,路易体疾病的临床和病理事件的进展存在大量的时间和生物学异质性,突出了知识差距。分期系统必须将这些证据纳入生物学进展的微妙概念框架中。这样的修订对于临床研究中参与者的适当选择和目标干预的正确时机至关重要。
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