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Tau Co-Pathology in DLB Clinical Heterogeneity

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experiment621 wordssynced 2026-04-02

Tau Co-Pathology in DLB Clinical Heterogeneity

Pathway Diagram

flowchart TD N0["TAU"] N1["APP"] N1 -->|"associated with"| N0 N2["AKT"] N2 -->|"associated with"| N0 N3["APOE"] N3 -->|"associated with"| N0 N4["SNCA"] N0 -->|"associated with"| N4 N5["MAPT"] N5 -->|"associated with"| N0 N0 -->|"associated with"| N3 N6["GFAP"] N0 -->|"biomarker for"| N6 N7["NFL"] N0 -->|"biomarker for"| N7 N8["PSEN1"] N0 -->|"associated with"| N8 N9["TARDBP"] N9 -->|"associated with"| N0 N0 -->|"associated with"| N6 N10["NEURODEGENERATION"] N0 -->|"associated with"| N10

Overview

Dementia with Lewy bodies (DLB) is the second most common neurodegenerative dementia after Alzheimer's disease, characterized primarily by pathological accumulation of alpha-synuclein in Lewy bodies and Lewy neurites. However, emerging evidence demonstrates that tau co-pathology—the concurrent accumulation of phosphorylated tau—plays a significant role in driving clinical heterogeneity in DLB presentations. Tau co-pathology in DLB represents a fundamental intersection between two major proteinopathies and serves as a critical variable explaining the wide spectrum of cognitive, motor, and neuropsychiatric manifestations observed across DLB patients. Understanding tau's contribution to DLB heterogeneity has profound implications for patient stratification, prognosis prediction, and therapeutic targeting.

Function/Biology


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