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Tau exacerbates the development of motor disturbances but has no effect on the development of irritability across the Braak stages – The HEAD Study
Tau exacerbates the development of motor disturbances but has no effect on the development of irritability across the Braak stages – The HEAD Study
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Tau exacerbates the development of motor disturbances but has no effect on the development of irritability across the Braak stages – The HEAD Study
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Tau exacerbates the development of motor disturbances but has no effect on the development of irritability across the Braak stages – The HEAD Study
Tau exacerbates the development of motor disturbances but has no effect on the development of irritability across the Braak stages – The HEAD Study

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Tau exacerbates the development of motor disturbances but has no effect on the development of irritability across the Braak stages – The HEAD Study
Tau exacerbates the development of motor disturbances but has no effect on the development of irritability across the Braak stages – The HEAD Study
Journal Article

Tau exacerbates the development of motor disturbances but has no effect on the development of irritability across the Braak stages – The HEAD Study

2025
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Overview
Background Previous studies demonstrated an association between tau pathology and the development of neuropsychiatric symptoms (NPS) in individuals with Alzheimer's disease (AD). However, the extent to which tau influences each specific NPS domain remains unclear. Here, we aim to investigate the association of tau and each NPS domain in the AD continuum. We hypothesized that tau plays a comparatively greater effect on the emergence of hyperactive and psychotic symptoms compared to other NPS domains. Method We assessed 385 individuals (216 cognitively unimpaired (CU), 128 MCI, and 41 AD dementia) from the HEAD study who underwent clinical assessments with the Neuropsychiatry Inventory Questionnaire (NPI‐Q) and had positron emission tomography (PET) for amyloid‐β (Aβ) ([18F]AZD4694 or [11C]PiB), and tau tangles ([18F]MK6240) at the same visit. Tau SUVR values were tailored with a mask from Braak stages I‐VI, using the inferior cerebellar gray matter as a reference region. All individuals with dementia had a positive Aß‐PET. Voxel‐wise and Tobit censored regression tested the association between NPS domains and biomarkers accounting for age, sex, cognitive status, and study site. We used censored regression models to account for skewed data alongside a leave‐one‐out (loo) approach to identify which NPS domains most contributed to results. Result CI individuals had significantly higher NPI‐Q scores and Tau PET SUVR than CU (Figure 1A, 1B). NPI‐Q score was significantly associated with tau‐PET predominantly in fronto‐parietal regions. Removing irritability from the models strengthened this association (Figures 2A‐C). Regression loo models revealed that motor disturbances contributed most to the association between NPS and tau‐PET across all Braak stages. Notably, irritability had a negative effect on the association in all Braak stages, suggesting that tau does not play a role in the development of irritability and is highly associated with motor disturbances (Figure 3). Conclusion Our study suggests that tau contributes to the development of motor disturbances but has no effect on the development of irritability across the AD continuum. These findings provide additional rationale for the development of new therapeutics aiming to mitigate motor disturbances and irritability in AD patients.