AbstractBackgroundCognitively unimpaired (CU) adults with Alzheimer’s disease (AD) pathologic change may be more vulnerable to developing neuropsychiatric symptoms. We reported an association of higher β‐amyloid (Aβ) and increased anxiety/depression during the COVID‐19 lockdown in CU adults (Akinci et al., 2022). Here, we investigated whether changes in Aβ1−42 predict post‐traumatic stress disorder (PTSD) symptomatology following COVID‐19 lockdown in CU adults at risk for AD.MethodWe included 128 CU participants who underwent lumbar puncture 2.3±0.6 years before and 1.1±0.4 years after the lockdown. The outcome of interest was self‐reported PTSD symptomatology (Impact of Event Scale Revised) measured 1.7±0.1 years after the lockdown. The main predictor was annual rate of change in cerebrospinal fluid (CSF) Aβ1−42 measured with the NeuroToolKit panel of robust prototype assays (Roche Diagnostics International Ltd, Rotkreuz, Switzerland). Other predictors included sex, age, years of education, stressors during COVID‐19, and anxiety/depression (Hospital Anxiety and Depression Scale, HADS) and perceived stress (Perceived Stress Scale, PSS) measured during lockdown. We performed regression analyses to explore the association between annual rate of change in Aβ1‐42 with PTSD scores adjusting for demographic and stressor variables, and further adjusting for HADS and PSS scores. We then explored the mediating effect of HADS and PSS on the association between change in Aβ1‐42 and PTSD scores.ResultParticipant age ranged from 53−72 and 59% were women (Table 1). Independent of demographic variables and stressors experienced during COVID‐19, the rate of annual change in Aβ1‐42 predicted PTSD scores (p = .008; Table 2). This association attenuated after introducing HADS and PSS scores into the model (p = .066). We found full mediation effects of HADS and PSS scores, explaining 46% and 40% of the effect of annual change in Aβ1‐42 on PTSD scores, respectively (Figure 1).ConclusionCU older adults with longitudinal CSF Aβ1−42 increases are more vulnerable to developing PTSD symptomatology after a stressful event, such as the pandemic. Anxiety/depression is one plausible mechanism through which increases in Aβ might exacerbate PTSD symptomatology. The results suggest a window for stress regulation during stressful events to prevent further mental health worsening in people at risk for AD.