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      18F‐MK6240 longitudinal tau PET in ageing and Alzheimer’s disease

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      https://www.riss.kr/link?id=O119464302

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      Longitudinal tau PET may prove useful for clinical trials, through its ability to detect patterns and rates of in vivo tau accumulation in ageing and Alzheimer’s disease (AD). Clinical trials are increasingly targeting the preclinical phase of AD. F...

      Longitudinal tau PET may prove useful for clinical trials, through its ability to detect patterns and rates of in vivo tau accumulation in ageing and Alzheimer’s disease (AD). Clinical trials are increasingly targeting the preclinical phase of AD. Flortaucipir studies estimate a 3% annual increase in global cortical tau SUVR in amyloid‐β positive (Aβ+ve) cognitively impaired (CI) cohorts, whereas either no change, or low rates of increase (0.5%), have been demonstrated in Aβ+ve cognitively unimpaired (CU) cohorts. F‐18 MK6240 is a novel tau tracer, with high target to background binding. We aimed to evaluate regional rates of 18F‐MK6240 accumulation in ageing and the AD continuum.
      We performed PET acquisition 90‐100 minutes post‐injection of 185MBq (±10%) 18F‐MK6240 at baseline and 12 months for 67 Aβ‐ve CU, 20 Aβ+ve CU and 19 Aβ+ve CI participants. SUVR (standardized uptake value ratio) for the entorhinal cortex, amygdala, hippocampus, parahippocampus and composite regions of interest (ROI) (Me, mesial temporal; Te, temporoparietal cortices) were generated using the cerebellar cortex as the reference region.
      Age did not significantly differ between the groups (mean age 74 ± 4.4 Aβ‐ve CU, 76.2 ± 5.7 Aβ+ve CU, 72.5 ± 6.4 Aβ+ve CI). Aβ+ve participants (CU and CI) had higher baseline tau SUVR and higher annual percentage increases in tau SUVR compared to Aβ‐ve participants in all regions examined (Table 1) (Figure 1). CU Aβ+ve participants had larger increases in Me vs Te (1.6% vs 0.7%), while CI Aβ+ve participants had larger increases in Te vs Me (4.3% vs 1.9%). Compared to Aβ‐ve CU participants, Aβ+ve CU participants had higher increases in the amygdala (2.9% vs 1.8%) and entorhinal cortex (1.9% vs 0.7%).
      Longitudinal tau imaging using 18F‐MK6240 discriminates between ageing and stages of AD. Rate of accumulation in preclinical AD (Aβ+ve CU) was highest in mesial temporal regions, while in CI individuals, rates were highest in the temporoparietal cortex. The amygdala and entorhinal cortex may be early regions to discriminate tau accumulation between Aβ‐ve CU and Aβ+ve groups. However, as the variance is large, the precision of these estimates may be refined with a larger sample size. Recruitment is ongoing.

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