Neuroinflammation and amyloid load in different age groups of individuals with Down syndrome: A PET imaging study.

INTRODUCTION

Down syndrome (DS) is associated with early-onset Alzheimer's disease (AD). This study evaluated neuroinflammation and amyloid beta (Aβ) load in individuals with DS of different ages, using positron emission tomography (PET) imaging.

METHODS

DS (n = 29) and age-matched non-DS (n = 35) individuals underwent [C]PK11195 and [C]PiB (Pittsburgh compound B) PET scans, for assessment of neuroinflammation and Aβ load, respectively. Voxel-wise and region-based analyses were conducted, and associations between [C]PK11195 binding and Aβ load were investigated.

RESULTS

Individuals with DS exhibited increased [C]PK11195 binding compared to non-DS controls, with most pronounced differences in older (≥50 years) adults, followed by younger (20-34 years), and intermediate (35-49 years) ages. Among DS participants, 13 individuals were amyloid positive. Associations were observed between [C]PK11195 binding and global Aβ load.

DISCUSSION

Neuroinflammation in DS follows a region-specific pattern, partially associated with amyloid deposition, and may contribute to the early progression of AD-related pathology.

HIGHLIGHTS

Neuroinflammation is elevated in Down syndrome (DS) versus age-matched non-DS controls. Neuroinflammation in DS shows a different pattern depending on the brain region. [C]PK11195 uptake has a positive monotonic association with amyloid burden.