Association of neuroinflammation with episodic memory: a [11C]PBR28 PET study in cognitively discordant twin pairs

Jaakko Kaprio; Päivi Marjamäki; Juha O Rinne; Mira Karrasch; Eero Vuoksimaa; Semi Helin; Jouni Tuisku; Noora Lindgren

Association of neuroinflammation with episodic memory: a [11C]PBR28 PET study in cognitively discordant twin pairs

Jaakko Kaprio; Päivi Marjamäki; Juha O Rinne; Mira Karrasch; Eero Vuoksimaa; Semi Helin; Jouni Tuisku; Noora Lindgren

Association of neuroinflammation with episodic memory: a [11C]PBR28 PET study in cognitively discordant twin pairs

Jaakko Kaprio

Päivi Marjamäki

Juha O Rinne

Mira Karrasch

Eero Vuoksimaa

Semi Helin

Jouni Tuisku

Noora Lindgren

Katso/Avaa

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Lataukset:

doi:10.1093/braincomms/fcaa024

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Julkaisun pysyvä osoite on:
https://urn.fi/URN:NBN:fi-fe2021042827237

Tiivistelmä

Alzheimer’s disease is associated with chronic response of innate immune
system, referred as neuroinflammation. PET radioligands binding to the
18 kDa translocator protein are potential biomarkers of
neuroinflammation. Translocator protein PET studies in mild cognitive
impairment and Alzheimer’s disease have indicated controversial results,
possibly reflecting interindividual variation and heterogeneity of
study populations. We controlled for genetic and environmental effects
by studying twin pairs discordant for episodic memory performance.
Episodic memory impairment is a well-known cognitive hallmark of early
Alzheimer’s disease process. Eleven same-sex twin pairs (four
monozygotic pairs, six female pairs, age 72–77 years) underwent [¹¹C]N-acetyl-N-(2-methoxybenzyl)-2-phenoxy-5-pyridinamine ([¹¹C]PBR28)
PET imaging, structural magnetic resonance imaging and
neuropsychological testing in 2014–17. Main PET outcome was the
volume-weighted average standardized uptake value of cortical regions
vulnerable to Alzheimer’s disease pathology. Ten pairs were discordant
for episodic memory performance. In the eight pairs with identical
translocator protein genotype, twins with poorer episodic memory had
∼20% higher cortical [¹¹C]PBR28 binding compared with their
better-performing co-twins (mean intra-pair difference 0.21 standardized
uptake value, 95% confidence interval 0.05–0.37, P = 0.017).
The result remained the same when including all discordant pairs and
controlling for translocator protein genotype. Increased translocator
protein PET signal suggests that increased microglial activation is
associated with poorer episodic memory performance. Twins with worse
episodic memory performance compared with their co-twins had on average
20% higher uptake of the neuroinflammatory marker translocator protein
PET tracer ¹¹[¹¹C]PBR28. The findings support a
negative association between neuroinflammation and episodic memory and
the use of translocator protein positron emission tomography as a useful
indicator of Alzheimer’s disease process.

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