Assessment of neurovascular uncoupling: <i>APOE</i> status is a key driver of early metabolic and vascular dysfunction-Reference-Cited by-同舟云学术

Assessment of neurovascular uncoupling: APOE status is a key driver of early metabolic and vascular dysfunction

Published:2024-05-07 Issue:7 Volume:20 Page:4951-4969
ISSN:1552-5260
Container-title:Alzheimer's & Dementia
language:en
Short-container-title:Alzheimer's & Dementia

Author:

Onos Kristen D.¹,Lin Peter B.²³,Pandey Ravi S.⁴,Persohn Scott A.²,Burton Charles P.²,Miner Ethan W.²,Eldridge Kierra²,Kanyinda Jonathan Nyandu¹,Foley Kate E.¹²,Carter Gregory W.¹⁴,Howell Gareth R.¹,Territo Paul R.²⁵

Affiliation:

1. The Jackson Laboratory Bar Harbor Maine USA

2. Stark Neurosciences Research Institute Indiana University School of Medicine Indianapolis Indiana USA

3. Department of Neurology Washington University in St. Louis St. Louis Missouri USA

4. The Jackson Laboratory for Genomic Medicine Farmington Connecticut USA

5. Department of Medicine Division of Clinical Pharmacology Indiana University School of Medicine Indianapolis Indiana USA

Abstract

AbstractBACKGROUNDAlzheimer's disease (AD) is the most common cause of dementia worldwide, with apolipoprotein Eε4 (APOEε4) being the strongest genetic risk factor. Current clinical diagnostic imaging focuses on amyloid and tau; however, new methods are needed for earlier detection.METHODSPET imaging was used to assess metabolism‐perfusion in both sexes of aging C57BL/6J, and hAPOE mice, and were verified by transcriptomics, and immunopathology.RESULTSAll hAPOE strains showed AD phenotype progression by 8 months, with females exhibiting the regional changes, which correlated with GO‐term enrichments for glucose metabolism, perfusion, and immunity. Uncoupling analysis revealed APOEε4/ε4 exhibited significant Type‐1 uncoupling (↓ glucose uptake, ↑ perfusion) at 8 and 12 months, while APOEε3/ε4 demonstrated Type‐2 uncoupling (↑ glucose uptake, ↓ perfusion), while immunopathology confirmed cell specific contributions.DISCUSSIONThis work highlights APOEε4 status in AD progression manifests as neurovascular uncoupling driven by immunological activation, and may serve as an early diagnostic biomarker.Highlights

We developed a novel analytical method to analyze PET imaging of 18F‐FDG and 64Cu‐PTSM data in both sexes of aging C57BL/6J, and hAPOEε3/ε3, hAPOEε4/ε4, and hAPOEε3/ε4 mice to assess metabolism‐perfusion profiles termed neurovascular uncoupling.

This analysis revealed APOEε4/ε4 exhibited significant Type‐1 uncoupling (decreased glucose uptake, increased perfusion) at 8 and 12 months, while APOEε3/ε4 demonstrated significant Type‐2 uncoupling (increased glucose uptake, decreased perfusion) by 8 months which aligns with immunopathology and transcriptomic signatures.

This work highlights that there may be different mechanisms underlying age related changes in APOEε4/ε4 compared with APOEε3/ε4. We predict that these changes may be driven by immunological activation and response, and may serve as an early diagnostic biomarker.

Publisher

Wiley

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