open access publication

Article, 2024

Developing a novel dual-injection FDG-PET imaging methodology to study the functional neuroanatomy of gait

NeuroImage, ISSN 1095-9572, 1053-8119, Volume 288, Page 120531, 10.1016/j.neuroimage.2024.120531

Contributors

Sigurdsson, Hilmar P 0000-0002-0624-065X (Corresponding author) [1] Alcock, Lisa 0000-0002-8364-9803 [1] [2] Firbank, Michael John 0000-0002-9536-0185 [1] Wilson, Ross [1] Brown, Philip [2] Maxwell, Ross [1] Bennett, Elizabeth [3] Pavese, Nicola 0000-0002-6801-6194 [1] [4] Brooks, David James 0000-0003-2602-2518 [1] [4] Rochester, Lynn 0000-0001-5774-9272 [1] [2]

Affiliations

  1. [1] Newcastle University
    2. [NORA names: United Kingdom; Europe, Non-EU; OECD];
  2. [2] Newcastle upon Tyne Hospitals NHS Foundation Trust
    3. [NORA names: United Kingdom; Europe, Non-EU; OECD];
  3. [3] North Cumbria Integrated Care NHS Foundation Trust
    4. [NORA names: United Kingdom; Europe, Non-EU; OECD];
  4. [4] Aarhus University
    5. [NORA names: AU Aarhus University; University; Denmark; Europe, EU; Nordic; OECD]

Abstract

Gait is an excellent indicator of physical, emotional, and mental health. Previous studies have shown that gait impairments in ageing are common, but the neural basis of these impairments are unclear. Existing methodologies are suboptimal and novel paradigms capable of capturing neural activation related to real walking are needed. In this study, we used a hybrid PET/MR system and measured glucose metabolism related to both walking and standing with a dual-injection paradigm in a single study session. For this study, 15 healthy older adults (10 females, age range: 60.5-70.7 years) with normal cognition were recruited from the community. Each participant received an intravenous injection of [18F]-2-fluoro-2-deoxyglucose (FDG) before engaging in two distinct tasks, a static postural control task (standing) and a walking task. After each task, participants were imaged. To discern independent neural functions related to walking compared to standing, we applied a bespoke dose correction to remove the residual 18F signal of the first scan (PETSTAND) from the second scan (PETWALK) and proportional scaling to the global mean, cerebellum, or white matter (WM). Whole-brain differences in walking-elicited neural activity measured with FDG-PET were assessed using a one-sample t-test. In this study, we show that a dual-injection paradigm in healthy older adults is feasible with biologically valid findings. Our results with a dose correction and scaling to the global mean showed that walking, compared to standing, increased glucose consumption in the cuneus (Z = 7.03), the temporal gyrus (Z = 6.91) and the orbital frontal cortex (Z = 6.71). Subcortically, we observed increased glucose metabolism in the supraspinal locomotor network including the thalamus (Z = 6.55), cerebellar vermis and the brainstem (pedunculopontine/mesencephalic locomotor region). Exploratory analyses using proportional scaling to the cerebellum and WM returned similar findings. Here, we have established the feasibility and tolerability of a novel method capable of capturing neural activations related to actual walking and extended previous knowledge including the recruitment of brain regions involved in sensory processing. Our paradigm could be used to explore pathological alterations in various gait disorders.

Keywords

F signals, FDG-PET, activity, actual walking, adults, age, alterations, analysis, basis, biology, brain regions, brainstem, cerebellar vermis, cerebellum, cognition, community, consumption, control task, correction, cortex, cuneus, differences, disorders, dose, dose correction, dual-injection, excellent indicator, exploratory analysis, feasibility, findings, frontal cortex, function, functional neuroanatomy, gait, gait disorders, gait impairment, global mean, glucose consumption, glucose metabolism, gyrus, health, healthy older adults, imaging methodology, impairment, increased glucose consumption, increased glucose metabolism, indicators, intravenous injection, knowledge, locomotor networks, matter, mean, measure glucose metabolism, mental health, metabolism, method, methodology, network, neural activity, neural basis, neural function, normal cognition, novel method, novel paradigms, older adults, one-sample t-test, orbital frontal cortex, paradigm, participants, pathological alterations, postural control task, process, proportional scaling, real walking, recruitment, recruitment of brain regions, region, results, scale, sensory processing, sessions, standing, study, study sessions, supraspinal locomotor network, t-test, task, temporal gyrus, thalamus, tolerance, validity findings, vermis, walking, walking task, white matter, whole-brain, whole-brain differences

Funders

  • Department of Health and Social Care
  • National Institute for Health and Care Research

Data Provider: Digital Science

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