Positron Emission Tomography Studies of the Glial Cell Marker Translocator Protein in Patients With Psychosis: A Meta-analysis Using Individual Participant Data

Plavén-Sigray, Pontus; Matheson, Granville J.; Collste, Karin; Ashok, Abhishekh Hulegar; Coughlin, Jennifer M.; Howes, Oliver; Mizrahi, Romina; Pomper, Martin G.; Rusjan, Pablo; Veronese, Mattia; Wang, Yuchuan; Červenka, Simon

doi:10.1016/j.biopsych.2018.02.1171

Cited by 106 publications

(109 citation statements)

References 69 publications

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“…These results in total suggest largely unique differentially expressed genes and processes associated with schizophrenia in the HIPPO compared with DLPFC and underscore the incompleteness of the molecular pathology associated with schizophrenia based on only DLPFC or HIPPO. The enrichment of immune processes in genes relatively decreased in expression in schizophrenia echoes several recent studies that have not confirmed earlier proposals of an upregulated immune response in the brain of patients with this illness (Birnbaum et al, 2018;Plavén-Sigray et al, 2018) .…”

Section: Developmental Differences In Expression Between Brain Regionssupporting

confidence: 54%

Regional heterogeneity in gene expression, regulation and coherence in hippocampus and dorsolateral prefrontal cortex across development and in schizophrenia

Collado‐Torres

Burke

Peterson

et al. 2018

Preprint

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Recent large-scale genomics efforts have better characterized the molecular correlates of schizophrenia in postmortem human neocortex, but not hippocampus which is a brain region prominently implicated in its pathogenesis. Here in the second phase of the BrainSeq Consortium (Phase II), we have generated RiboZero RNA-seq data for 900 samples across both the dorsolateral prefrontal cortex (DLPFC) and the hippocampus (HIPPO) for 551 individuals (286 affected by schizophrenia disorder: SCZD). We identify substantial regional differences in gene expression, in both pre-and post-natal life, and find widespread differences in how genes are regulated across development. By extending quality surrogate variable analysis (qSVA) to multiple brain regions, we identified 48 and 245 differentially expressed genes (DEG) by SCZD diagnosis (FDR<5%) in HIPPO and DLPFC, respectively, with surprisingly minimal overlap in DEG between the two brain regions. We further identified 205,618 brain region-dependent eQTLs (FDR<1%) and found that 124 GWAS risk loci contain eQTLs in at least one of the regions. We also identify potential molecular correlates of in vivo evidence of altered prefrontal-hippocampal functional coherence in schizophrenia. These results underscore the complexity and regional heterogeneity of the transcriptional correlates of schizophrenia, and suggest future schizophrenia therapeutics may need to target molecular pathologies localized to specific brain regions. Main text

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Section: Developmental Differences In Expression Between Brain Regionssupporting

confidence: 54%

Regional heterogeneity in gene expression, regulation and coherence in hippocampus and dorsolateral prefrontal cortex across development and in schizophrenia

Collado‐Torres

Burke

Peterson

et al. 2018

Preprint

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“…A recent study, however, reported a significantly lower TSPO expression in first-episode psychosis as compared to healthy volunteer using [ 11 C]PBR28 16 . Supporting this, a recent meta-analysis of PET studies with second-generation radioligands in psychosis suggests an overall reduction of TSPO expression in psychosis 22 .…”

Section: Discussionmentioning

confidence: 84%

“…Also, in the study by Holmes and colleagues, increase in TSPO expression was only observed in medicated schizophrenia, not in drug-naïve patients 18 . It is noteworthy that a recent meta-analysis of individual data of previous PET studies with second-generation radioligands in psychosis suggests an overall reduction of TSPO expression in psychosis 22 .…”

Section: Introductionmentioning

confidence: 99%

TSPO expression and brain structure in the psychosis spectrum

Hafizi

Guma

Koppel

et al. 2018

Brain, Behavior, and Immunity

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Psychosis is associated with abnormal structural changes in the brain including decreased regional brain volumes and abnormal brain morphology. However, the underlying causes of these structural abnormalities are less understood. The immune system, including microglial activation, has been implicated in the pathophysiology of psychosis. Although previous studies have suggested a connection between peripheral proinflammatory cytokines and structural brain abnormalities in schizophrenia, no in-vivo studies have investigated whether microglial activation is also linked to brain structure alterations previously observed in schizophrenia and its putative prodrome. In this study, we investigated the link between mitochondrial 18 kDa translocator protein (TSPO) and structural brain characteristics (i.e. regional brain volume, cortical thickness, and hippocampal shape) in key brain regions such as dorsolateral prefrontal cortex and hippocampus of a large group of participants (N = 90) including individuals at clinical high risk (CHR) for psychosis, first-episode psychosis (mostly antipsychotic-naïve) patients, and healthy volunteers. The participants underwent structural brain MRI scan and [F]FEPPA positron emission tomography (PET) targeting TSPO. A significant [F]FEPPA binding-by-group interaction was observed in morphological measures across the left hippocampus. In first-episode psychosis, we observed associations between [F]FEPPA V (total volume of distribution) and outward and inward morphological alterations, respectively, in the dorsal and ventro-medial portions of the left hippocampus. These associations were not significant in CHR or healthy volunteers. There was no association between [F]FEPPA V and other structural brain characteristics. Our findings suggest a link between TSPO expression and alterations in hippocampal morphology in first-episode psychosis.

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“…For instance, previous work showed no differences in TSPO PET signal in cocaine dependence (Narendran et al, 2014), and decreased signal in alcohol dependence (Hillmer et al, 2017; Kalk et al, 2017). In patients with psychosis, initial studies with first generation TSPO tracers showed an increase, whereas recent studies using second-generation radioligands are supportive of a decrease in TSPO levels (Plaven-Sigray et al, 2018). Thus, further work is needed to better assess the potential usefulness of TSPO as a means to image neuroinflammation, and the meaning of the observed TSPO signal changes, particularly in certain pathologies.…”

Section: Discussionmentioning

confidence: 99%

Brain glial activation in fibromyalgia – A multi-site positron emission tomography investigation

Albrecht

Forsberg

Sandström

et al. 2019

Brain, Behavior, and Immunity

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Fibromyalgia (FM) is a poorly understood chronic condition characterized by widespread musculoskeletal pain, fatigue, and cognitive difficulties. While mounting evidence suggests a role for neuroinflammation, no study has directly provided evidence of brain glial activation in FM. In this study, we conducted a Positron Emission Tomography (PET) study using [C]PBR28, which binds to the translocator protein (TSPO), a protein upregulated in activated microglia and astrocytes. To enhance statistical power and generalizability, we combined datasets collected independently at two separate institutions (Massachusetts General Hospital [MGH] and Karolinska Institutet [KI]). In an attempt to disentangle the contributions of different glial cell types to FM, a smaller sample was scanned at KI with [C]--deprenyl-D PET, thought to primarily reflect astrocytic (but not microglial) signal. Thirty-one FM patients and 27 healthy controls (HC) were examined using [C]PBR28 PET. 11 FM patients and 11 HC were scanned using [C]--deprenyl-D PET. Standardized uptake values normalized by occipital cortex signal (SUVR) and distribution volume (V) were computed from the [C]PBR28 data. [C]--deprenyl-D was quantified using λ k. PET imaging metrics were compared across groups, and when differing across groups, against clinical variables. Compared to HC, FM patients demonstrated widespread cortical elevations, and no decreases, in [C]PBR28 V and SUVR, most pronounced in the medial and lateral walls of the frontal and parietal lobes. No regions showed significant group differences in [C]--deprenyl-D signal, including those demonstrating elevated [C]PBR28 signal in patients (p's ≥ 0.53, uncorrected). The elevations in [C]PBR28 V and SUVR were correlated both spatially (i.e., were observed in overlapping regions) and, in several areas, also in terms of magnitude. In exploratory, uncorrected analyses, higher subjective ratings of fatigue in FM patients were associated with higher [C]PBR28 SUVR in the anterior and posterior middle cingulate cortices (p's < 0.03). SUVR was not significantly associated with any other clinical variable. Our work provides the first in vivo evidence supporting a role for glial activation in FM pathophysiology. Given that the elevations in [C]PBR28 signal were not also accompanied by increased [C]--deprenyl-D signal, our data suggests that microglia, but not astrocytes, may be driving the TSPO elevation in these regions. Although [C]--deprenyl-D signal was not found to be increased in FM patients, larger studies are needed to further assess the role of possible astrocytic contributions in FM. Overall, our data support glial modulation as a potential therapeutic strategy for FM.

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Positron Emission Tomography Studies of the Glial Cell Marker Translocator Protein in Patients With Psychosis: A Meta-analysis Using Individual Participant Data

Cited by 106 publications

References 69 publications

Regional heterogeneity in gene expression, regulation and coherence in hippocampus and dorsolateral prefrontal cortex across development and in schizophrenia

Regional heterogeneity in gene expression, regulation and coherence in hippocampus and dorsolateral prefrontal cortex across development and in schizophrenia

TSPO expression and brain structure in the psychosis spectrum

Brain glial activation in fibromyalgia – A multi-site positron emission tomography investigation

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