Decreased hippocampal translocator protein (18 kDa) expression in alcohol dependence: a [11C]PBR28 PET study

Kalk, Nicola J.; Guo, Qi; Owen, David R.; Cherian, Raquin; Erritzoe, David; Gilmour, Ashley; Ribeiro, A. M. R.; McGonigle, John; Waldman, Adam D.; Matthews, Paul M.; Cavanagh, Jonathan; McInnes, Iain B.; Dar, Karim; Gunn, Roger N.; Rabiner, Eugenii A.; Lingford-Hughes, Anne

doi:10.1038/tp.2016.264

Cited by 59 publications

(57 citation statements)

References 71 publications

(85 reference statements)

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“…However, while a plethora of human and preclinical studies support TSPO as a glial marker, it is important to note that not all studies have detected TSPO upregulation in neuropathologies with a hypothesized inflammatory component. 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).…”

Section: Discussionmentioning

confidence: 89%

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

Albrecht

Forsberg

Sandström

et al. 2019

Brain, Behavior, and Immunity

201

170

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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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Section: Discussionmentioning

confidence: 89%

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

Albrecht

Forsberg

Sandström

et al. 2019

Brain, Behavior, and Immunity

201

170

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“…However, the author’s reported [ 11 C]PBR28 binding was unaffected among those subjects [143]. In the third study, Kalk et al[146] imaged 9 alcohol-dependent subjects approximately three weeks since their last drink (ad libitum cigarette smoking prior to scanning) and healthy controls. This [ 11 C]PBR28 study reported significantly lower TSPO availability (partial-volume corrected V T ) by 19% in the hippocampus relative to age-matched healthy controls, with similar trends in the midbrain, thalamus, ACC, and cerebellum.…”

Section: Resultsmentioning

confidence: 99%

“…This [ 11 C]PBR28 study reported significantly lower TSPO availability (partial-volume corrected V T ) by 19% in the hippocampus relative to age-matched healthy controls, with similar trends in the midbrain, thalamus, ACC, and cerebellum. On average, subjects were imaged 14 days since last benzodiazepine dose, and thus, benzodiazepines were unlikely to alter TSPO availability in this study [146]. …”

Section: Resultsmentioning

confidence: 99%

“…First, preclinical research indicates acute alcohol exposure increases proinflammatory markers systemically [151, 152] and in the brain [153, 154]. Second, human studies of long-term alcohol consumption observe significantly lower TSPO levels [142, 143, 146], which remain lower than controls 3 weeks since last drink [146]. Third, in vivo gray matter volume is lower among alcohol-dependent subjects versus healthy controls [155].…”

Section: Resultsmentioning

confidence: 99%

“…However, no TSPO PET studies of cannabis users were identified. In the case of alcohol, the MRS literature is mixed, while 3 independent TSPO PET studies reported alcohol-dependent individuals reliably exhibited suppressed or impaired neuroimmune system relative to controls [142, 143, 146]. Alcohol’s osmotic effects and/or overlapping resonance with myo- inositol may contribute to the discordant MRS and PET findings.…”

Section: Discussion and Future Directionsmentioning

confidence: 99%

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Imaging Biomarkers of the Neuroimmune System among Substance Use Disorders: A Systematic Review

et al. 2019

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There is tremendous interest in the role of the neuroimmune system and inflammatory processes in substance use disorders (SUDs). Imaging biomarkers of the neuroimmune system in vivo provide a vital translational bridge between preclinical and clinical research. Herein, we examine two imaging techniques that measure putative indices of the neuroimmune system and review their application among SUDs. Positron emission tomography (PET) imaging of 18 kDa translocator protein availability is a marker associated with microglia. Proton magnetic resonance spectroscopy quantification of myo-inositol levels is a putative glial marker found in astrocytes. Neuroinflammatory responses are initiated and maintained by microglia and astrocytes, and thus represent important imaging markers. The goal of this review is to summarize neuroimaging findings from the substance use literature that report data using these markers and discuss possible mechanisms of action. The extant literature indicates abused substances exert diverse and complex neuroimmune effects. Moreover, drug effects may change across addiction stages, i.e. the neuroimmune effects of acute drug administration may differ from chronic use. This burgeoning field has considerable potential to improve our understanding and treatment of SUDs. Future research is needed to determine how targeting the neuroimmune system may improve treatment outcomes.

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Increased transcription of TSPO, HDAC2, and HDAC6 in the amygdala of males with alcohol use disorder

et al. 2020

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Introduction Repeated exposure to high doses of alcohol triggers neuroinflammatory processes that contribute to craving and mood dysfunction in alcohol use disorder (AUD). The upregulation of the translocator protein (TSPO) is considered a biomarker of neuroinflammation, and TSPO ligands have been used as neuroimaging biomarkers of neuroinflammation. Epigenetic mechanisms are also implicated in neuroinflammatory responses to alcohol, and elevated expression of HDAC2 and HDAC6 has been reported in the brain of animals exposed to chronic alcohol. Methods The present study examined the transcriptional regulation of TSPO, HDAC2, and HDAC6 in human postmortem brain tissue from males previously diagnosed with AUD (n = 11) compared to age‐matched nondependent males (n = 13) in four brain regions relevant to AUD: prefrontal cortex (PFC), nucleus accumbens (NAc), hippocampus (HPP), and amygdala (AMY). Results Translocator protein mRNA levels in AMY and PFC and HDAC2 and HDAC6 mRNA levels in AMY were upregulated in AUD compared to controls. In AMY, TSPO mRNA levels were positively associated with HDAC2 and HDAC6 mRNA levels, suggesting a possible regulation of TSPO by HDAC2 and HDAC6 in this brain region. In contrast, there were no group differences for TSPO, HDAC2, and HDAC6 in NAc and HPP. Conclusion Our study is the first to find upregulated TSPO mRNA levels in AMY and PFC in postmortem brains from AUD consistent with neuroinflammation, and in the amygdala, they implicate epigenetic regulation of TSPO by HDAC2 and HDAC6.

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Decreased hippocampal translocator protein (18 kDa) expression in alcohol dependence: a [11C]PBR28 PET study

Cited by 59 publications

References 71 publications

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

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

Imaging Biomarkers of the Neuroimmune System among Substance Use Disorders: A Systematic Review

Increased transcription of TSPO, HDAC2, and HDAC6 in the amygdala of males with alcohol use disorder

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