Cerebrospinal fluid sTREM2 in Alzheimer’s disease: comparisons between clinical presentation and AT classification

Knapskog, Anne Brita; Henjum, Kristi; Idland, Ane‐Victoria; Eldholm, Rannveig Sakshaug; Persson, Karin; Saltvedt, Ingvild; Watne, Leiv Otto; Engedal, Knut; Nilsson, Lars

doi:10.1038/s41598-020-72878-8

Cited by 33 publications

(40 citation statements)

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“…Furthermore, its ectodomain is cleaved in the cell surface and shed at the plasma membrane, thus releasing a soluble fragment (sTREM2) which can be measured in the CSF as an indicator of microglial activity [78][79][80]. As it is involved in the regulation of microglia dynamics, and the subsequent amyloid plaque formation and synaptic plasticity, increased levels of sTREM2 within the CSF have been related to a protective response against AD pathology, thus serving as a potential biomarker [80][81][82][83]. On the other hand, YKL-40, the inflammation-related glycoprotein known as chitinase-3-like protein 1, breast regression protein 39, human cartilage glycoprotein 39 or chondrex, belongs to the family of chitinase-like proteins, but lacks the enzymatic activity of chitinases [84,85].…”

Section: Cerebrospinal Fluid Biomarkersmentioning

confidence: 99%

Body Fluid Biomarkers for Alzheimer’s Disease—An Up-To-Date Overview

2020

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Neurodegeneration is a highly complex process which is associated with a variety of molecular mechanisms related to ageing. Among neurodegenerative disorders, Alzheimer’s disease (AD) is the most common, affecting more than 45 million individuals. The underlying mechanisms involve amyloid plaques and neurofibrillary tangles (NFTs) deposition, which will subsequently lead to oxidative stress, chronic neuroinflammation, neuron dysfunction, and neurodegeneration. The current diagnosis methods are still limited in regard to the possibility of the accurate and early detection of the diseases. Therefore, research has shifted towards the identification of novel biomarkers and matrices as biomarker sources, beyond amyloid-β and tau protein levels within the cerebrospinal fluid (CSF), that could improve AD diagnosis. In this context, the aim of this paper is to provide an overview of both conventional and novel biomarkers for AD found within body fluids, including CSF, blood, saliva, urine, tears, and olfactory fluids.

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Section: Cerebrospinal Fluid Biomarkersmentioning

confidence: 99%

Body Fluid Biomarkers for Alzheimer’s Disease—An Up-To-Date Overview

2020

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“…Presence of mixed pathology and the differences in recruitment biases to atypical AD should also be considered when comparisons are made between cohorts in longitudinal outcomes (Dubois et al, 2007;Pillai et al, 2016). It is likely these are some possible reasons behind significant differences in sTREM2 levels reported by prior studies across the AD spectrum (Kleinberger et al, 2014;Gispert et al, 2016b;Henjum et al, 2016;Bekris et al, 2018;Suárez-Calvet et al, 2019;Knapskog et al, 2020).…”

Section: Limitationsmentioning

confidence: 99%

“…Clinical reports regarding cerebrospinal fluid (CSF) levels of sTREM2, a soluble TREM2 protein fragment produced by the cleavage of TREM2, have demonstrated varying levels of this protein in the different stages of AD (Wunderlich et al, 2013 ). Although most studies have shown that CSF sTREM2 is increased in the presence of AD biomarkers, the results are somewhat inconsistent regarding sTREM2 levels in amyloid-positive (A+) and tau-positive (T+) cognitively normal (CN) individuals (Ewers et al, 2019 ; Suárez-Calvet et al, 2019 ), patients with mild cognitive impairment (MCI) (Gispert et al, 2016b ; Henjum et al, 2016 ; Suárez-Calvet et al, 2016b , 2019 ; Ewers et al, 2019 ; Knapskog et al, 2020 ), and those with AD dementia (Gispert et al, 2016b ; Piccio et al, 2016 ; Suárez-Calvet et al, 2016b , 2019 ). Some studies have demonstrated no differences in sTREM2 levels across the AD spectrum (Gispert et al, 2016a ; Henjum et al, 2016 ; Knapskog et al, 2020 ), whereas other research has demonstrated decreased levels of sTREM2 in patients with AD dementia, perhaps partially reflecting the variability in clinical symptoms even within the same stage of AD (Kleinberger et al, 2014 ; Bekris et al, 2018 ).…”

Section: Introductionmentioning

confidence: 99%

“…Although most studies have shown that CSF sTREM2 is increased in the presence of AD biomarkers, the results are somewhat inconsistent regarding sTREM2 levels in amyloid-positive (A+) and tau-positive (T+) cognitively normal (CN) individuals (Ewers et al, 2019 ; Suárez-Calvet et al, 2019 ), patients with mild cognitive impairment (MCI) (Gispert et al, 2016b ; Henjum et al, 2016 ; Suárez-Calvet et al, 2016b , 2019 ; Ewers et al, 2019 ; Knapskog et al, 2020 ), and those with AD dementia (Gispert et al, 2016b ; Piccio et al, 2016 ; Suárez-Calvet et al, 2016b , 2019 ). Some studies have demonstrated no differences in sTREM2 levels across the AD spectrum (Gispert et al, 2016a ; Henjum et al, 2016 ; Knapskog et al, 2020 ), whereas other research has demonstrated decreased levels of sTREM2 in patients with AD dementia, perhaps partially reflecting the variability in clinical symptoms even within the same stage of AD (Kleinberger et al, 2014 ; Bekris et al, 2018 ). However, other studies have found that CSF sTREM2 has a dynamic response in the tracking of AD progression (Suárez-Calvet et al, 2016c , 2019 ; Ma et al, 2020 ), and a study in patients with MCI or AD dementia who had A+ and T+ biomarkers found that higher concentrations of sTREM2 in CSF were associated with reduced memory decline, lower CSF p-tau levels, and hippocampal shrinkage (Ewers et al, 2019 ).…”

Section: Introductionmentioning

confidence: 99%

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Temporal Ordering of Inflammatory Analytes sTNFR2 and sTREM2 in Relation to Alzheimer's Disease Biomarkers and Clinical Outcomes

Pillai

Khrestian

Bena

et al. 2021

Front. Aging Neurosci.

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Inflammatory changes are among the key markers of Alzheimer's disease (AD) related pathological changes. Pro-inflammatory analytes have been related to cognitive decline while others have been related to attenuating neuronal death. Among them, changes in cerebrospinal fluid (CSF) levels of soluble triggering receptor expressed on myeloid cells 2 (sTREM2) and soluble tumor necrosis factor receptor 2 (sTNFR2) have been described as impacting favorable clinical outcomes in AD. We therefore evaluate the effect of CSF sTREM2 and sTNFR2 when taken together on AD biomarkers and longitudinal clinical decline to understand their relative role on impacting AD clinical biomarkers and subsequent clinical outcomes. This longitudinal observational cohort study included 168 amyloid-positive (A+) and p-tau-positive (T+) participants with mild cognitive impairment (MCI) or AD dementia from the Alzheimer's Disease Neuroimaging Initiative (ADNI) with 109 of them having concomitant CSF sTREM2 and sTNFR2 data and 48 A+ T+ participants with MCI from a tertiary memory clinic cohort. An exploratory analysis was performed using data from 86 cognitively normal (CN) participants from ADNI with 72 of them having concomitant CSF AD biomarkers and CSF sTREM2 and sTNFR2 data. General linear models were used to evaluate the effect of sTREM2 and sTNFR2 levels on baseline CSF Aβ42, t-tau, and p-tau, and a linear mixed-effects model was used to assess longitudinal cognitive change after controlling for well-known covariates. Among ADNI A+ T+ MCI and AD dementia participants, CSF sTNFR2 had a stronger association, than CSF sTREM2, with CSF t-tau and p-tau. This was replicated among A+ T+ MCI participants from the memory clinic cohort. On the contrary, among A+ T+ CN participants, CSF sTREM2 explained significant variance in CSF t-tau and p-tau, while CSF sTNFR2 did not. When the effects of CSF sTNFR2 and t-tau on longitudinal cognitive change were taken into account, higher CSF sTREM2 predicted slower cognitive decline in A+ T+ AD dementia participants and faster decline in A+ T+ CN participants. Our results show that given the dynamic changes in sTREM2 and sTNFR2, the clinical impact of these distinct inflammation related biomarkers in tracking AD temporal progression across disease stages are likely to differ.

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“…sTREM2 tem seu nível elevado já na fase présintomática, e foi visto aumento de 18%-23% em indivíduos em estado demencial 41 , porém aparenta ter seu pico na fase prodrômica, o que seria uma limitação para seu uso, complicando o desenvolvimento de um ponto de corte clínico 31,58 . Uma forte associação foi observada entre sTREM2 e a idade, patologia tau, YKL-40 e injuria neuronal, mas pouca ou nenhuma com níveis de Aβ 21,26,28,35,41,58 . No estudo de Henjum et al 27 , entretanto, só foi vista a correlação entre sTREM2, t-tau e p-tau em LCR no grupo de controles saudáveis, e não nos grupos com CCL ou DA, usando um novo ELISA foi desenvolvido para esse estudo.…”

Section: Trem2unclassified

Biomarcadores gliais da doença de Alzheimer

Bittencourt

Müller

2021

CBR

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Introdução: A neuroinflamação associada às células gliais é um elemento importante do processo patológico da doença de Alzheimer (DA). Este estudo apresenta uma revisão dos marcadores gliais quitinase 3-like 1 (YKL-40), do receptor desencadeado expresso nas células mieloides 2 (Triggering receptor expressed on myeloid cells 2 -TREM2), da proteína acídica fibrilar glial (GFAP) e da proteína B S100 ligante de cálcio (S100B). Métodos: Nesta revisão são analisados os marcadores gliais YKL-40, TREM2, GFAP e S100B presentes em sangue e/ou líquido cefalorraquidiano (LCR), a partir de estudos publicados até 2020 nos bancos de dados do PubMed, Medline e Periódicos Capes. Resultados: Foram recuperados 233 documentos, dentre os quais foram incluídos 60. Todos os marcadores se encontram aumentados na DA em LCR -YKL-40 e TREM2 solúvel (sTREM2), já na fase pré-clínica -, e em sangue, e estão correlacionados ao declínio cognitivo. No entanto, nenhum dos marcadores analisados apresentou grande potencial para o diagnóstico diferencial. Além da proteína TREM2 solúvel no LCR, no sangue também se pode identificar alteração nos níveis do RNAm de TREM2. GFAP sanguíneo mostra ser o melhor em distinguir controles de pacientes com Alzheimer. Há evidências de um efeito protetivo da ativação glial em reação ao acúmulo amiloide. Conclusão: Os marcadores gliais no geral têm pouca utilidade para o diagnóstico diferencial, mas podem auxiliar no prognóstico e como biomarcadores inespecíficos para doenças neurodegenerativas.

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Cerebrospinal fluid sTREM2 in Alzheimer’s disease: comparisons between clinical presentation and AT classification

Cited by 33 publications

References 50 publications

Body Fluid Biomarkers for Alzheimer’s Disease—An Up-To-Date Overview

Body Fluid Biomarkers for Alzheimer’s Disease—An Up-To-Date Overview

Temporal Ordering of Inflammatory Analytes sTNFR2 and sTREM2 in Relation to Alzheimer's Disease Biomarkers and Clinical Outcomes

Biomarcadores gliais da doença de Alzheimer

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