Longitudinal cerebrospinal fluid measurements show glial hypo- and hyperactivation in predementia Alzheimer's disease

Kaja Nordengen; Bjørn-Eivind Kirsebom; Grit Richter; Lene Pålhaugen; Berglind Gísladóttir; Nikias Siafarikas; Arne Nakling; Arvid Rongve; Geir Bråthen; Gøril Rolfseng Grøntvedt; Fernando Gonzalez; Knut Waterloo; Kulbhushan Sharma; Thomas Karikari; Eleonora M Vromen; Betty M Tijms; Pieter J Visser; Per Selnes; Milicia G Kramberger; Bengt Winblad; Kaj Blennow; Tormod Fladby

doi:https://doi.org/10.1186/s12974-023-02973-w

Longitudinal cerebrospinal fluid measurements show glial hypo- and hyperactivation in predementia Alzheimer's disease

Kaja Nordengen, Bjørn-Eivind Kirsebom, Grit Richter, Lene Pålhaugen, Berglind Gísladóttir, Nikias Siafarikas, Arne Nakling, Arvid Rongve, Geir Bråthen, Gøril Rolfseng Grøntvedt, Fernando Gonzalez, Knut Waterloo, Kulbhushan Sharma, Thomas Karikari, Eleonora M Vromen, Betty M Tijms, Pieter J Visser, Per Selnes, Milicia G Kramberger, Bengt WinbladKaj Blennow, Tormod Fladby

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Background: Brain innate immune activation is associated with Alzheimer’s disease (AD), but degrees of activation may vary between disease stages. Thus, brain innate immune activation must be assessed in longitudinal clinical studies that include biomarker negative healthy controls and cases with established AD pathology. Here, we employ longitudinally sampled cerebrospinal fluid (CSF) core AD, immune activation and glial biomarkers to investigate early (predementia stage) innate immune activation levels and biomarker profiles. Methods: We included non-demented cases from a longitudinal observational cohort study, with CSF samples available at baseline (n = 535) and follow-up (n = 213), between 1 and 6 years from baseline (mean 2.8 years). We measured Aβ42/40 ratio, p-tau181, and total-tau to determine Ab (A+), tau-tangle pathology (T+), and neurodegeneration (N+), respectively. We classified individuals into these groups: A−/T−/N−, A+/T−/N−, A+/T+ or N+, or A−/T+ or N+. Using linear and mixed linear regression, we compared levels of CSF sTREM2, YKL-40, clusterin, fractalkine, MCP-1, IL-6, IL-1, IL-18, and IFN-γ both cross-sectionally and longitudinally between groups. A post hoc analysis was also performed to assess biomarker differences between cognitively healthy and impaired individuals in the A+/T+ or N+ group. Results: Cross-sectionally, CSF sTREM2, YKL-40, clusterin and fractalkine were higher only in groups with tau pathology, independent of amyloidosis (p < 0.001, A+/T+ or N+ and A−/T+ or N+, compared to A−/T−/N−). No significant group differences were observed for the cytokines CSF MCP-1, IL-6, IL-10, IL18 or IFN-γ. Longitudinally, CSF YKL-40, fractalkine and IFN-γ were all significantly lower in stable A+/T−/N− cases (all p < 0.05). CSF sTREM2, YKL-40, clusterin, fractalkine (p < 0.001) and MCP-1 (p < 0.05) were all higher in T or N+, with or without amyloidosis at baseline, but remained stable over time. High CSF sTREM2 was associated with preserved cognitive function within the A+/T+ or N+ group, relative to the cognitively impaired with the same A/T/N biomarker profile (p < 0.01). Conclusions: Immune hypoactivation and reduced neuron–microglia communication are observed in isolated amyloidosis while activation and increased fractalkine accompanies tau pathology in predementia AD. Glial hypo- and hyperactivation through the predementia AD continuum suggests altered glial interaction with Ab and tau pathology, and may necessitate differential treatments, depending on the stage and patient-specific activation patterns.

Original language	English
Article number	298
Pages (from-to)	298
Journal	Journal of neuroinflammation
Volume	20
Issue number	1
DOIs	https://doi.org/10.1186/s12974-023-02973-w
Publication status	Published - 13 Dec 2023

Keywords

Alzheimer’s disease
Biomarkers
Cerebrospinal fluid
Inflammation

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https://doi.org/10.1186/s12974-023-02973-w

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Nordengen, K., Kirsebom, B.-E., Richter, G., Pålhaugen, L., Gísladóttir, B., Siafarikas, N., Nakling, A., Rongve, A., Bråthen, G., Grøntvedt, G. R., Gonzalez, F., Waterloo, K., Sharma, K., Karikari, T., Vromen, E. M., Tijms, B. M., Visser, P. J., Selnes, P., Kramberger, M. G., ... Fladby, T. (2023). Longitudinal cerebrospinal fluid measurements show glial hypo- and hyperactivation in predementia Alzheimer's disease. Journal of neuroinflammation, 20(1), 298. Article 298. https://doi.org/10.1186/s12974-023-02973-w

@article{05444366face49fa935b5e080b4757ec,

title = "Longitudinal cerebrospinal fluid measurements show glial hypo- and hyperactivation in predementia Alzheimer's disease",

abstract = "Background: Brain innate immune activation is associated with Alzheimer{\textquoteright}s disease (AD), but degrees of activation may vary between disease stages. Thus, brain innate immune activation must be assessed in longitudinal clinical studies that include biomarker negative healthy controls and cases with established AD pathology. Here, we employ longitudinally sampled cerebrospinal fluid (CSF) core AD, immune activation and glial biomarkers to investigate early (predementia stage) innate immune activation levels and biomarker profiles. Methods: We included non-demented cases from a longitudinal observational cohort study, with CSF samples available at baseline (n = 535) and follow-up (n = 213), between 1 and 6 years from baseline (mean 2.8 years). We measured Aβ42/40 ratio, p-tau181, and total-tau to determine Ab (A+), tau-tangle pathology (T+), and neurodegeneration (N+), respectively. We classified individuals into these groups: A−/T−/N−, A+/T−/N−, A+/T+ or N+, or A−/T+ or N+. Using linear and mixed linear regression, we compared levels of CSF sTREM2, YKL-40, clusterin, fractalkine, MCP-1, IL-6, IL-1, IL-18, and IFN-γ both cross-sectionally and longitudinally between groups. A post hoc analysis was also performed to assess biomarker differences between cognitively healthy and impaired individuals in the A+/T+ or N+ group. Results: Cross-sectionally, CSF sTREM2, YKL-40, clusterin and fractalkine were higher only in groups with tau pathology, independent of amyloidosis (p < 0.001, A+/T+ or N+ and A−/T+ or N+, compared to A−/T−/N−). No significant group differences were observed for the cytokines CSF MCP-1, IL-6, IL-10, IL18 or IFN-γ. Longitudinally, CSF YKL-40, fractalkine and IFN-γ were all significantly lower in stable A+/T−/N− cases (all p < 0.05). CSF sTREM2, YKL-40, clusterin, fractalkine (p < 0.001) and MCP-1 (p < 0.05) were all higher in T or N+, with or without amyloidosis at baseline, but remained stable over time. High CSF sTREM2 was associated with preserved cognitive function within the A+/T+ or N+ group, relative to the cognitively impaired with the same A/T/N biomarker profile (p < 0.01). Conclusions: Immune hypoactivation and reduced neuron–microglia communication are observed in isolated amyloidosis while activation and increased fractalkine accompanies tau pathology in predementia AD. Glial hypo- and hyperactivation through the predementia AD continuum suggests altered glial interaction with Ab and tau pathology, and may necessitate differential treatments, depending on the stage and patient-specific activation patterns.",

keywords = "Alzheimer{\textquoteright}s disease, Biomarkers, Cerebrospinal fluid, Inflammation",

author = "Kaja Nordengen and Bj{\o}rn-Eivind Kirsebom and Grit Richter and Lene P{\aa}lhaugen and Berglind G{\'i}slad{\'o}ttir and Nikias Siafarikas and Arne Nakling and Arvid Rongve and Geir Br{\aa}then and Gr{\o}ntvedt, {G{\o}ril Rolfseng} and Fernando Gonzalez and Knut Waterloo and Kulbhushan Sharma and Thomas Karikari and Vromen, {Eleonora M} and Tijms, {Betty M} and Visser, {Pieter J} and Per Selnes and Kramberger, {Milicia G} and Bengt Winblad and Kaj Blennow and Tormod Fladby",

note = "Funding Information: We thank Erna Utnes and Marianne Wettergreen (Akershus University hospital, Norway) for assistance with data collection and analysis. Funding Information: The project was funded by the Norwegian Research council, JPND/PMI-AD (NRC 311993) and from the regional health authorities (Helse S{\o}r-{\O}st and Helse Nord [HNF1540-20]). Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = dec,

day = "13",

doi = "https://doi.org/10.1186/s12974-023-02973-w",

language = "English",

volume = "20",

pages = "298",

journal = "Journal of neuroinflammation",

issn = "1742-2094",

publisher = "BioMed Central",

number = "1",

}

Nordengen, K, Kirsebom, B-E, Richter, G, Pålhaugen, L, Gísladóttir, B, Siafarikas, N, Nakling, A, Rongve, A, Bråthen, G, Grøntvedt, GR, Gonzalez, F, Waterloo, K, Sharma, K, Karikari, T, Vromen, EM , Tijms, BM , Visser, PJ, Selnes, P, Kramberger, MG, Winblad, B, Blennow, K & Fladby, T 2023, 'Longitudinal cerebrospinal fluid measurements show glial hypo- and hyperactivation in predementia Alzheimer's disease', Journal of neuroinflammation, vol. 20, no. 1, 298, pp. 298. https://doi.org/10.1186/s12974-023-02973-w

TY - JOUR

T1 - Longitudinal cerebrospinal fluid measurements show glial hypo- and hyperactivation in predementia Alzheimer's disease

AU - Nordengen, Kaja

AU - Kirsebom, Bjørn-Eivind

AU - Richter, Grit

AU - Pålhaugen, Lene

AU - Gísladóttir, Berglind

AU - Siafarikas, Nikias

AU - Nakling, Arne

AU - Rongve, Arvid

AU - Bråthen, Geir

AU - Grøntvedt, Gøril Rolfseng

AU - Gonzalez, Fernando

AU - Waterloo, Knut

AU - Sharma, Kulbhushan

AU - Karikari, Thomas

AU - Vromen, Eleonora M

AU - Tijms, Betty M

AU - Visser, Pieter J

AU - Selnes, Per

AU - Kramberger, Milicia G

AU - Winblad, Bengt

AU - Blennow, Kaj

AU - Fladby, Tormod

N1 - Funding Information: We thank Erna Utnes and Marianne Wettergreen (Akershus University hospital, Norway) for assistance with data collection and analysis. Funding Information: The project was funded by the Norwegian Research council, JPND/PMI-AD (NRC 311993) and from the regional health authorities (Helse Sør-Øst and Helse Nord [HNF1540-20]). Publisher Copyright: © 2023, The Author(s).

PY - 2023/12/13

Y1 - 2023/12/13

N2 - Background: Brain innate immune activation is associated with Alzheimer’s disease (AD), but degrees of activation may vary between disease stages. Thus, brain innate immune activation must be assessed in longitudinal clinical studies that include biomarker negative healthy controls and cases with established AD pathology. Here, we employ longitudinally sampled cerebrospinal fluid (CSF) core AD, immune activation and glial biomarkers to investigate early (predementia stage) innate immune activation levels and biomarker profiles. Methods: We included non-demented cases from a longitudinal observational cohort study, with CSF samples available at baseline (n = 535) and follow-up (n = 213), between 1 and 6 years from baseline (mean 2.8 years). We measured Aβ42/40 ratio, p-tau181, and total-tau to determine Ab (A+), tau-tangle pathology (T+), and neurodegeneration (N+), respectively. We classified individuals into these groups: A−/T−/N−, A+/T−/N−, A+/T+ or N+, or A−/T+ or N+. Using linear and mixed linear regression, we compared levels of CSF sTREM2, YKL-40, clusterin, fractalkine, MCP-1, IL-6, IL-1, IL-18, and IFN-γ both cross-sectionally and longitudinally between groups. A post hoc analysis was also performed to assess biomarker differences between cognitively healthy and impaired individuals in the A+/T+ or N+ group. Results: Cross-sectionally, CSF sTREM2, YKL-40, clusterin and fractalkine were higher only in groups with tau pathology, independent of amyloidosis (p < 0.001, A+/T+ or N+ and A−/T+ or N+, compared to A−/T−/N−). No significant group differences were observed for the cytokines CSF MCP-1, IL-6, IL-10, IL18 or IFN-γ. Longitudinally, CSF YKL-40, fractalkine and IFN-γ were all significantly lower in stable A+/T−/N− cases (all p < 0.05). CSF sTREM2, YKL-40, clusterin, fractalkine (p < 0.001) and MCP-1 (p < 0.05) were all higher in T or N+, with or without amyloidosis at baseline, but remained stable over time. High CSF sTREM2 was associated with preserved cognitive function within the A+/T+ or N+ group, relative to the cognitively impaired with the same A/T/N biomarker profile (p < 0.01). Conclusions: Immune hypoactivation and reduced neuron–microglia communication are observed in isolated amyloidosis while activation and increased fractalkine accompanies tau pathology in predementia AD. Glial hypo- and hyperactivation through the predementia AD continuum suggests altered glial interaction with Ab and tau pathology, and may necessitate differential treatments, depending on the stage and patient-specific activation patterns.

AB - Background: Brain innate immune activation is associated with Alzheimer’s disease (AD), but degrees of activation may vary between disease stages. Thus, brain innate immune activation must be assessed in longitudinal clinical studies that include biomarker negative healthy controls and cases with established AD pathology. Here, we employ longitudinally sampled cerebrospinal fluid (CSF) core AD, immune activation and glial biomarkers to investigate early (predementia stage) innate immune activation levels and biomarker profiles. Methods: We included non-demented cases from a longitudinal observational cohort study, with CSF samples available at baseline (n = 535) and follow-up (n = 213), between 1 and 6 years from baseline (mean 2.8 years). We measured Aβ42/40 ratio, p-tau181, and total-tau to determine Ab (A+), tau-tangle pathology (T+), and neurodegeneration (N+), respectively. We classified individuals into these groups: A−/T−/N−, A+/T−/N−, A+/T+ or N+, or A−/T+ or N+. Using linear and mixed linear regression, we compared levels of CSF sTREM2, YKL-40, clusterin, fractalkine, MCP-1, IL-6, IL-1, IL-18, and IFN-γ both cross-sectionally and longitudinally between groups. A post hoc analysis was also performed to assess biomarker differences between cognitively healthy and impaired individuals in the A+/T+ or N+ group. Results: Cross-sectionally, CSF sTREM2, YKL-40, clusterin and fractalkine were higher only in groups with tau pathology, independent of amyloidosis (p < 0.001, A+/T+ or N+ and A−/T+ or N+, compared to A−/T−/N−). No significant group differences were observed for the cytokines CSF MCP-1, IL-6, IL-10, IL18 or IFN-γ. Longitudinally, CSF YKL-40, fractalkine and IFN-γ were all significantly lower in stable A+/T−/N− cases (all p < 0.05). CSF sTREM2, YKL-40, clusterin, fractalkine (p < 0.001) and MCP-1 (p < 0.05) were all higher in T or N+, with or without amyloidosis at baseline, but remained stable over time. High CSF sTREM2 was associated with preserved cognitive function within the A+/T+ or N+ group, relative to the cognitively impaired with the same A/T/N biomarker profile (p < 0.01). Conclusions: Immune hypoactivation and reduced neuron–microglia communication are observed in isolated amyloidosis while activation and increased fractalkine accompanies tau pathology in predementia AD. Glial hypo- and hyperactivation through the predementia AD continuum suggests altered glial interaction with Ab and tau pathology, and may necessitate differential treatments, depending on the stage and patient-specific activation patterns.

KW - Alzheimer’s disease

KW - Biomarkers

KW - Cerebrospinal fluid

KW - Inflammation

UR - http://www.scopus.com/inward/record.url?scp=85179690022&partnerID=8YFLogxK

U2 - https://doi.org/10.1186/s12974-023-02973-w

DO - https://doi.org/10.1186/s12974-023-02973-w

M3 - Article

C2 - 38093257

SN - 1742-2094

VL - 20

SP - 298

JO - Journal of neuroinflammation

JF - Journal of neuroinflammation

IS - 1

M1 - 298

ER -

Longitudinal cerebrospinal fluid measurements show glial hypo- and hyperactivation in predementia Alzheimer's disease

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