Csf proteomic alzheimer’s disease-predictive subtypes in cognitively intact amyloid negative individuals

Betty Marije Tijms; Johan Gobom; Charlotte Teunissen; Valerija Dobricic; Magda Tsolaki; Frans Verhey; Julius Popp; Pablo Martinez-Lage; Rik Vandenberghe; Alberto Lleó; José Luís Molinuévo; Sebastiaan Engelborghs; Yvonne Freund-Levi; Lutz Froelich; Lars Bertram; Simon Lovestone; Johannes Streffer; Stephanie Vos; Kaj Blennow; Philip Scheltens; Henrik Zetterberg; Pieter Jelle Visser

doi:https://doi.org/10.3390/proteomes9030036

Csf proteomic alzheimer’s disease-predictive subtypes in cognitively intact amyloid negative individuals

Betty Marije Tijms, Johan Gobom, Charlotte Teunissen, Valerija Dobricic, Magda Tsolaki, Frans Verhey, Julius Popp, Pablo Martinez-Lage, Rik Vandenberghe, Alberto Lleó, José Luís Molinuévo, Sebastiaan Engelborghs, Yvonne Freund-Levi, Lutz Froelich, Lars Bertram, Simon Lovestone, Johannes Streffer, Stephanie Vos, Kaj Blennow, Philip ScheltensHenrik Zetterberg, Pieter Jelle Visser

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

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Abstract

We recently discovered three distinct pathophysiological subtypes in Alzheimer’s disease (AD) using cerebrospinal fluid (CSF) proteomics: one with neuronal hyperplasticity, a second with innate immune system activation, and a third subtype with blood–brain barrier dysfunction. It remains unclear whether AD proteomic subtype profiles are a consequence of amyloid aggregation, or might exist upstream from aggregated amyloid. We studied this question in 127 older individuals with intact cognition and normal AD biomarkers in two independent cohorts (EMIF-AD MBD and ADNI). We clustered 705 proteins measured in CSF that were previously related to AD. We identified in these cognitively intact individuals without AD pathology three subtypes: two subtypes were seen in both cohorts (n = 49 with neuronal hyperplasticity and n = 44 with blood–brain barrier dysfunction), and one only in ADNI (n = 12 with innate immune activation). The proteins specific for these subtypes strongly overlapped with AD subtype protein profiles (overlap coefficients 92%–71%). Longitudinal p181-tau and amyloid β 1–42 (Aβ42) CSF analysis showed that in the hyperplasticity subtype p181-tau increased (β = 2.6 pg/mL per year, p = 0.01) and Aβ42 decreased over time (β = −4.4 pg/mL per year, p = 0.03), in the innate immune activation subtype p181-tau increased (β = 3.1 pg/mL per year, p = 0.01) while in the blood–brain barrier dysfunction subtype Aβ42 decreased (β = −3.7 pg/mL per year, p = 0.009). These findings suggest that AD proteomic subtypes might already manifest in cognitively normal individuals and may predispose for AD before amyloid has reached abnormal levels.

Original language	English
Article number	36
Journal	Proteomes
Volume	9
Issue number	3
DOIs	https://doi.org/10.3390/proteomes9030036
Publication status	Published - 1 Sept 2021

Keywords

Alzheimer’s disease
Amyloid beta
Cerebrospinal fluid proteomics
Cognitive functioning
Risk factors
Tau

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https://doi.org/10.3390/proteomes9030036

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Tijms, B. M., Gobom, J., Teunissen, C., Dobricic, V., Tsolaki, M., Verhey, F., Popp, J., Martinez-Lage, P., Vandenberghe, R., Lleó, A., Molinuévo, J. L., Engelborghs, S., Freund-Levi, Y., Froelich, L., Bertram, L., Lovestone, S., Streffer, J., Vos, S., Blennow, K., ... Visser, P. J. (2021). Csf proteomic alzheimer’s disease-predictive subtypes in cognitively intact amyloid negative individuals. Proteomes, 9(3), Article 36. https://doi.org/10.3390/proteomes9030036

@article{46c6f432defe46aa9198a56abbe6c6ed,

title = "Csf proteomic alzheimer{\textquoteright}s disease-predictive subtypes in cognitively intact amyloid negative individuals",

abstract = "We recently discovered three distinct pathophysiological subtypes in Alzheimer{\textquoteright}s disease (AD) using cerebrospinal fluid (CSF) proteomics: one with neuronal hyperplasticity, a second with innate immune system activation, and a third subtype with blood–brain barrier dysfunction. It remains unclear whether AD proteomic subtype profiles are a consequence of amyloid aggregation, or might exist upstream from aggregated amyloid. We studied this question in 127 older individuals with intact cognition and normal AD biomarkers in two independent cohorts (EMIF-AD MBD and ADNI). We clustered 705 proteins measured in CSF that were previously related to AD. We identified in these cognitively intact individuals without AD pathology three subtypes: two subtypes were seen in both cohorts (n = 49 with neuronal hyperplasticity and n = 44 with blood–brain barrier dysfunction), and one only in ADNI (n = 12 with innate immune activation). The proteins specific for these subtypes strongly overlapped with AD subtype protein profiles (overlap coefficients 92%–71%). Longitudinal p181-tau and amyloid β 1–42 (Aβ42) CSF analysis showed that in the hyperplasticity subtype p181-tau increased (β = 2.6 pg/mL per year, p = 0.01) and Aβ42 decreased over time (β = −4.4 pg/mL per year, p = 0.03), in the innate immune activation subtype p181-tau increased (β = 3.1 pg/mL per year, p = 0.01) while in the blood–brain barrier dysfunction subtype Aβ42 decreased (β = −3.7 pg/mL per year, p = 0.009). These findings suggest that AD proteomic subtypes might already manifest in cognitively normal individuals and may predispose for AD before amyloid has reached abnormal levels.",

keywords = "Alzheimer{\textquoteright}s disease, Amyloid beta, Cerebrospinal fluid proteomics, Cognitive functioning, Risk factors, Tau",

author = "Tijms, {Betty Marije} and Johan Gobom and Charlotte Teunissen and Valerija Dobricic and Magda Tsolaki and Frans Verhey and Julius Popp and Pablo Martinez-Lage and Rik Vandenberghe and Alberto Lle{\'o} and Molinu{\'e}vo, {Jos{\'e} Lu{\'i}s} and Sebastiaan Engelborghs and Yvonne Freund-Levi and Lutz Froelich and Lars Bertram and Simon Lovestone and Johannes Streffer and Stephanie Vos and Kaj Blennow and Philip Scheltens and Henrik Zetterberg and Visser, {Pieter Jelle}",

note = "Funding Information: This research was funded by ZonMW Memorabel Grant programme, grant number #733050824; the Innovative Medicines Initiative Joint undertaking under EMIF grant number #115372; the European Research Council, grant number #681712; the Swedish research council, grant number #201802532; and the Alzheimerfonden, grant number #AF-930934. Statistical analyses were performed at the VUmc Alzheimer Center that is part of the neurodegeneration research program of the Neuroscience Campus Amsterdam. EMIF-AD MBD proteomic analyses were performed at the Department of Psychiatry and Neurochemistry, the Sahlgrenska Academy at the University of Gothenburg, Sweden. The VUmc Alzheimer Center is supported by Stichting Alzheimer Nederland and Stichting VUmc fonds. ADNI data were used for this project of which collection and sharing was funded by the Alzheimer?s Disease Neuroimaging Initiative (ADNI) (National Institutes of Health Grant U01 AG024904) and DOD ADNI (Department of Defense award number W81XWH-12-20012). ADNI is funded by the National Institute on Aging, the National Institute of Biomedical Imaging and Bioengineering, and through generous contributions from the following: AbbVie, Alzheimer?s Association; Alzheimer?s Drug Discovery Foundation; Araclon Biotech; BioClinica, Inc.; Biogen; Bristol-Myers Squibb Company; CereSpir, Inc.; Cogstate; Eisai Inc.; Elan Pharmaceuticals, Inc.; Eli Lilly and Company; EuroImmun; F. Hoffmann-La Roche Ltd. and its affiliated company Genentech, Inc.; Fujirebio; GE Healthcare; IXICO Ltd.; Janssen Alzheimer Immunotherapy Research & Development, LLC.; Johnson & Johnson Pharmaceutical Research & Development LLC.; Lumosity; Lundbeck; Merck & Co., Inc.; Meso Scale Diagnostics, LLC.; NeuroRx Research; Neurotrack Technologies; Novartis Pharmaceuticals Corporation; Pfizer Inc.; Piramal Imaging; Servier; Takeda Pharmaceutical Company; and Transition Therapeutics. The Canadian Institutes of Health Research is providing funds to support ADNI clinical sites in Canada. Private sector contributions are facilitated by the Foundation for the National Institutes of Health (www.fnih.org). The grantee organization is the Northern California Institute for Research and Education, and the study is coordinated by the Alzheimer?s Therapeutic Research Institute at the University of Southern California. ADNI data are disseminated by the Laboratory for Neuro Imaging at the University of Southern California. Conflicts of Interest: H.Z. has served at scientific advisory boards for Alector, Eisai, Denali, Roche Diagnostics, Wave, Samumed, Siemens Healthineers, Pinteon Therapeutics, Nervgen, AZTherapies, and CogRx, has given lectures in symposia sponsored by Cellectricon, Fujirebio, Alzecure, and Biogen, and is a co-founder of Brain Biomarker Solutions in Gothenburg AB (BBS), which is a part of the GU Ventures Incubator Program. The other authors declare no conflict of interest. Publisher Copyright: {\textcopyright} 2021 by the authors. Licensee MDPI, Basel, Switzerland.",

year = "2021",

month = sep,

day = "1",

doi = "https://doi.org/10.3390/proteomes9030036",

language = "English",

volume = "9",

journal = "Proteomes",

issn = "2227-7382",

publisher = "MDPI AG",

number = "3",

}

Tijms, BM, Gobom, J, Teunissen, C, Dobricic, V, Tsolaki, M, Verhey, F, Popp, J, Martinez-Lage, P, Vandenberghe, R, Lleó, A, Molinuévo, JL, Engelborghs, S, Freund-Levi, Y, Froelich, L, Bertram, L, Lovestone, S, Streffer, J, Vos, S, Blennow, K, Scheltens, P, Zetterberg, H & Visser, PJ 2021, 'Csf proteomic alzheimer’s disease-predictive subtypes in cognitively intact amyloid negative individuals', Proteomes, vol. 9, no. 3, 36. https://doi.org/10.3390/proteomes9030036

TY - JOUR

T1 - Csf proteomic alzheimer’s disease-predictive subtypes in cognitively intact amyloid negative individuals

AU - Tijms, Betty Marije

AU - Gobom, Johan

AU - Teunissen, Charlotte

AU - Dobricic, Valerija

AU - Tsolaki, Magda

AU - Verhey, Frans

AU - Popp, Julius

AU - Martinez-Lage, Pablo

AU - Vandenberghe, Rik

AU - Lleó, Alberto

AU - Molinuévo, José Luís

AU - Engelborghs, Sebastiaan

AU - Freund-Levi, Yvonne

AU - Froelich, Lutz

AU - Bertram, Lars

AU - Lovestone, Simon

AU - Streffer, Johannes

AU - Vos, Stephanie

AU - Blennow, Kaj

AU - Scheltens, Philip

AU - Zetterberg, Henrik

AU - Visser, Pieter Jelle

N1 - Funding Information: This research was funded by ZonMW Memorabel Grant programme, grant number #733050824; the Innovative Medicines Initiative Joint undertaking under EMIF grant number #115372; the European Research Council, grant number #681712; the Swedish research council, grant number #201802532; and the Alzheimerfonden, grant number #AF-930934. Statistical analyses were performed at the VUmc Alzheimer Center that is part of the neurodegeneration research program of the Neuroscience Campus Amsterdam. EMIF-AD MBD proteomic analyses were performed at the Department of Psychiatry and Neurochemistry, the Sahlgrenska Academy at the University of Gothenburg, Sweden. The VUmc Alzheimer Center is supported by Stichting Alzheimer Nederland and Stichting VUmc fonds. ADNI data were used for this project of which collection and sharing was funded by the Alzheimer?s Disease Neuroimaging Initiative (ADNI) (National Institutes of Health Grant U01 AG024904) and DOD ADNI (Department of Defense award number W81XWH-12-20012). ADNI is funded by the National Institute on Aging, the National Institute of Biomedical Imaging and Bioengineering, and through generous contributions from the following: AbbVie, Alzheimer?s Association; Alzheimer?s Drug Discovery Foundation; Araclon Biotech; BioClinica, Inc.; Biogen; Bristol-Myers Squibb Company; CereSpir, Inc.; Cogstate; Eisai Inc.; Elan Pharmaceuticals, Inc.; Eli Lilly and Company; EuroImmun; F. Hoffmann-La Roche Ltd. and its affiliated company Genentech, Inc.; Fujirebio; GE Healthcare; IXICO Ltd.; Janssen Alzheimer Immunotherapy Research & Development, LLC.; Johnson & Johnson Pharmaceutical Research & Development LLC.; Lumosity; Lundbeck; Merck & Co., Inc.; Meso Scale Diagnostics, LLC.; NeuroRx Research; Neurotrack Technologies; Novartis Pharmaceuticals Corporation; Pfizer Inc.; Piramal Imaging; Servier; Takeda Pharmaceutical Company; and Transition Therapeutics. The Canadian Institutes of Health Research is providing funds to support ADNI clinical sites in Canada. Private sector contributions are facilitated by the Foundation for the National Institutes of Health (www.fnih.org). The grantee organization is the Northern California Institute for Research and Education, and the study is coordinated by the Alzheimer?s Therapeutic Research Institute at the University of Southern California. ADNI data are disseminated by the Laboratory for Neuro Imaging at the University of Southern California. Conflicts of Interest: H.Z. has served at scientific advisory boards for Alector, Eisai, Denali, Roche Diagnostics, Wave, Samumed, Siemens Healthineers, Pinteon Therapeutics, Nervgen, AZTherapies, and CogRx, has given lectures in symposia sponsored by Cellectricon, Fujirebio, Alzecure, and Biogen, and is a co-founder of Brain Biomarker Solutions in Gothenburg AB (BBS), which is a part of the GU Ventures Incubator Program. The other authors declare no conflict of interest. Publisher Copyright: © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

PY - 2021/9/1

Y1 - 2021/9/1

N2 - We recently discovered three distinct pathophysiological subtypes in Alzheimer’s disease (AD) using cerebrospinal fluid (CSF) proteomics: one with neuronal hyperplasticity, a second with innate immune system activation, and a third subtype with blood–brain barrier dysfunction. It remains unclear whether AD proteomic subtype profiles are a consequence of amyloid aggregation, or might exist upstream from aggregated amyloid. We studied this question in 127 older individuals with intact cognition and normal AD biomarkers in two independent cohorts (EMIF-AD MBD and ADNI). We clustered 705 proteins measured in CSF that were previously related to AD. We identified in these cognitively intact individuals without AD pathology three subtypes: two subtypes were seen in both cohorts (n = 49 with neuronal hyperplasticity and n = 44 with blood–brain barrier dysfunction), and one only in ADNI (n = 12 with innate immune activation). The proteins specific for these subtypes strongly overlapped with AD subtype protein profiles (overlap coefficients 92%–71%). Longitudinal p181-tau and amyloid β 1–42 (Aβ42) CSF analysis showed that in the hyperplasticity subtype p181-tau increased (β = 2.6 pg/mL per year, p = 0.01) and Aβ42 decreased over time (β = −4.4 pg/mL per year, p = 0.03), in the innate immune activation subtype p181-tau increased (β = 3.1 pg/mL per year, p = 0.01) while in the blood–brain barrier dysfunction subtype Aβ42 decreased (β = −3.7 pg/mL per year, p = 0.009). These findings suggest that AD proteomic subtypes might already manifest in cognitively normal individuals and may predispose for AD before amyloid has reached abnormal levels.

AB - We recently discovered three distinct pathophysiological subtypes in Alzheimer’s disease (AD) using cerebrospinal fluid (CSF) proteomics: one with neuronal hyperplasticity, a second with innate immune system activation, and a third subtype with blood–brain barrier dysfunction. It remains unclear whether AD proteomic subtype profiles are a consequence of amyloid aggregation, or might exist upstream from aggregated amyloid. We studied this question in 127 older individuals with intact cognition and normal AD biomarkers in two independent cohorts (EMIF-AD MBD and ADNI). We clustered 705 proteins measured in CSF that were previously related to AD. We identified in these cognitively intact individuals without AD pathology three subtypes: two subtypes were seen in both cohorts (n = 49 with neuronal hyperplasticity and n = 44 with blood–brain barrier dysfunction), and one only in ADNI (n = 12 with innate immune activation). The proteins specific for these subtypes strongly overlapped with AD subtype protein profiles (overlap coefficients 92%–71%). Longitudinal p181-tau and amyloid β 1–42 (Aβ42) CSF analysis showed that in the hyperplasticity subtype p181-tau increased (β = 2.6 pg/mL per year, p = 0.01) and Aβ42 decreased over time (β = −4.4 pg/mL per year, p = 0.03), in the innate immune activation subtype p181-tau increased (β = 3.1 pg/mL per year, p = 0.01) while in the blood–brain barrier dysfunction subtype Aβ42 decreased (β = −3.7 pg/mL per year, p = 0.009). These findings suggest that AD proteomic subtypes might already manifest in cognitively normal individuals and may predispose for AD before amyloid has reached abnormal levels.

KW - Alzheimer’s disease

KW - Amyloid beta

KW - Cerebrospinal fluid proteomics

KW - Cognitive functioning

KW - Risk factors

KW - Tau

UR - http://www.scopus.com/inward/record.url?scp=85112291359&partnerID=8YFLogxK

U2 - https://doi.org/10.3390/proteomes9030036

DO - https://doi.org/10.3390/proteomes9030036

M3 - Article

C2 - 34449748

SN - 2227-7382

VL - 9

JO - Proteomes

JF - Proteomes

IS - 3

M1 - 36

ER -

Csf proteomic alzheimer’s disease-predictive subtypes in cognitively intact amyloid negative individuals

Abstract

Keywords

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