APOE ε4 genotype-dependent cerebrospinal fluid proteomic signatures in Alzheimer's disease

被引：30

作者：

Konijnenberg, Elles ^{[1
]}

Tijms, Betty M. ^{[1
]}

Gobom, Johan ^{[2
,3
]}

Dobricic, Valerija ^{[4
]}

Bos, Isabelle ^{[1
,5
]}

Vos, Stephanie ^{[5
]}

Tsolaki, Magda ^{[6
]}

Verhey, Frans ^{[5
]}

Popp, Julius ^{[7
]}

Martinez-Lage, Pablo ^{[8
]}

Vandenberghe, Rik ^{[9
]}

Lleo, Alberto ^{[10
]}

Froelich, Lutz ^{[11
]}

Lovestone, Simon ^{[12
,13
]}

Streffer, Johannes ^{[14
,15
]}

Bertram, Lars ^{[4
,16
,17
]}

Blennow, Kaj ^{[18
,19
]}

Teunissen, Charlotte E. ^{[20
,21
]}

Veerhuis, Robert ^{[20
,21
,22
]}

Smit, August B. ^{[23
]}

Scheltens, Philip ^{[1
]}

Zetterberg, Henrik ^{[19
,20
,21
,24
,25
]}

Visser, Pieter Jelle ^{[1
,5
,26
]}

机构：

[1] Vrije Univ Amsterdam, Alzheimer Ctr Amsterdam, Dept Neurol, Amsterdam Neurosci,Amsterdam UMC, POB 7057, NL-1007 MB Amsterdam, Netherlands

[2] Sahlgrens Univ Hosp, Clin Neurochem Lab, Molndal, Sweden

[3] Univ Gothenburg, Inst Neurosci & Physiol, Dept Psychiat & Neurochem, Sahlgrenska Acad, Molndal, Sweden

[4] Univ Lubeck, Lubeck Interdisciplinary Platform Genome Analyt, Lubeck, Germany

[5] Maastricht Univ, Alzheimer Ctr Limburg, Sch Mental Hlth & Neurosci, Dept Psychiat & Neuropsychol, Maastricht, Netherlands

[6] AHEPA Univ Hosp, Dept Neurol 1, Macedonia Greece, Thessaloniki, Greece

[7] Univ Hosp Lausanne, Dept Psychiat, Lausanne, Switzerland

[8] CITA Alzheimer Fdn, Ctr Res & Adv Therapies, Dept Neurol, San Sebastian, Spain

[9] Univ Hosp Leuven, Leuven, Belgium

[10] Hosp Santa Creu & Sant Pau, Barcelona, Spain

[11] Heidelberg Univ, Zentralinst Seel Gesundheit, Dept Geriatr Psychiat, Mannheim, Germany

[12] Univ Oxford, Dept Psychiat, Oxford, England

[13] Janssen R&D, Beerse, Belgium

[14] UCB Biopharma SPRL, Early Clin Neurol, Braine Lalleud, Belgium

[15] Janssen R&D LLC, Beerse, Belgium

[16] Imperial Coll London, Sch Publ Hlth, London, England

[17] Univ Oslo, Dept Psychol, Oslo, Norway

[18] Sahlgrens Univ Hosp, Inst Neurosci & Physiol, Clin Neurochem Lab, Molndal, Sweden

[19] Univ Gothenburg, Inst Neurosci & Physiol, Dept Psychiat & Neurochem, Molndal, Sweden

[20] Vrije Univ Amsterdam, Dept Clin Chem, Amsterdam UMC, Neurochem Lab, Amsterdam, Netherlands

[21] Vrije Univ Amsterdam, Dept Clin Chem, Amsterdam UMC, Biobank, Amsterdam, Netherlands

[22] Vrije Univ Amsterdam, Dept Psychiat, Amsterdam UMC, Amsterdam, Netherlands

[23] Vrije Univ Amsterdam, Ctr Neurogen & Cognit Res, Dept Mol & Cellular Neurobiol, Amsterdam, Netherlands

[24] UCL Inst Neurol, Dept Mol Neurosci, London, England

[25] UK Dementia Res Inst, London, England

[26] Karolinska Inst, Div Neurogeriatr, Dept Neurobiol Care Sci & Soc, Stockholm, Sweden

来源：

ALZHEIMERS RESEARCH & THERAPY | 2020年 / 12卷 / 01期

关键词：

Amyloid aggregation; APOE genotype; CSF proteomics; APOLIPOPROTEIN E4; POSTERIOR CINGULATE; BIOMARKERS; COMPLEMENT; PREVALENCE; DEMENTIA; ALLELE; INFLAMMATION; ASSOCIATION; MICROGLIA;

D O I：

10.1186/s13195-020-00628-z

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Background Aggregation of amyloid beta into plaques in the brain is one of the earliest pathological events in Alzheimer's disease (AD). The exact pathophysiology leading to dementia is still uncertain, but the apolipoprotein E (APOE) epsilon 4 genotype plays a major role. We aimed to identify the molecular pathways associated with amyloid beta aggregation using cerebrospinal fluid (CSF) proteomics and to study the potential modifying effects of APOE epsilon 4 genotype. Methods We tested 243 proteins and protein fragments in CSF comparing 193 subjects with AD across the cognitive spectrum (65% APOE epsilon 4 carriers, average age 75 +/- 7 years) against 60 controls with normal CSF amyloid beta, normal cognition, and no APOE epsilon 4 allele (average age 75 +/- 6 years). Results One hundred twenty-nine proteins (53%) were associated with aggregated amyloid beta. APOE epsilon 4 carriers with AD showed altered concentrations of proteins involved in the complement pathway and glycolysis when cognition was normal and lower concentrations of proteins involved in synapse structure and function when cognitive impairment was moderately severe. APOE epsilon 4 non-carriers with AD showed lower expression of proteins involved in synapse structure and function when cognition was normal and lower concentrations of proteins that were associated with complement and other inflammatory processes when cognitive impairment was mild. Repeating analyses for 114 proteins that were available in an independent EMIF-AD MBD dataset (n = 275) showed that 80% of the proteins showed group differences in a similar direction, but overall, 28% effects reached statistical significance (ranging between 6 and 87% depending on the disease stage and genotype), suggesting variable reproducibility. Conclusions These results imply that AD pathophysiology depends on APOE genotype and that treatment for AD may need to be tailored according to APOE genotype and severity of the cognitive impairment.

引用

页数：11

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