Cerebrospinal Fluid BACE1 Activity and sAβPPβ as Biomarker Candidates of Alzheimer’s Disease

Alexopoulos, Panagiotis; Thierjung, Nathalie; Grimmer, Timo; Ortner, Marion; Economou, Polychronis; Assimakopoulos, Konstantinos; Gourzis, Philippos; Politis, Antonios; Perneczky, Robert

doi:10.1159/000488481

Cited by 17 publications

(17 citation statements)

References 49 publications

(60 reference statements)

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“…Although it might be challenging to establish from post-mortem tissue whether a specific change is a late or early event or an epiphenomenon in disease pathogenesis 24 , Cole et al showed that BACE1 elevation was correlated with amyloid pathology in mouse models both in the absence (model: Tg2576) and presence (5XFAD) of significant neuronal loss 24,25 . In agreement with an early involvement of BACE1 in LOAD, enzyme activity was found to be higher in CSF and plasma of MCI converters compared to non-converters 16,18,26 .…”

Section: Discussionsupporting

confidence: 78%

Increased blood BACE1 activity as a potential common pathogenic factor of vascular dementia and late onset Alzheimer's disease

Zuliani

Trentini

Rosta

et al. 2020

Sci Rep

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Late onset Alzheimer disease (LOAD) is traditionally considered as a separate disease from vascular dementia (VAD). However, growing evidence suggests that β-amyloid (Aβ) accumulation, that initiates LOAD-related neurodegeneration, is preceded by vascular events. Previous in vitro studies showed that β-secretase 1 (BACE1), the key-enzyme of amyloidogenesis, is upregulated by cerebrovascular insult; moreover, its activity is increased both in brain and serum of LOAD patients. We aimed to investigate whether BACE1 serum activity is altered also in dementias related, or not, to cerebrovascular disease. Thus, we evaluated serum BACE1 activity in a sample of individuals, including patients with LOAD (n. 175), VAD (n. 40), MIXED (LOAD/VAD) dementia (n. 123), other types of dementia (n. 56), and healthy Controls (n. 204). We found that BACE1 was significantly higher not only in LOAD (+ 30%), but also in VAD (+ 35%) and MIXED dementia (+ 22%) (p < 0.001 for all), but not in the other types of dementia (+ 10%). Diagnostic accuracy was 77% for LOAD, 83% for VAD, and 77% for MIXED dementia. In conclusion, we showed for the first time that the increase in peripheral BACE1 activity is a common feature of LOAD and VAD, thus underlying a further pathogenic link between these two forms of dementia.

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Section: Discussionsupporting

confidence: 78%

Increased blood BACE1 activity as a potential common pathogenic factor of vascular dementia and late onset Alzheimer's disease

Zuliani

Trentini

Rosta

et al. 2020

Sci Rep

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“…The generation of Aβ monomeric forms is dependent upon the activity of BACE1, this being directly related to synaptic functions, plasticity and homeostasis [ 69 , 72 ]. Studies have shown the significantly increased concentrations and activity rates of BACE1 in AD brains and CSF, which is thought to cause a vicious cycle by producing Aβ peptides near synapses [ 69 , 72 , 73 , 74 , 75 ]. Other synaptic dysfunction-associated biomarkers for AD include synaptotagmin, a calcium sensor protein, SNAP-25, a component of the soluble N-ethylmaleimide sensitive factor attachment protein receptor complex, GAP-43, a pre-synaptic membrane protein, and synaptophysin, which has exhibited increased levels in the CSF of AD patients [ 69 , 76 ].…”

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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“…In this context, Rosen and colleagues found that BACE1 activity was significantly increased in AD patients with mild dementia compared to patients at more severe stages [12]. A recent study showed that BACE1 biomarker candidates are significantly increased in individuals with MCI, but not with ADD, when compared with the HC group [13]. Therefore, it is likely that the disease stage of the individual patient may influence BACE1 concentration and activity, and thus, clinical heterogeneity of included individuals may have neutralized inter-group differences.…”

Section: Potential Explanation Of Controversial Results In Csf (And Bmentioning

confidence: 98%

“…Most of the recent studies used CSF core biomarkers of AD, where BACE1 correlated indeed with Aβ and tau markers. In particular, Mulder and colleagues found that BACE1 activity was increased in individuals showing characteristic AD biological features compared to individuals with negative AD biomarkers [16], while Alexopoulos and colleagues showed significantly decreased CSF BACE1 activity in individuals with MCI without AD pathophysiology compared to patients with MCI due to AD [13].…”

Section: Potential Explanation Of Controversial Results In Csf (And Bmentioning

confidence: 99%

β-Secretase1 biological markers for Alzheimer’s disease: state-of-art of validation and qualification

Vanmechelen¹,

Zetterberg

Galgani

et al. 2020

Alz Res Therapy

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β-Secretase1 (BACE1) protein concentrations and rates of enzyme activity, analyzed in human bodily fluids, are promising candidate biological markers for guidance in clinical trials investigating BACE1 inhibitors to halt or delay the dysregulation of the amyloid-β pathway in Alzheimer’s disease (AD). A robust body of evidence demonstrates an association between cerebrospinal fluid/blood BACE1 biomarkers and core pathophysiological mechanisms of AD, such as brain protein misfolding and aggregration, neurodegeneration, and synaptic dysfunction. In pharmacological trials, BACE1 candidate biomarkers may be applied to a wide set of contexts of use (CoU), including proof of mechanism, dose-finding, response and toxicity dose estimation. For clinical CoU, BACE1 biomarkers show good performance for prognosis and disease prediction. The roadmap toward validation and qualification of BACE1 biomarkers requires standardized pre-analytical and analytical protocols to reduce inter-site variance that may have contributed to inconsistent results. BACE1 biomarker-drug co-development programs, including biomarker-guided outcomes and endpoints, may support the identification of sub-populations with a higher probability to benefit from BACE1 inhibitors with a reduced risk of adverse effects, in line with the evolving precision medicine paradigm.

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Cerebrospinal Fluid BACE1 Activity and sAβPPβ as Biomarker Candidates of Alzheimer’s Disease

Cited by 17 publications

References 49 publications

Increased blood BACE1 activity as a potential common pathogenic factor of vascular dementia and late onset Alzheimer's disease

Increased blood BACE1 activity as a potential common pathogenic factor of vascular dementia and late onset Alzheimer's disease

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

β-Secretase1 biological markers for Alzheimer’s disease: state-of-art of validation and qualification

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