Translating genetic risk of Alzheimer’s disease into mechanistic insight and drug targets

Sierksma, Annerieke; Escott‐Price, Valentina; Strooper, Bart De

doi:10.1126/science.abb8575

Cited by 103 publications

(83 citation statements)

References 59 publications

(87 reference statements)

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“…In the threshold model, liability for a genetic disorder is (normally) distributed across the population and polygenic risk scores are a measure of disease liability 39 . The relative contributions of alleles of various effect sizes and frequencies are not fully resolved; while common alleles of small risk, captured by genome-wide association study arrays, capture between a third and a half of the genetic variance in liability, APOE alone substantially increases risk for the disorder 40 . A major problem with AD and using PRS to categorise people at risk, is the age of the study participants.…”

Section: Discussionmentioning

confidence: 99%

“…In conclusion, identifying individuals at high and low polygenic risk is very important for further work to understand how genetic risk translates into mechanisms of disease 40 . It might also become very relevant for drug development efforts targeting precise mechanisms of disease, as the PRS scores could be used to select small samples of patients in which proof of concept for the treatment can be obtained before testing the drug in larger cohorts.…”

Section: Discussionmentioning

confidence: 99%

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Identifying individuals with high risk of Alzheimer’s disease using polygenic risk scores is most accurate when using all genetic information.

Leonenko

Baker

Stevenson-Hoare

et al. 2021

Preprint

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There is little agreement regarding the approach and optimal p-value threshold of SNPs to calculate genetic risk scores for Alzheimer’s disease (AD). This reflects a fundamental underlying debate on the polygenic versus oligogenic disease architecture. We re-investigated the assumptions underlying the choice of specific p-value thresholds defining genetic loci used to determine polygenic risk scores (PRS). We find the optimal p-value threshold for SNP selection is 0.1, which supports the polygenic architecture of AD. We found that previous studies supporting an oligogenic model of AD did not take account of the reduction of APOE-ε4 allele frequency in older individuals, which skewed the results towards lower p-value thresholds and eclipsed the contribution of genes associated to AD with higher p-values. The polygenic approach to AD is also effective to identify individuals at high or low AD risk, when only APOE-ε3 homozygous individuals are considered. We also introduce the standardisation of PRS against a population data which ensures comparability of the PRS between studies. In conclusion, our work demonstrates that AD is fundamentally a polygenic disease and that stratifying populations for AD risk best takes the full PRS score into account.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Identifying individuals with high risk of Alzheimer’s disease using polygenic risk scores is most accurate when using all genetic information.

Leonenko

Baker

Stevenson-Hoare

et al. 2021

Preprint

Self Cite

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“…Soluble Aβ dimers and oligomers are able to hyperactivate and damage glutamateric neurons and synapses [ 27 , 31 ]. In addition, all major gene modifications, which have been identified so far in association with an increased AD risk, are related to Aβ generation, aggregation and clearance, and microglia responses [ 4 ]. Furthermore, the anti-Aβ antibodies aducanumab [ 32 ] and donanemab [ 33 ] have shown potential to delay cognitive decline by reducing brain Aβ load, when treatment of patients with antibody takes place very early in the disease.…”

Section: Alzheimer’s Disease—toxic Amyloid-β Proteins and Triggered Neuropathogenic Phenomenamentioning

confidence: 99%

“…In Alzheimer’s disease (AD), neurodegenerative but also contributing vascular and hemostatic changes in the brain lead to the loss of memory and cognitive skills, robbing humans ultimately of their essential personality. To date, there is no medicine in clinical use or recognizable in the research pipeline that can effectively combat AD, a disease, which affects more than 1 million people in Germany and 40 million worldwide [ 1 , 2 , 3 , 4 , 5 , 6 ]. Of these individuals, less than 10% develop symptoms well before the age of 65 due to their hereditary predisposition, known as early-onset AD [ 4 ].…”

Section: Introductionmentioning

confidence: 99%

“…To these standard AD therapeutics belong cholinesterase inhibitors, such as donepezil, galantamine, rivastigmin, and glutamate antagonists like memantine [ 5 ]. Therefore, an urgent task of pharmaceutical research is to search for novel, more effective drugs to possibly cure or considerably mitigate AD [ 3 , 4 ]. Another strategy is to look for new therapeutic approaches, which are based on already known active ingredients with other approval for use [ 6 ].…”

Section: Introductionmentioning

confidence: 99%

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Alzheimer’s Disease—Rationales for Potential Treatment with the Thrombin Inhibitor Dabigatran

Großmann

2021

IJMS

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Alzheimer’s disease (AD) is caused by neurodegenerative, but also vascular and hemostatic changes in the brain. The oral thrombin inhibitor dabigatran, which has been used for over a decade in preventing thromboembolism and has a well-known pharmacokinetic, safety and antidote profile, can be an option to treat vascular dysfunction in early AD, a condition known as cerebral amyloid angiopathy (CAA). Recent results have revealed that amyloid-β proteins (Aβ), thrombin and fibrin play a crucial role in triggering vascular and parenchymal brain abnormalities in CAA. Dabigatran blocks soluble thrombin, thrombin-mediated formation of fibrin and Aβ-containing fibrin clots. These clots are deposited in brain parenchyma and blood vessels in areas of CAA. Fibrin-Aβ deposition causes microvascular constriction, occlusion and hemorrhage, leading to vascular and blood–brain barrier dysfunction. As a result, blood flow, perfusion and oxygen and nutrient supply are chronically reduced, mainly in hippocampal and neocortical brain areas. Dabigatran has the potential to preserve perfusion and oxygen delivery to the brain, and to prevent parenchymal Aβ-, thrombin- and fibrin-triggered inflammatory and neurodegenerative processes, leading to synapse and neuron death, and cognitive decline. Beneficial effects of dabigatran on CAA and AD have recently been shown in preclinical studies and in retrospective observer studies on patients. Therefore, clinical studies are warranted, in order to possibly expand dabigatran approval for repositioning for AD treatment.

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Gold Nanostrip Array‐Mediated Wireless Electrical Stimulation for Accelerating Functional Neuronal Differentiation

Yang

Sun

et al. 2022

Advanced Science

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Neural stem cell (NSC)‐based therapy holds great promise for the treatment of neurodegenerative diseases. Presently, however, it is hindered by poor functional neuronal differentiation. Electrical stimulation is considered one of the most effective ways to promote neuronal differentiation of NSCs. In addition to surgically implanted electrodes, traditional electrical stimulation includes wires connected to the external power supply, and an additional surgery is required to remove the electrodes or wires following stimulation, which may cause secondary injuries and infections. Herein, a novel method is reported for generation of wireless electrical signals on an Au nanostrip array by leveraging the effect of electromagnetic induction under a rotating magnetic field. The intensity of the generated electrical signals depends on the rotation speed and magnetic field strength. The Au nanostrip array‐mediated electric stimulation promotes NSC differentiation into mature neurons within 5 days, at the mRNA, protein, and function levels. The rate of differentiation is faster by at least 5 days than that in cells without treatment. The Au nanostrip array‐based wireless device also accelerates neuronal differentiation of NSCs in vivo. The novel method to accelerate the neuronal differentiation of NSCs has the advantages of wireless, timely, localized and precise controllability, and noninvasive power supplementation.

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Translating genetic risk of Alzheimer’s disease into mechanistic insight and drug targets

Cited by 103 publications

References 59 publications

Identifying individuals with high risk of Alzheimer’s disease using polygenic risk scores is most accurate when using all genetic information.

Identifying individuals with high risk of Alzheimer’s disease using polygenic risk scores is most accurate when using all genetic information.

Alzheimer’s Disease—Rationales for Potential Treatment with the Thrombin Inhibitor Dabigatran

Gold Nanostrip Array‐Mediated Wireless Electrical Stimulation for Accelerating Functional Neuronal Differentiation

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