BACE-1 and γ-Secretase as Therapeutic Targets for Alzheimer’s Disease

Maia, Mariana; Sousa, Emı́lia

doi:10.3390/ph12010041

Cited by 89 publications

(64 citation statements)

References 80 publications

(146 reference statements)

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“…The property of a therapeutic agent in AD to penetrate the BBB has generally been regarded as a prerequisite for new drugs [96]. Recognition of the importance of the liver in A␤ production and clearance means that targeting the liver might be a promising therapeutic approach.…”

Section: Gene Silencing and Genome Editingmentioning

confidence: 99%

Is Alzheimer’s Disease a Liver Disease of the Brain?

Bassendine

Taylor-Robinson

Fertleman

et al. 2020

JAD

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Clinical specialization is not only a force for progress, but it has also led to the fragmentation of medical knowledge. The focus of research in the field of Alzheimer's disease (AD) is neurobiology, while hepatologists focus on liver diseases and lipid specialists on atherosclerosis. This article on AD focuses on the role of the liver and lipid homeostasis in the development of AD. Amyloid-␤ (A␤) deposits accumulate as plaques in the brain of an AD patient long before cognitive decline is evident. A␤ generation is a normal physiological process; the steady-state level of A␤ in the brain is determined by balance between A␤ production and its clearance. We present evidence suggesting that the liver is the origin of brain A␤ deposits and that it is involved in peripheral clearance of circulating A␤ in the blood. Hence the liver could be targeted to decrease A␤ production or increase peripheral clearance.

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Section: Gene Silencing and Genome Editingmentioning

confidence: 99%

Is Alzheimer’s Disease a Liver Disease of the Brain?

Bassendine

Taylor-Robinson

Fertleman

et al. 2020

JAD

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“…Nanomolar inhibitors based on several heterocyclic scaffolds have been developed and a number have progressed to clinical trials [ 17 , 18 , 26 ]. Although some programs have been discontinued due to phase III failure, interest in BACE-1 inhibitors is still high, in particular for the development of modifying therapies for early stage AD [ 27 , 28 ].…”

Section: Introductionmentioning

confidence: 99%

One Pot Synthesis of Micromolar BACE-1 Inhibitors Based on the Dihydropyrimidinone Scaffold and Their Thia and Imino Analogues

et al. 2020

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A library of dihydropyrimidinones was synthesized via a “one-pot” three component Biginelli reaction using different aldehydes in combination with β-dicarbonyl compounds and urea. Selected 2-thiooxo and 2-imino analogs were also obtained with the Biginelli reaction from thiourea and guanidine hydrochloride, respectively. The products were screened in vitro for their β-secretase inhibitory activity. The majority of the compounds resulted to be active, with IC50 in the range 100 nM–50 μM.

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“…With aspartic proteases being found in nearly all body tissues and involved in various physiological functions, off-target activity causing severe side effects is possible and likely if an inhibitor is not specific to BACE1 [ 19 ]. LY2811376, a promising clinical candidate of BACE1 inhibitor (IC 50 , 0.24 μM), did not proceed to phase II clinical trials because of its off-target activity against cathepsin D [ 20 ]. The present results clearly suggest that our compound only suppressed specific targeted enzyme BACE1 without causing adverse effects.…”

Section: Resultsmentioning

confidence: 99%

Discovery of Sulforaphane as a Potent BACE1 Inhibitor Based on Kinetics and Computational Studies

et al. 2020

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BACE1 is the rate-limiting enzyme involved in the production and deposition of β-amyloid (Aβ). Since neurotoxic Aβ plays a critical role in Alzheimer’s disease (AD) pathogenesis, BACE1 has emerged as a key target for preventing AD. In the present study, the potential of sulforaphane, an isothiocyanate found in cruciferous vegetables, as a BACE1 inhibitor has been investigated. Sulforaphane exhibited six times more potent activity against BACE1 compared to well-known positive controls including resveratrol and quercetin. Sulforaphane presented selective and non-competitive BACE1 inhibitory activity with low off-target inhibition of BACE2 and other aspartic and serine proteases. In addition, sulforaphane presented negative binding energy, suggesting that the compound had a high affinity for BACE1. It interacted with locations other than the active binding sites of BACE1 through van der Waals forces. Overall, sulforaphane appeared to be a promising candidate with potent and selective BACE1 inhibitory properties that play an important role in AD prevention.

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BACE-1 and γ-Secretase as Therapeutic Targets for Alzheimer’s Disease

Cited by 89 publications

References 80 publications

Is Alzheimer’s Disease a Liver Disease of the Brain?

Is Alzheimer’s Disease a Liver Disease of the Brain?

One Pot Synthesis of Micromolar BACE-1 Inhibitors Based on the Dihydropyrimidinone Scaffold and Their Thia and Imino Analogues

Discovery of Sulforaphane as a Potent BACE1 Inhibitor Based on Kinetics and Computational Studies

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