Quantum mechanics study of the hydroxyethylamines–BACE-1 active site interaction energies

Gueto-Tettay, Carlos; Drosos, Juan Carlos; Vivas‐Reyes, Ricardo

doi:10.1007/s10822-011-9443-z

Cited by 17 publications

(9 citation statements)

References 49 publications

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“…Thus, designing inhibitors that are capable of forming those vital anchor point interactions with BACE1 and maintaining this interaction over time is crucial to yield the best possible inhibitory activity. It was observed that the protonation status of hydroxyethyl amines could be shifted with time resulting in loss of essential interactions with BACE1 residues shifting the flap confirmation from the active (closed) back to the open form . Therefore, this shift in the flap confirmation can explain how some HEAs derivatives would fail to inhibit the BACE1 activity in real time.…”

Section: Failure Of Bace1 Inhibitors: Lessons To the Futurementioning

confidence: 99%

BACE1 inhibitors: Current status and future directions in treating Alzheimer's disease

Moussa-Pacha

Abdin

Omar

et al. 2019

Medicinal Research Reviews

187

175

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Alzheimer's disease (AD) is an irreversible, progressive neurodegenerative brain disorder with no current cure. One of the important therapeutic approaches of AD is the inhibition of β‐site APP cleaving enzyme‐1 (BACE1), which is involved in the rate‐limiting step of the cleavage process of the amyloid precursor protein (APP) leading to the generation of the neurotoxic amyloid β (Aβ) protein after the γ‐secretase completes its function. The produced insoluble Aβ aggregates lead to plaques deposition and neurodegeneration. BACE1 is, therefore, one of the attractive targets for the treatment of AD. This approach led to the development of potent BACE1 inhibitors, many of which were advanced to late stages in clinical trials. Nonetheless, the high failure rate of lead drug candidates targeting BACE1 brought to the forefront the need for finding new targets to uncover the mystery behind AD. In this review, we aim to discuss the most promising classes of BACE1 inhibitors with a description and analysis of their pharmacodynamic and pharmacokinetic parameters, with more focus on the lead drug candidates that reached late stages of clinical trials, such as MK8931, AZD‐3293, JNJ‐54861911, E2609, and CNP520. In addition, the manuscript discusses the safety concerns and insignificant physiological effects, which were highlighted for the most successful BACE1 inhibitors. Furthermore, the review demonstrates with increasing evidence that despite tremendous efforts and promising results conceived with BACE1 inhibitors, the latest studies suggest that their clinical use for treating Alzheimer's disease should be reconsidered. Finally, the review sheds light on alternative therapeutic options for targeting AD.

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Section: Failure Of Bace1 Inhibitors: Lessons To the Futurementioning

confidence: 99%

BACE1 inhibitors: Current status and future directions in treating Alzheimer's disease

Moussa-Pacha

Abdin

Omar

et al. 2019

Medicinal Research Reviews

187

175

View full text Add to dashboard Cite

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“…These plaques consist of aggregated amyloid--peptide (A ) deposits, -protein aggregation, oxidative stress, dyshomeostasis of biometals, and low acetylcholine (ACh) levels and plays significant role in the pathophysiology of the disease [7]. Nowadays, the most used therapeutic treatment against AD involves the use of acetylcholinesterase inhibitors (AChEIs) that improve AD symptoms by AChE inhibition [8][9][10][11][12]. The reversible AChE inhibition has become the promising target for the treatment of AD which is mainly associated with low in vivo AChE levels.…”

Section: Introductionmentioning

confidence: 99%

Scale Alpha and Beta of Quantitative Convergence and Chemical Reactivity Analysis in Dual Cholinesterase/Monoamine Oxidase Inhibitors for the Alzheimer Disease Treatment Using Density Functional Theory (DFT)

Morales-Bayuelo

Baldiris

Vivas‐Reyes

2013

Journal of Theoretical Chemistry

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Molecular quantum similarity descriptors and Density Functional Theory (DFT) based reactivity descriptors were studied for a series of cholinesterase/monoamine oxidase inhibitors used for the Alzheimer's disease treatment (AD). This theoretical study is expected to shed some light onto some molecular aspects that could contribute to the knowledge of the molecular mechanics behind interactions of these molecules with acetylcholinesterase (AChE) and butyrylcholinesterase (BuChE), as well as with monoamine oxidase (MAO) A and B. The Topogeometrical Superposition Algorithm to handle flexible molecules (TGSA-Flex) alignment method was used to solve the problem of the relative orientation in the quantum similarity (QS) field. Using the molecular quantum similarity (MQS) field and reactivity descriptors supported in the DFT was possible the quantification of the steric and electrostatic effects through of the Coulomb and Overlap quantitative convergence scales (alpha and beta). In addition, an analysis of reactivity indexes is development, using global and local descriptors, identifying the binding sites and selectivity in the (cholinesterase/monoamine oxidase) inhibitors, understanding the retrodonor process, and showing new insight for drugs design in a disease of difficult control as Alzheimer.

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“…Alternatively, smaller, approximate models can be used at higher levels of QM theory to evaluate particular regions of interest more rapidly. [41][42][43][44] Each of the methods discussed above offers distinct advantages in particular circumstances. For example, MM methods are very quick to evaluate, meaning extensive sampling is possible.…”

Section: Introductionmentioning

confidence: 99%

“…A number of methods are available to predict the strength of interaction of individual functional groups which can prove extremely insightful in the design and modification of lead series. 41,43,44,[49][50][51] In this work we consider the use of small QM models of receptors, consisting of the key polar active site interactions, rather than generic probes. The region selected is not as extensive as used in the approach of Gueto-Tettay, who used residues within 5 Å of the active site, which, due to the significant size, necessitates the use of the semi-empirical PM6 method.…”

Section: Introductionmentioning

confidence: 99%

“…The region selected is not as extensive as used in the approach of Gueto-Tettay, who used residues within 5 Å of the active site, which, due to the significant size, necessitates the use of the semi-empirical PM6 method. 41 Here we investigate smaller, yet more interaction relevant active site models. We are not, per se, interested in predicting the much more challenging absolute binding free energy, 28 rather, the goal is to determine whether such methods could be used to assess the relative interaction strength of inhibitors with key polar elements of a receptor, with the view to using them to rapidly assess alternative modifications of lead series to improve the contribution to enthalpic binding.…”

Section: Introductionmentioning

confidence: 99%

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Evaluating the enthalpic contribution to ligand binding using QM calculations: effect of methodology on geometries and interaction energies

et al. 2012

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As a result of research on ligand efficiency in the pharmaceutical industry, there is greater focus on optimizing the strength of polar interactions within receptors, so that the contribution of overall size and lipophilicity to binding can be decreased. A number of quantum mechanical (QM) methods involving simple probes are available to assess the H-bonding potential of different heterocycles or functional groups. However, in most receptors, multiple features are present, and these have distinct directionality, meaning very minimalist models may not be so ideal to describe the interactions. We describe how the use of gas phase QM models of kinase protein-ligand complex, which can more closely mimic the polar features of the active site region, can prove useful in assessing alterations to a core template, or different substituents. We investigate some practical issues surrounding the use of QM cluster models in structure based design (SBD). These include the choice of the method; semi-empirical, density functional theory or ab-initio, the choice of the basis set, whether to include implicit or explicit solvation, whether BSSE should be included, etc. We find a combination of the M06-2X method and the 6-31G* basis set is sufficiently rapid, and accurate, for the computation of structural and energetic parameters for this system.

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Quantum mechanics study of the hydroxyethylamines–BACE-1 active site interaction energies

Cited by 17 publications

References 49 publications

BACE1 inhibitors: Current status and future directions in treating Alzheimer's disease

BACE1 inhibitors: Current status and future directions in treating Alzheimer's disease

Scale Alpha and Beta of Quantitative Convergence and Chemical Reactivity Analysis in Dual Cholinesterase/Monoamine Oxidase Inhibitors for the Alzheimer Disease Treatment Using Density Functional Theory (DFT)

Evaluating the enthalpic contribution to ligand binding using QM calculations: effect of methodology on geometries and interaction energies

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