Increased sodium channel use-dependent inhibition by a new potent analogue of tocainide greatly enhances in vivo antimyotonic activity

Bellis, Michela De; Carbonara, Roberta; Roussel, Julien; Farinato, Alessandro; Massari, Ada Maria; Pierno, Sabata; Muraglia, Marilena; Corbo, Filomena; Franchini, Carlo; Carratù, Maria Rosaria; A, De Luca; Camerino, Diana Conte; Desaphy, Jean-François

doi:10.1016/j.neuropharm.2016.10.013

Cited by 27 publications

(31 citation statements)

References 53 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Another main aim of our study was to investigate about a potential anti-oxidant effect of the tetramethyl-pyrroline-derivatives, by means of assessing their cyto-protective action on a model of H 2 O 2 -induced oxidative stress cytotoxicity. However, data from our and other laboratories underlined a direct potential cytotoxicity of local anesthetic-like drugs on various cell types (Hofmann et al, 2013 ; Sung et al, 2014 ; De Bellis et al, 2017a ). Then we first evaluated the ability of the lead compound Mex, to modulate by itself C 2 C 12 cell viability with respect to H 2 O 2 .…”

Section: Results Pharmacologymentioning

confidence: 81%

“…We then assessed the activity of the new Mex and Me5 derivatives on Na V 1.4 channel (De Bellis et al, 2017a ). This was of importance considering the presence of the pyrroline moiety on the main pharmacophore group (amino-terminal group).…”

Section: Results Pharmacologymentioning

confidence: 99%

“…Surprisingly, the new analog CI16 is the most use-dependent mexiletine-like sodium channel blocker described so far, with a ratio IC 50 TB/IC 50 10-Hz UDB of 21 (Table 2 ). The use-dependent behavior is a complex dynamic process involving the kinetics of drug binding to and unbinding from the channel in relation to both state-dependent drug affinity and physicochemical properties (De Bellis et al, 2017a , b ). The recovery from inactivation of drug-bound channels was determined.…”

Section: Results Pharmacologymentioning

confidence: 99%

“…The acquired traces were analyzed offline using Clampfit software (pClamp6; Axon Instruments). This method was shown to be predictable of drug efficacy on mammalian sodium channel and myotonic conditions (De Luca et al, 2004 ; De Bellis et al, 2017a ).…”

Section: Methodsmentioning

confidence: 99%

See 3 more Smart Citations

Dual Action of Mexiletine and Its Pyrroline Derivatives as Skeletal Muscle Sodium Channel Blockers and Anti-oxidant Compounds: Toward Novel Therapeutic Potential

et al. 2018

Self Cite

View full text Add to dashboard Cite

Mexiletine (Mex) has been recently appointed as an orphan-drug in myotonic-syndromes, being a potent use-dependent blocker of skeletal-muscle sodium channels (NaV1.4). Available evidences about a potential anti-oxidant effect of Mex and its tetramethyl-pyrroline-derivatives in vivo, suggest the possibility to further enlarge the therapeutic potential of Mex-like compounds in myopathies in which alteration of excitation-contraction coupling is paralleled by oxidative stress. In line with this and based on our previous structure-activity-relationship studies, we synthesized new compounds with a tetramethyl-pyrroline-ring on the amino-group of both Mex (VM11) and of its potent use-dependent isopropyl-derivative (CI16). The compounds were tested for their ability to block native NaV1.4 and to exert cyto-protective effects against oxidative-stress injury in myoblasts. Voltage-clamp-recordings on adult myofibers were performed to assess the tonic and use-dependent block of peak sodium-currents (INa) by VM11 and CI16, as well as Mex, VM11 and CI16 were 3 and 6-fold more potent than Mex in producing a tonic-block of peak sodium-currents (INa), respectively. Interestingly, CI16 showed a 40-fold increase of potency with respect to Mex during high-frequency stimulation (10-Hz), resulting the strongest use-dependent Mex-like compound so far. The derivatives also behaved as inactivated channel blockers, however the voltage dependent block was modest. The experimental data fitted with the molecular-modeling simulation based on previously proposed interaction of main pharmacophores with NaV1.4 binding-site. CI16 and VM11 were then compared to Mex and its isopropyl derivative (Me5) for the ability to protect C2C12-cells from H2O2-cytotoxicity in the concentration range effective on Nav1.4. Mex and Me5 showed a moderate cyto-protective effect in the presence of H2O2, Importantly, CI16 and VM11 showed a remarkable cyto-protection at concentrations effective for use-dependent block of NaV1.4. This effect was comparable to that of selected anti-oxidant drugs proved to exert protective effect in preclinical models of progressive myopathies such as muscular dystrophies. Then, the tetramethyl-pyrroline compounds have increased therapeutic profile as sodium channel blockers and an interesting cyto-protective activity. The overall profile enlarges therapeutic potential from channelopathies to myopathies in which alteration of excitation-contraction coupling is paralleled by oxidative-stress, i.e., muscular dystrophies.

show abstract

Section: Results Pharmacologymentioning

confidence: 81%

Section: Results Pharmacologymentioning

confidence: 99%

Section: Results Pharmacologymentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

Dual Action of Mexiletine and Its Pyrroline Derivatives as Skeletal Muscle Sodium Channel Blockers and Anti-oxidant Compounds: Toward Novel Therapeutic Potential

et al. 2018

Self Cite

View full text Add to dashboard Cite

show abstract

“…Even more importantly, similar computational approaches can be used as one of the steps to design drugs, which have similar membrane binding affinities and bind around mutated protein residues that result in altered channel function. Such an approach focusing on a desired drug lipophilicity and spatial arrangement of crucial functional groups was used, for instance, to design selective sodium channel blockers (Muraglia et al, 2007 ; De Luca et al, 2012 ; De Bellis et al, 2017 ). Such a structure-function based approach was shown to improve drug safety profile through mitigation of off-target effects, including hERG block (De Bellis et al, 2017 ).…”

Section: Discussionmentioning

confidence: 99%

Digging into Lipid Membrane Permeation for Cardiac Ion Channel Blocker d-Sotalol with All-Atom Simulations

et al. 2018

View full text Add to dashboard Cite

Interactions of drug molecules with lipid membranes play crucial role in their accessibility of cellular targets and can be an important predictor of their therapeutic and safety profiles. Very little is known about spatial localization of various drugs in the lipid bilayers, their active form (ionization state) or translocation rates and therefore potency to bind to different sites in membrane proteins. All-atom molecular simulations may help to map drug partitioning kinetics and thermodynamics, thus providing in-depth assessment of drug lipophilicity. As a proof of principle, we evaluated extensively lipid membrane partitioning of d-sotalol, well-known blocker of a cardiac potassium channel Kv11.1 encoded by the hERG gene, with reported substantial proclivity for arrhythmogenesis. We developed the positively charged (cationic) and neutral d-sotalol models, compatible with the biomolecular CHARMM force field, and subjected them to all-atom molecular dynamics (MD) simulations of drug partitioning through hydrated lipid membranes, aiming to elucidate thermodynamics and kinetics of their translocation and thus putative propensities for hydrophobic and aqueous hERG access. We found that only a neutral form of d-sotalol accumulates in the membrane interior and can move across the bilayer within millisecond time scale, and can be relevant to a lipophilic channel access. The computed water-membrane partitioning coefficient for this form is in good agreement with experiment. There is a large energetic barrier for a cationic form of the drug, dominant in water, to cross the membrane, resulting in slow membrane translocation kinetics. However, this form of the drug can be important for an aqueous access pathway through the intracellular gate of hERG. This route will likely occur after a neutral form of a drug crosses the membrane and subsequently re-protonates. Our study serves to demonstrate a first step toward a framework for multi-scale in silico safety pharmacology, and identifies some of the challenges that lie therein.

show abstract

Bioisosteric Modification of To042: Synthesis and Evaluation of Promising Use‐Dependent Inhibitors of Voltage‐Gated Sodium Channels

et al. 2021

Self Cite

View full text Add to dashboard Cite

Three analogues of To042, a tocainide‐related lead compound recently reported for the treatment of myotonia, were synthesized and evaluated in vitro as skeletal muscle sodium channel blockers possibly endowed with enhanced use‐dependent behavior. Patch‐clamp experiments on hNav1.4 expressed in HEK293 cells showed that N‐[(naphthalen‐1‐yl)methyl]‐4‐[(2,6‐dimethyl)phenoxy]butan‐2‐amine, the aryloxyalkyl bioisostere of To042, exerted a higher use‐dependent block than To042 thus being able to preferentially block the channels in over‐excited membranes while preserving healthy tissue function. It also showed the lowest active transport across BBB according to the results of P‐glycoprotein (P‐gp) interacting activity evaluation and the highest cytoprotective effect on HeLa cells. Quantum mechanical calculations and dockings gave insights on the most probable conformation of the aryloxyalkyl bioisostere of To042 in solution and the target residues involved in the binding, respectively. Both approaches indicated the conformations that might be adopted in both the unbound and bound state of the ligand. Overall, N‐[(naphthalen‐1‐yl)methyl]‐4‐[(2,6‐dimethyl)phenoxy]butan‐2‐amine exhibits an interesting toxico‐pharmacological profile and deserves further investigation.

show abstract

Increased sodium channel use-dependent inhibition by a new potent analogue of tocainide greatly enhances in vivo antimyotonic activity

Cited by 27 publications

References 53 publications

Dual Action of Mexiletine and Its Pyrroline Derivatives as Skeletal Muscle Sodium Channel Blockers and Anti-oxidant Compounds: Toward Novel Therapeutic Potential

Dual Action of Mexiletine and Its Pyrroline Derivatives as Skeletal Muscle Sodium Channel Blockers and Anti-oxidant Compounds: Toward Novel Therapeutic Potential

Digging into Lipid Membrane Permeation for Cardiac Ion Channel Blocker d-Sotalol with All-Atom Simulations

Bioisosteric Modification of To042: Synthesis and Evaluation of Promising Use‐Dependent Inhibitors of Voltage‐Gated Sodium Channels

Contact Info

Product

Resources

About