Novel and High Affinity 2-[(Diphenylmethyl)sulfinyl]acetamide (Modafinil) Analogues as Atypical Dopamine Transporter Inhibitors

Cao, Jianjing; Slack, Rachel D.; Bakare, Oluyomi M.; Burzynski, Caitlin; Rais, Rana; Slusher, Barbara S.; Kopajtic, Theresa; Bonifazi, Alessandro; Ellenberger, Michael P.; Yano, Hideaki; He, Yi; Bi, Guo Hua; Xi, Zheng‐Xiong; Løland, Claus J.; Newman, Amy Hauck

doi:10.1021/acs.jmedchem.6b01373

Cited by 59 publications

(160 citation statements)

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“…On the other hand, JJC8-016 had many 'hits' at a concentration of 10 μM ( Supplementary Tables S1 and S2). Nevertheless, in addition to the binding profile recently described (Cao et al, 2016) JJC8-016 only showed Ca +2 channel binding at a concentration of 100 nM, in line with its DAT K i value of 116 nM. Thus, these other off-target activities are likely not pharmacologically relevant.…”

Section: Discussionmentioning

confidence: 67%

“…JJC8-016 (N-(2-((bis(4-fluorophenyl)methyl)thio)ethyl)-3-phenylpropan-1-amine) was selected as a lead compound as its affinity for the DAT (K i = 116 nM) and the serotonin transporter (SERT; K i = 360 nM) were higher than the parent drug, (±)MOD, and comparable to those of cocaine (Okunola-Bakare et al, 2014) (Table 1). We compared JJC8-016 with R-MOD at SERT, the D 2 -like, and sigma 1 receptors, as previous structure-activity relationship studies in a series of both modafinil and benztropine-like molecules have shown overlap in binding affinities at these sites (Cao et al, 2016) (Table 1). Herein we extended these binding studies to a screen of~70 receptors, transporters, and enzymes at concentrations of 100 nM and 10 μM.…”

Section: Introductionmentioning

confidence: 99%

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The Novel Modafinil Analog, JJC8-016, as a Potential Cocaine Abuse Pharmacotherapeutic

Zhang

Yang

et al. 2017

Neuropsychopharmacol

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(±)Modafinil ((±)MOD) and its R-enantiomer (R-modafinil; R-MOD) have been investigated for their potential as treatments for psychostimulant addiction. We recently reported a series of (±)MOD analogs, of which JJC8-016 (N-(2-((bis(4-fluorophenyl)methyl)thio)ethyl)-3-phenylpropan-1-amine) was selected for further development. JJC8-016 and R-MOD were evaluated for binding across ~70 receptors, transporters, and enzymes. Although at a concentration of 10 μM, there were many hits for JJC8-016, binding affinities in the range of its DAT affinity were only observed at the serotonin transporter (SERT), dopamine D-like, and sigma receptors. R-MOD was more selective, but had much lower affinity at the DAT (K=3 μM) than JJC8-016 (K=116 nM). In rats, systemic administration of R-MOD alone (10-30 mg/kg i.p.) dose-dependently increased locomotor activity and electrical brain-stimulation reward, whereas JJC8-016 (10-30 mg/kg i.p.) did not produce these effects. Strikingly, pretreatment with JJC8-016 dose-dependently inhibited cocaine-enhanced locomotion, cocaine self-administration, and cocaine-induced reinstatement of drug-seeking behavior, whereas R-MOD inhibited cocaine-induced reinstatement only at the high dose of 100 mg/kg. Notably, JJC8-016 alone neither altered extracellular dopamine in the nucleus accumbens nor maintained self-administration. It also failed to induce reinstatement of drug-seeking behavior. These findings suggest that JJC8-016 is a unique DAT inhibitor that has no cocaine-like abuse potential by itself. Moreover, pretreatment with JJC8-016 significantly inhibits cocaine-taking and cocaine-seeking behavior likely by interfering with cocaine binding to DAT. In addition, off-target actions may also contribute to its potential therapeutic utility in the treatment of cocaine abuse.

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Section: Discussionmentioning

confidence: 67%

Section: Introductionmentioning

confidence: 99%

The Novel Modafinil Analog, JJC8-016, as a Potential Cocaine Abuse Pharmacotherapeutic

Zhang

Yang

et al. 2017

Neuropsychopharmacol

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“…Indeed, although R-modafinil is not self-administered (Zhang et al, 2017) it does share other behavioral actions with cocaine in rodents (Loland et al, 2012). Notably, R-modafinil is not as effective in attenuating the self-administration of cocaine as JHW 007 or a recently reported modafinil analogue, JJC8-016 (Okunola-Bakare et al, 2014; Cao et al, 2016; Zhang et al, 2017). In contrast, JHW 007 appeared to blunt the cellular effects of cocaine in a concentration-dependent manner that did not resemble occlusion.…”

Section: Discussionmentioning

confidence: 77%

“…In contrast however, JHW 007 decreased IPSC amplitude in a manner consistent with D2 receptor antagonism. Unlike cocaine and R-modafinil (Zhang et al, 2017), JHW 007 has affinity for the D2L receptor (47.1 nM, Katz et al, 2004) and is a weak D2 receptor antagonist (IC 50 = 2 μM, Cao et al, 2016) in addition to exhibiting 12 nM binding affinity for DAT (Kopajtic et al, 2010). This could explain how mid-micromolar concentrations of JHW 007 reduced DA-mediated current amplitudes.…”

Section: Discussionmentioning

confidence: 99%

“…An ideal treatment would not be reinforcing and would have little effect on normal cellular physiology, all while blunting the behavioral and cellular effects of cocaine. An additional consideration is that JHW 007, in addition to binding to DAT and D2 receptors, also exhibits high affinity for other potential targets (Katz et al, 2004; Cao et al, 2016). Future work will explore the role of these other targets in the cellular effects of atypical DAT inhibitors, and could reveal ideal cellular actions for the design of potential medications for the treatment of cocaine abuse.…”

Section: Discussionmentioning

confidence: 99%

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Atypical dopamine transporter inhibitors R-modafinil and JHW 007 differentially affect D2 autoreceptor neurotransmission and the firing rate of midbrain dopamine neurons

et al. 2017

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Abuse of psychostimulants like cocaine that inhibit dopamine (DA) reuptake through the dopamine transporter (DAT) represents a major public health issue, however FDA-approved pharmacotherapies have yet to be developed. Recently a class of ligands termed “atypical DAT inhibitors” has gained attention due to their range of effectiveness in increasing extracellular dopamine (DA) levels without demonstrating significant abuse liability. These compounds not only hold promise as therapeutic agents to treat stimulant use disorders but also as experimental tools to improve our understanding of DAT function. Here we used patch clamp electrophysiology in mouse brain slices to explore the effects of two atypical DAT inhibitors (R-modafinil and JHW 007) on the physiology of single DA neurons in the substantia nigra and ventral tegmental area. Despite their commonalities of being DAT inhibitors that lack cocaine-like behavioral profiles, these compounds exhibited surprisingly divergent cellular effects. Similar to cocaine, R-modafinil slowed DA neuron firing in a D2 receptor-dependent manner and rapidly enhanced the amplitude and duration of D2 receptor-mediated currents in the midbrain. In contrast, JHW 007 exhibited little effect on firing, slow DAT blockade, and an unexpected inhibition of D2 receptor-mediated currents that may be due to direct D2 receptor antagonism. Furthermore, pretreatment with JHW 007 blunted the cellular effects of cocaine, suggesting that it may be valuable to investigate similar DAT inhibitors as potential therapeutic agents. Further exploration of these and other atypical DAT inhibitors may reveal important cellular effects of compounds that will have potential as pharmacotherapies for treating cocaine use disorders.

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Catalyst‐free 1,6‐Conjugate Addition of S‐Nucleophiles to para‐Quinone Methides

Xie

Zang

Liu³

et al. 2022

Asian J Org Chem

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An efficient access to a large array of diarylmethane thioether derivatives is developed through catalyst‐free 1,6‐conjugate addition of 1,4‐dithiane‐2,5‐diols with para‐quinone methides in high to excellent yields. Moreover, this reaction system is also suitable for other sulfur‐based nucleophiles, and the resulting products can be readily converted into other valuable diarylmethane derivatives.

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Novel and High Affinity 2-[(Diphenylmethyl)sulfinyl]acetamide (Modafinil) Analogues as Atypical Dopamine Transporter Inhibitors

Cited by 59 publications

References 57 publications

The Novel Modafinil Analog, JJC8-016, as a Potential Cocaine Abuse Pharmacotherapeutic

The Novel Modafinil Analog, JJC8-016, as a Potential Cocaine Abuse Pharmacotherapeutic

Atypical dopamine transporter inhibitors R-modafinil and JHW 007 differentially affect D2 autoreceptor neurotransmission and the firing rate of midbrain dopamine neurons

Catalyst‐free 1,6‐Conjugate Addition of S‐Nucleophiles to para‐Quinone Methides

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