Treating cocaine addiction with viruses

Carrera, Marta; Kaufmann, Gunnar F.; Mee, Jenny M.; Meijler, Michaël M.; Koob, George F.; Janda, Kim D.

doi:10.1073/pnas.0403795101

Cited by 102 publications

(95 citation statements)

References 46 publications

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“…[1][2][3][4]6 An alternative approach is to interfere with the delivery of cocaine to its receptors or accelerate its metabolism in the body. 4,[7][8][9][10][11][12][13][14][15][16][17] Butyrylcholinesterase (BChE), the principal plasma enzyme that catalyzes cocaine hydrolysis into its biologically inactive metabolites, is an ideal target for this purpose. There are some clear advantages of using this enzyme to accelerate the cocaine metabolism.…”

Section: Introductionmentioning

confidence: 99%

Free Energy Perturbation (FEP) Simulation on the Transition States of Cocaine Hydrolysis Catalyzed by Human Butyrylcholinesterase and Its Mutants

et al. 2007

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A novel computational protocol based on free energy perturbation (FEP) simulations on both the free enzyme and transition state structures has been developed and tested to predict the mutation-caused shift of the free energy change from the free enzyme to the rate-determining transition state for human butyrylcholinesterase (BChE)-catalyzed hydrolysis of (-)-cocaine. The calculated shift, denoted by ΔΔG(1→2), of such kind of free energy change determines the catalytic efficiency (k cat /K M ) change caused by the simulated mutation transforming enzyme 1 to enzyme 2. By using the FEP-based computational protocol, the ΔΔG(1→2) values for the mutations A328W/Y332A → A328W/Y332G and A328W/Y332G → A328W/Y332G/A199S were calculated to be -0.22 and -1.94 kcal/mol, respectively. The calculated ΔΔG(1→2) values predict that the change from the A328W/Y332A mutant to the A328W/Y332G mutant should slightly improve the catalytic efficiency and that the change from the A328W/Y332G mutant to the A328W/Y332G/A199S mutant should significantly improve the catalytic efficiency of the enzyme for the (-)-cocaine hydrolysis. The predicted catalytic efficiency increases are supported by the experimental data showing that k cat /K M = 8.5 × 10 6 , 1.4 × 10 7 , and 7.2 × 10 7 min -1 M -1 for the A328W/Y332A, A328W/Y332G, and A328W/Y332G/A199S mutants, respectively. The qualitative agreement between the computational and experimental data suggests that the FEP simulations may provide a promising protocol for rational design of highactivity mutants of an enzyme. The general computational strategy of the FEP simulation on a transition state can be used to study the effects of a mutation on the activation free energy for any enzymatic reaction.

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Section: Introductionmentioning

confidence: 99%

Free Energy Perturbation (FEP) Simulation on the Transition States of Cocaine Hydrolysis Catalyzed by Human Butyrylcholinesterase and Its Mutants

et al. 2007

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“…[36][37][38][39] Janda et al 20 desarrollaron el bacteriófago GNC92H2-p-VIII, al cual se le modificaron las proteínas de superficie pVIII, con el fin de generar una especie de malla esponjosa capaz de capturar las moléculas de cocaína dentro del SNC. La inmunización (dos veces diariamente) de ratas, vía intranasal con el bacteriófago, atenuó significativamente la actividad locomotora, pero sólo para dosis bajas o medias de cocaína.…”

Section: 31unclassified

Inmunoprotección activa contra cocaína

Salazar-Juárez

Méndez

Jurado

et al. 2015

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IntroductionThe classic pharmacopoeia used to attenuate cocaine dependence has proved a poor therapeutic efficacy. Based on this discouraging clinical and therapeutic panorama, since more than a decade, various researchers have developed new therapeutic strategies against cocaine addiction. These new experimental strategies are based on the structural design and synthesis of therapeutic vaccine formulations against cocaine addiction. ObjectiveTo describe the development and therapeutic evaluation of active immunization against cocaine. MethodA bibliographical search was made using PubMed, using as descriptors the words "Cocaine" and "Vaccine." 155 articles were obtained which were used for these review 46 items. ResultsAt preclinical level, active vaccination generates high levels of antibodies capable of recognizing with high specificity the cocaine present in the bloodstream, which attenuates the behavioral changes induced by different doses of cocaine. Discussion and conclusionPreclinical and clinical results have reinforced "proof of concept" active therapeutic vaccination to pharmacological control to cocaine use relapse in humans, but gave guidelines to the postulation and justification of synthesizing new models of anti-cocaine vaccines for human use.This experimental pharmacological strategy of "immunoprotective" nature has proven an effective treatment that significantly reduces drug-seeking behaviors, both at pre-clinical levels in the rodent model as well as in humans.Key words: Addiction, cocaine, active immune-protection, antibodies and pharmacotherapies. RESUMEN IntroducciónLa farmacopea clásica, empleada para atenuar la dependencia a ciertas drogas de abuso ilegal, como la cocaína, ha demostrado una pobre eficacia terapéutica. Basado en este desalentador panorama clínico-terapéutico, desde hace más de una década diversos investigadores han desarrollado nuevas estrategias terapéuticas contra la adicción a la cocaína. Estas nuevas estrategias experimentales están basadas en el diseño y la síntesis de formulaciones estructurales de vacunas terapéuticas contra la adicción a la cocaína. ObjetivoRealizar una descripción del desarrollo y la validación terapéutica de la inmunización activa contra la cocaína. MétodoSe realizó una búsqueda bibliográfica con el uso del PubMed, usando como descriptores las palabras "Cocaine" y "Vaccine". Se obtuvieron 155 artículos, de los cuales se usaron 46 para esta revisión. ResultadosA nivel preclínico, la vacunación activa genera altos niveles de anticuerpos capaces de reconocer con alta especificidad a la cocaína dentro del torrente sanguíneo, atenuando las alteraciones conductuales inducidas por diversas dosis de cocaína. Discusión y conclusiónLos resultados preclínicos y clínicos han reforzado "la prueba de concepto" terapéutica de la vacunación activa para el control farmacoló-gico de la recaída al consumo adictivo de la cocaína en el humano, sin embargo, dieron pauta a la postulación y a la justificación de sintetizar nuevos modelos de uso humano de vacuna...

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“…21,22 Como resultado de esta alteración significativa de "antagonismo farmacológico de permeación hematoencefálica de la droga", el valor reforzante placentero que ésta induce disminuye notablemente, lo cual reduce el porcentaje de recaídas al consumo 21,22 (figura 1). Esta estrategia farmacológica experimental de naturaleza "inmunoprotectora" ha demostrado ser un tratamiento con eficacia terapéutica para atenuar significativamente y/o inhibir las conductas de búsqueda y consumo adictivo a la cocaína, la nicotina y la morfina/heroína, tanto al nivel preclínico en el roedor [23][24][25][26][27][28][29][30][31][32] como en el humano. 33,34 Además es importante resaltar que dada la naturaleza del mecanismo farmacocinético antes descrito, relacionado con los efectos de la droga, al disminuirse significativamente la permeación de la droga hacia el tejido cerebral se bloquean los efectos reforzadores que induce la droga a nivel central, y además no se producen los efectos secundarios tóxicos colaterales generados a menudo con los fármacos clásicos empleados comúnmente contra los procesos de adicción.…”

Section: Inmunofarmacoterapiasunclassified

Nuevas vacunas contra la morfina-heroína

Salazar-Juárez¹,

Méndez²,

Alonso³

et al. 2013

Salud Ment

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SUMMARYDrug addiction is one of the most important health problems in the world. This psychiatry disease results in the death of about 500 000 individuals annually in the world. Despite this scenario, the development of effective drug therapies against this disease has been slow and not very successful. In recent years, new alternative pharmacological strategies against drug addiction have been designed and validated. Among them are vaccines against drugs like nicotine, morphine or cocaine and their subsequent use in immunotherapeutic pharmacological procedures for the treatment of addictive behaviors of drug consumption, both in animal models and in humans.These strategies are based on the experimental design and synthesis of various structural formulations of therapeutic vaccines against drugs of abuse. When dosed in active immunization schedules, they induce the production of specific antibodies, which recognize and bind these substances in the intravascular space and prevent the drug permeability through the blood brain barrier, resulting in decreased effects of drugs into the brain.In 2006, our research group at the National Institute of Psychiatry Ramón de la Fuente Muñiz (INPRFM) achieved and consolidated the design, synthesis, application and validation of immunoprotective therapeutic effects against relapse to morphine/heroin addiction in a rodent animal model, a model vaccine for potential human use against addiction to morphine/heroin. This model shows immunogenic capacities (high and sustained titers of highly specific antibodies) and immunoprotection (attenuates the effect up to 15mg/kg sc morphine) that the structural vaccine models competing have not been matched, which makes it the leading vaccine model against the addictive effects of heroin and morphine.Key words: Addiction, morphine/heroin, vaccines, immunotherapy, active and passive immunization. RESUMENLa adicción a una droga de abuso representa uno de los problemas sanitarios más importantes ya que esta patología genera la muerte de cerca de 500 000 sujetos anualmente en el mundo. A pesar de este panorama, el desarrollo de terapias farmacológicas efectivas contra esta enfermedad es lento y poco exitoso. En los últimos años se han diseñado y validado nuevas estrategias farmacológicas alternativas contra la adicción a drogas de abuso, como las vacunas y su uso en procedimientos farmacológicos inmunoterapéuticos para el tratamiento de esas conductas tanto en modelos de animales como en el humano.Estas nuevas estrategias experimentales están basadas en el diseño y síntesis de diversas formulaciones estructurales de vacunas terapéuticas contra las sustancias de abuso las cuales, al ser dosificadas en esquemas de inmunización activa, inducen la producción de anticuerpos séricos específicos que reconocen y se unen a estas sustancias en el espacio intravascular sistémico e impiden que crucen la barrera hematoencefálica, con lo cual disminuyen sus efectos en el cerebro.En el año 2006 nuestro grupo de trabajo en el Instituto Nacional de Psiquiatría R...

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Treating cocaine addiction with viruses

Cited by 102 publications

References 46 publications

Free Energy Perturbation (FEP) Simulation on the Transition States of Cocaine Hydrolysis Catalyzed by Human Butyrylcholinesterase and Its Mutants

Free Energy Perturbation (FEP) Simulation on the Transition States of Cocaine Hydrolysis Catalyzed by Human Butyrylcholinesterase and Its Mutants

Inmunoprotección activa contra cocaína

Nuevas vacunas contra la morfina-heroína

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