Global ETD Search

31	The Involvement of Ventral Tegmental Area Dopamine and CRF Activity in Mediating the Opponent Motivational Effects of Acute and Chronic Nicotine Grieder, Taryn Elizabeth 12 December 2012 (has links) A fundamental question in the neurobiological study of drug addiction concerns the mechanisms mediating the motivational effects of chronic drug withdrawal. According to one theory, drugs of abuse activate opposing motivational processes after both acute and chronic drug use. The negative experience of withdrawal is the opponent process of chronic drug use that drives relapse to drug-seeking and -taking, making the identification of the neurobiological substrates mediating withdrawal an issue of central importance in addiction research. In this thesis, I identify the involvement of the neurotransmitters dopamine (DA) and corticotropin-releasing factor (CRF) in the opponent motivational a- and b-processes occurring after acute and chronic nicotine administration. I report that acute nicotine stimulates an initial aversive a-process followed by a rewarding opponent b-process, and chronic nicotine stimulates a rewarding a-process followed by an aversive opponent b-process (withdrawal). These responses can be modeled using a place conditioning paradigm. I demonstrate that the acute nicotine a-process is mediated by phasic dopaminergic activity and the DA receptor subtype-1 (D1R) but not by tonic dopaminergic activity and the DA receptor subtype-2 (D2R) or CRF activity, and the opponent b-process is neither DA- nor CRF-mediated. I also demonstrate that the chronic nicotine a-process is DA- but not CRF-mediated, and that withdrawal from chronic nicotine (the b-process) decreases tonic but not phasic DA activity in the ventral tegmental area (VTA), an effect that is D2R- but not D1R-mediated. I show that a specific pattern of signaling at D1Rs and D2Rs mediates the motivational responses to acute nicotine and chronic nicotine withdrawal, respectively, by demonstrating that both increasing or decreasing signaling at these receptors prevents the expression of the conditioned motivational response. Furthermore, I report that the induction of nicotine dependence increases CRF mRNA in VTA DA neurons, and that blocking either the upregulation of CRF mRNA or the activation of VTA CRF receptors prevents the anxiogenic and aversive motivational responses to withdrawal from chronic nicotine. The results described in this thesis provide novel evidence of a VTA DA/CRF system, and demonstrate that both CRF and a specific pattern of tonic DA activity in the VTA are necessary for the aversive motivational experience of nicotine withdrawal. nicotine dopamine withdrawal conditioned place aversion opponent process theory of motivation corticotropin-releasing factor motivation D1 receptor D2 receptor neuropharmacology phasic dopamine drug addiction tonic dopamine ventral tegmental area Neuroscience 0317
32	Bedeutung einer Beeinträchtigung der D2- und D3-vermittelten dopaminergen Transmission für die motorische Aktivität und das motorische Lernverhalten im Mausmodell / The significance of an impairment of the D2-/D3-mediated dopaminergic transmission for motor activity and motor learning in mice Hasan, Kenan 29 June 2015 (has links) No description available. 610 Dopamin Motorisches Lernen D2-Rezeptor D3-Rezeptor Laufrad motor learning dopamine d2 receptor d3 receptor running wheel
33	The Involvement of Ventral Tegmental Area Dopamine and CRF Activity in Mediating the Opponent Motivational Effects of Acute and Chronic Nicotine Grieder, Taryn Elizabeth 12 December 2012 (has links) A fundamental question in the neurobiological study of drug addiction concerns the mechanisms mediating the motivational effects of chronic drug withdrawal. According to one theory, drugs of abuse activate opposing motivational processes after both acute and chronic drug use. The negative experience of withdrawal is the opponent process of chronic drug use that drives relapse to drug-seeking and -taking, making the identification of the neurobiological substrates mediating withdrawal an issue of central importance in addiction research. In this thesis, I identify the involvement of the neurotransmitters dopamine (DA) and corticotropin-releasing factor (CRF) in the opponent motivational a- and b-processes occurring after acute and chronic nicotine administration. I report that acute nicotine stimulates an initial aversive a-process followed by a rewarding opponent b-process, and chronic nicotine stimulates a rewarding a-process followed by an aversive opponent b-process (withdrawal). These responses can be modeled using a place conditioning paradigm. I demonstrate that the acute nicotine a-process is mediated by phasic dopaminergic activity and the DA receptor subtype-1 (D1R) but not by tonic dopaminergic activity and the DA receptor subtype-2 (D2R) or CRF activity, and the opponent b-process is neither DA- nor CRF-mediated. I also demonstrate that the chronic nicotine a-process is DA- but not CRF-mediated, and that withdrawal from chronic nicotine (the b-process) decreases tonic but not phasic DA activity in the ventral tegmental area (VTA), an effect that is D2R- but not D1R-mediated. I show that a specific pattern of signaling at D1Rs and D2Rs mediates the motivational responses to acute nicotine and chronic nicotine withdrawal, respectively, by demonstrating that both increasing or decreasing signaling at these receptors prevents the expression of the conditioned motivational response. Furthermore, I report that the induction of nicotine dependence increases CRF mRNA in VTA DA neurons, and that blocking either the upregulation of CRF mRNA or the activation of VTA CRF receptors prevents the anxiogenic and aversive motivational responses to withdrawal from chronic nicotine. The results described in this thesis provide novel evidence of a VTA DA/CRF system, and demonstrate that both CRF and a specific pattern of tonic DA activity in the VTA are necessary for the aversive motivational experience of nicotine withdrawal. nicotine dopamine withdrawal conditioned place aversion opponent process theory of motivation corticotropin-releasing factor motivation D1 receptor D2 receptor neuropharmacology phasic dopamine drug addiction tonic dopamine ventral tegmental area Neuroscience 0317
34	Efeitos a longo prazo de diferentes separações dos filhotes no período neonatal sobre as genitoras Toigo, Eduardo von Poser January 2011 (has links) Esse estudo foi realizado para verificar se a exposição a separações repetidas (por diferentes intervalos de tempo) de mães dos seus filhotes no período neonatal poderiam ser classificadas como indutoras de um estado do tipo deprimido em genitoras. Sessenta ratas Wistar prenhes foram divididas em 3 grupos: controle, separação por 10 minutos e separação por 3 horas. As intervenções neonatais foram realizadas nos dias 1-10 pós parto. Após o desmame as genitoras foram submetidas ao teste do nado forçado, ao teste do labirinto em cruz elevado e ao teste do odor de predador. Também foi avaliado o comportamento alimentar e os padrões de reatividade a um sabor doce e a um sabor amargo. Foi medido os níveis de ocitocina no líquido cefaloraquidiano, corticosterona plasmática e atividade hipocampal Na+, K+-ATPase, assim como a atividade das enzimas antioxidantes catalase, glutationa peroxidase, superoxido dismutase, produção de radicais livres, e a produção de óxido nítrico, além dos níveis dos receptores A2A de adenosina e D2 de dopamina no estriado dorsoventral e no hipocampo. Foi observado que somente a separação por 3 h induziu um aumento significativo no tempo de imobilidade no teste do nado forçado, o que é consistente com estudos prévios. A atividade hipocampal da Na+, K+-ATPase se mostrou diminuída no grupo separado por 10 minutos e mais significativamente diminuída nas genitoras submetidas a separação por 3 horas de seus filhotes. Adicionalmente, os níveis de ocitocina no líquido cefaloraquidiano se encontravam aumentados no grupo separado por 10 minutos, o que pode estar relacionado a um aumento no cuidado materno, induzido por esta manipulação dos filhotes, por parte das genitoras, como reportado na literatura. Uma redução nos níveis de óxido nítrico no hipocampo das genitoras separadas por 3 horas foi observado Nessas genitoras também foi verificado um aumento no comportamento de risco, uma diminuição no sentimento prazeroso frente a uma solução doce e aumento na sensibilidade a uma solução aversiva, o que é congruente a um perfil de estado do tipo deprimido. Além disso, nós verificamos uma diminuição na quantidade do receptor de dopamina D2 no estriado das mães submetidas a separação por 3 horas dos filhotes, o que poderia ser relacionado com uma diminuição no prazer (anedonia) que acontece na depressão. Conclui-se que a retirada dos filhotes das mães por longos períodos tornam essas mães mais susceptíveis ao desenvolvimento de características depressivas. / This study was carried out to ascertain whether exposure to repeated separations (different times) of mothers from their pups in the neonatal period could be classified as an induction of a depressive-like state in dams. Sixty Wistar rats were divided into 3 groups: control, brief separation and long-term separation. The neonatal interventions were done on postpartum days 1-10. After weaning, the dams were subjected to the forced swimming test, elevated plus maze and predator odor test. It was also evaluated the feeding behavior and the taste reactivity patterns to a sweet and to a bitter solution. It was mesaured cerebral spinal fluid oxytocin, plasma corticosterone, and hippocampal Na+, K+-ATPase activity, as well as the activity of the antioxidant enzymes catalase, glutathione peroxidase, superoxide dismutase, free radicals production, and the production of nitric oxide and the levels of adenosine A2A and dopamine D2 receptors in the dorsoventral striatum and hippocampus. It was observed that only the 3 h separation induced a significant increase in the immobility time of rats in the forced swimming test, which is consistent with previous studies. Hippocampal Na+, K+-ATPase activity was decreased in the brief separated group and more significantly decreased in dams subjected to 3h separation from their pups. Additionally, cerebral spinal fluid oxytocin was increased in dams of the brief separated group, which may be related to the increased handled-induced maternal care, as reported in the literature. A reduction in nitric oxide levels in the hippocampus in dams of the long separated group was also observed. It was also verify an increase in the risk-taking behavior by the 3h separated mothers. The 3h separated mother also demonstrated a diminished feeling of pleasure with a sucrose solution and a increased sensibility to a aversive solution, wich is congruent with a depressive like state profile. Furthermore, we shown a decrease in the dopamine D2 receptor quantity in the striatum of the 3 h separated mothers, wich could be related to a decrease in pleasure feeling (anhedonia) experienced in depression. It is concluded that the withdrawal of pups from their mothers for long periods make the mothers more susceptible to the development of depressive features. Manipulação neonatal Comportamento animal Ocitocina Estresse oxidativo Depressão Neonatal separation Oxytocin Forced swimming test Na+ K+-ATPase Nitric oxide Dopamine D2 receptor Adenosine A2A receptor Risk-taking behavior Plus-maze Predator odor test Taste reactivity paradigm
35	Efeitos a longo prazo de diferentes separações dos filhotes no período neonatal sobre as genitoras Toigo, Eduardo von Poser January 2011 (has links) Esse estudo foi realizado para verificar se a exposição a separações repetidas (por diferentes intervalos de tempo) de mães dos seus filhotes no período neonatal poderiam ser classificadas como indutoras de um estado do tipo deprimido em genitoras. Sessenta ratas Wistar prenhes foram divididas em 3 grupos: controle, separação por 10 minutos e separação por 3 horas. As intervenções neonatais foram realizadas nos dias 1-10 pós parto. Após o desmame as genitoras foram submetidas ao teste do nado forçado, ao teste do labirinto em cruz elevado e ao teste do odor de predador. Também foi avaliado o comportamento alimentar e os padrões de reatividade a um sabor doce e a um sabor amargo. Foi medido os níveis de ocitocina no líquido cefaloraquidiano, corticosterona plasmática e atividade hipocampal Na+, K+-ATPase, assim como a atividade das enzimas antioxidantes catalase, glutationa peroxidase, superoxido dismutase, produção de radicais livres, e a produção de óxido nítrico, além dos níveis dos receptores A2A de adenosina e D2 de dopamina no estriado dorsoventral e no hipocampo. Foi observado que somente a separação por 3 h induziu um aumento significativo no tempo de imobilidade no teste do nado forçado, o que é consistente com estudos prévios. A atividade hipocampal da Na+, K+-ATPase se mostrou diminuída no grupo separado por 10 minutos e mais significativamente diminuída nas genitoras submetidas a separação por 3 horas de seus filhotes. Adicionalmente, os níveis de ocitocina no líquido cefaloraquidiano se encontravam aumentados no grupo separado por 10 minutos, o que pode estar relacionado a um aumento no cuidado materno, induzido por esta manipulação dos filhotes, por parte das genitoras, como reportado na literatura. Uma redução nos níveis de óxido nítrico no hipocampo das genitoras separadas por 3 horas foi observado Nessas genitoras também foi verificado um aumento no comportamento de risco, uma diminuição no sentimento prazeroso frente a uma solução doce e aumento na sensibilidade a uma solução aversiva, o que é congruente a um perfil de estado do tipo deprimido. Além disso, nós verificamos uma diminuição na quantidade do receptor de dopamina D2 no estriado das mães submetidas a separação por 3 horas dos filhotes, o que poderia ser relacionado com uma diminuição no prazer (anedonia) que acontece na depressão. Conclui-se que a retirada dos filhotes das mães por longos períodos tornam essas mães mais susceptíveis ao desenvolvimento de características depressivas. / This study was carried out to ascertain whether exposure to repeated separations (different times) of mothers from their pups in the neonatal period could be classified as an induction of a depressive-like state in dams. Sixty Wistar rats were divided into 3 groups: control, brief separation and long-term separation. The neonatal interventions were done on postpartum days 1-10. After weaning, the dams were subjected to the forced swimming test, elevated plus maze and predator odor test. It was also evaluated the feeding behavior and the taste reactivity patterns to a sweet and to a bitter solution. It was mesaured cerebral spinal fluid oxytocin, plasma corticosterone, and hippocampal Na+, K+-ATPase activity, as well as the activity of the antioxidant enzymes catalase, glutathione peroxidase, superoxide dismutase, free radicals production, and the production of nitric oxide and the levels of adenosine A2A and dopamine D2 receptors in the dorsoventral striatum and hippocampus. It was observed that only the 3 h separation induced a significant increase in the immobility time of rats in the forced swimming test, which is consistent with previous studies. Hippocampal Na+, K+-ATPase activity was decreased in the brief separated group and more significantly decreased in dams subjected to 3h separation from their pups. Additionally, cerebral spinal fluid oxytocin was increased in dams of the brief separated group, which may be related to the increased handled-induced maternal care, as reported in the literature. A reduction in nitric oxide levels in the hippocampus in dams of the long separated group was also observed. It was also verify an increase in the risk-taking behavior by the 3h separated mothers. The 3h separated mother also demonstrated a diminished feeling of pleasure with a sucrose solution and a increased sensibility to a aversive solution, wich is congruent with a depressive like state profile. Furthermore, we shown a decrease in the dopamine D2 receptor quantity in the striatum of the 3 h separated mothers, wich could be related to a decrease in pleasure feeling (anhedonia) experienced in depression. It is concluded that the withdrawal of pups from their mothers for long periods make the mothers more susceptible to the development of depressive features. Manipulação neonatal Comportamento animal Ocitocina Estresse oxidativo Depressão Neonatal separation Oxytocin Forced swimming test Na+ K+-ATPase Nitric oxide Dopamine D2 receptor Adenosine A2A receptor Risk-taking behavior Plus-maze Predator odor test Taste reactivity paradigm
36	Efeitos a longo prazo de diferentes separações dos filhotes no período neonatal sobre as genitoras Toigo, Eduardo von Poser January 2011 (has links) Esse estudo foi realizado para verificar se a exposição a separações repetidas (por diferentes intervalos de tempo) de mães dos seus filhotes no período neonatal poderiam ser classificadas como indutoras de um estado do tipo deprimido em genitoras. Sessenta ratas Wistar prenhes foram divididas em 3 grupos: controle, separação por 10 minutos e separação por 3 horas. As intervenções neonatais foram realizadas nos dias 1-10 pós parto. Após o desmame as genitoras foram submetidas ao teste do nado forçado, ao teste do labirinto em cruz elevado e ao teste do odor de predador. Também foi avaliado o comportamento alimentar e os padrões de reatividade a um sabor doce e a um sabor amargo. Foi medido os níveis de ocitocina no líquido cefaloraquidiano, corticosterona plasmática e atividade hipocampal Na+, K+-ATPase, assim como a atividade das enzimas antioxidantes catalase, glutationa peroxidase, superoxido dismutase, produção de radicais livres, e a produção de óxido nítrico, além dos níveis dos receptores A2A de adenosina e D2 de dopamina no estriado dorsoventral e no hipocampo. Foi observado que somente a separação por 3 h induziu um aumento significativo no tempo de imobilidade no teste do nado forçado, o que é consistente com estudos prévios. A atividade hipocampal da Na+, K+-ATPase se mostrou diminuída no grupo separado por 10 minutos e mais significativamente diminuída nas genitoras submetidas a separação por 3 horas de seus filhotes. Adicionalmente, os níveis de ocitocina no líquido cefaloraquidiano se encontravam aumentados no grupo separado por 10 minutos, o que pode estar relacionado a um aumento no cuidado materno, induzido por esta manipulação dos filhotes, por parte das genitoras, como reportado na literatura. Uma redução nos níveis de óxido nítrico no hipocampo das genitoras separadas por 3 horas foi observado Nessas genitoras também foi verificado um aumento no comportamento de risco, uma diminuição no sentimento prazeroso frente a uma solução doce e aumento na sensibilidade a uma solução aversiva, o que é congruente a um perfil de estado do tipo deprimido. Além disso, nós verificamos uma diminuição na quantidade do receptor de dopamina D2 no estriado das mães submetidas a separação por 3 horas dos filhotes, o que poderia ser relacionado com uma diminuição no prazer (anedonia) que acontece na depressão. Conclui-se que a retirada dos filhotes das mães por longos períodos tornam essas mães mais susceptíveis ao desenvolvimento de características depressivas. / This study was carried out to ascertain whether exposure to repeated separations (different times) of mothers from their pups in the neonatal period could be classified as an induction of a depressive-like state in dams. Sixty Wistar rats were divided into 3 groups: control, brief separation and long-term separation. The neonatal interventions were done on postpartum days 1-10. After weaning, the dams were subjected to the forced swimming test, elevated plus maze and predator odor test. It was also evaluated the feeding behavior and the taste reactivity patterns to a sweet and to a bitter solution. It was mesaured cerebral spinal fluid oxytocin, plasma corticosterone, and hippocampal Na+, K+-ATPase activity, as well as the activity of the antioxidant enzymes catalase, glutathione peroxidase, superoxide dismutase, free radicals production, and the production of nitric oxide and the levels of adenosine A2A and dopamine D2 receptors in the dorsoventral striatum and hippocampus. It was observed that only the 3 h separation induced a significant increase in the immobility time of rats in the forced swimming test, which is consistent with previous studies. Hippocampal Na+, K+-ATPase activity was decreased in the brief separated group and more significantly decreased in dams subjected to 3h separation from their pups. Additionally, cerebral spinal fluid oxytocin was increased in dams of the brief separated group, which may be related to the increased handled-induced maternal care, as reported in the literature. A reduction in nitric oxide levels in the hippocampus in dams of the long separated group was also observed. It was also verify an increase in the risk-taking behavior by the 3h separated mothers. The 3h separated mother also demonstrated a diminished feeling of pleasure with a sucrose solution and a increased sensibility to a aversive solution, wich is congruent with a depressive like state profile. Furthermore, we shown a decrease in the dopamine D2 receptor quantity in the striatum of the 3 h separated mothers, wich could be related to a decrease in pleasure feeling (anhedonia) experienced in depression. It is concluded that the withdrawal of pups from their mothers for long periods make the mothers more susceptible to the development of depressive features. Manipulação neonatal Comportamento animal Ocitocina Estresse oxidativo Depressão Neonatal separation Oxytocin Forced swimming test Na+ K+-ATPase Nitric oxide Dopamine D2 receptor Adenosine A2A receptor Risk-taking behavior Plus-maze Predator odor test Taste reactivity paradigm
37	The Effects of Nicotine Conditioned Place Preference in D2 Primed Adolescent Rats: Age-Related and Gender Effects. Ogawa, Yoko Emily 14 August 2007 (has links) (PDF) This study investigated nicotine conditioned place preference (CPP) in two different ages of adolescence using a rodent model of schizophrenia. Both 2- and 3-chambered CPP apparatuses were used to test whether the CPP was due to an aversion to the white chamber. Animals were neontally treated with the dopamine D2/D3 agonist, quinpirole, or saline and raised to either early postweanling age (P 22) or adolescence (P 29). Rats were conditioned to prefer the white chamber using nicotine. Results showed that nicotine induced CPP and appeared to alleviate an increased stress response in D2 primed animals, which appeared to diminish over time. Additionally, adult D2 and non-D2 primed rats were tested on the elevated T-maze. Results revealed that D2 primed rats demonstrated a significant increase in unconditioned fear. This study showed that nicotine induced CPP in D2 and non-D2 primed rats regardless of age, and D2 primed rats appear to demonstrate an increase in stress levels that was alleviated by nicotine. Schizophrenia Quinpirole Nicotine Elevated T-Maze (ETM) D2 Receptor Supersensitization Conditioned Place Preference (CPP) Adolescence Early Postweanling Age Chemical Actions and Uses Chemicals and Drugs Medicine and Health Sciences Mental Disorders Psychiatry and Psychology
38	PAOPA, a potent dopamine D2 receptor allosteric modulator, prevents and reverses behavioural and biochemical abnormalities in an amphetamine-sensitized preclinical animal model of schizophrenia. Beyaert, Michael G.R. 10 1900 (has links) <p>Allosteric modulators are emerging as a new class of therapeutics for the treatment of complex disorders, including psychiatric illnesses such as schizophrenia. The disease is marked by hyperdopaminergic signaling in the striatum, which plays a role in the development of positive symptoms like delusions, hallucinations, and paranoia. Conventional antipsychotic drug therapy typically employs dopamine D2 receptor antagonists that compete with endogenous dopamine at the orthosteric, or dopamine-binding site, in an attempt to normalize these psychotic symptoms. However, they are often associated with adverse motor and metabolic side effects. Furthermore, only some antipsychotic drugs are able to treat the negative symptoms of schizophrenia, which include social withdrawal and anhedonia, and there is currently no treatment for the cognitive impairment associated with the disease.</p> <p>Allosteric modulators are safer alternatives to conventional orthosteric therapeutics as they interact with their receptor at a novel binding site and their mechanism involves modulation of endogenous signaling. Therefore, levels of endogenous ligand limit the activity of an allosteric modulator. Our lab has synthesized and evaluated over 185 compounds for their activity at the dopamine D2 receptor. Of these compounds, PAOPA is the most potent allosteric modulator, and has been shown to be effective in treating the MK-801 induced preclinical animal model of schizophrenia without causing the adverse effects induced by currently prescribed antipsychotic drugs. The objective of this study was to evaluate PAOPA’s ability to treat behavioural abnormalities in an amphetamine-sensitized model of schizophrenia.</p> <p>Four groups (n=10/group) of male Sprague Dawley rats received intraperitoneal injections three days per week on alternate days over three weeks. Group A received saline, group B received D-amphetamine (1mg/kg during week one, 2mg/kg during week two, 3mg/kg during week three), group C received PAOPA (1mg/kg), and group D received the same doses of amphetamine as group B with PAOPA (1mg/kg). Following a three-week withdrawal, each group was tested for prepulse inhibition, social interaction, and locomotor activity. Amphetamine-sensitized rats were subjected to the same tests following PAOPA administration (1mg/kg). To assess whether behavioural changes were associated with changes in brain chemistry, post-mortem dopamine levels were measured in the striatum, nucleus accumbens, and medial prefrontal cortex. Data were analyzed by one-way ANOVA or paired t test where appropriate.</p> <p>Amphetamine sensitization induced schizophrenic-like behavioural abnormalities, including deficits in prepulse inhibition and social interaction, as well as increased locomotor activity and sensitivity to amphetamine challenge. Concurrent amphetamine and PAOPA treatment prevented all amphetamine- induced behavioural abnormalities. Furthermore, amphetamine-induced deficits in prepulse inhibition and social interaction were reversed one hour following PAOPA treatment. PAOPA treatment alone had no effect on behaviour or post-mortem striatal dopamine. Behavioural changes in amphetamine-sensitized rats were accompanied by a reduction in post-mortem striatal dopamine levels. In correlation with behavioural results, PAOPA administration during amphetamine sensitization prevented this biochemical change.</p> <p>These results demonstrate that PAOPA can prevent and reverse behavioural and associated biochemical abnormalities in amphetamine-sensitized rats. PAOPA is a candidate for the development of treatments for schizophrenia.</p> / Master of Science (MSc) schizophrenia dopamine dopamine D2 receptor allosteric modulator amphetamine PAOPA Amino Acids, Peptides, and Proteins Behavior and Behavior Mechanisms Chemical and Pharmacologic Phenomena Medical Biochemistry Medical Pharmacology Medicinal and Pharmaceutical Chemistry Mental Disorders Neurosciences Pharmaceutical Preparations Substance Abuse and Addiction Amino Acids, Peptides, and Proteins
39	Homology modeling and structural analysis of the antipsychotic drugs receptorome López Muñoz, Laura 22 June 2010 (has links) Classically it was assumed that the compounds with therapeutic effect exert their action interacting with a single receptor. Nowadays it is widely recognized that the pharmacological effect of most drugs is more complex and involves a set of receptors, some associated to their positive effects and some others to the side effects and toxicity. Antipsychotic drugs are an example of effective compounds characterized by a complex pharmacological profile binding to several receptors (mainly G protein-coupled-receptors, GPCR). In this work we will present a detailed study of known antipsychotic drugs and the receptors potentially involved in their binding profile, in order to understand the molecular mechanisms of the antipsychotic pharmacologic effects.The study started with obtaining homology models for all the receptors putatively involved in the antipsychotic drugs receptorome, suitable for building consistent drug-receptor complexes. These complexes were structurally analyzed and compared using multivariate statistical methods, which in turn allowed the identification of the relationship between the pharmacological properties of the antipsychotic drugs and the structural differences in the receptor targets. The results can be exploited for the design of safer and more effective antipsychotic drugs with an optimum binding profile. / Tradicionalmente se asumía que los fármacos terapéuticamente efectivos actuaban interaccionando con un único receptor. Actualmente está ampliamente reconocido que el efecto farmacológico de la mayoría de los fármacos es más complejo y abarca a un conjunto de receptores, algunos asociados a los efectos terapéuticos y otros a los secundarios y toxicidad. Los fármacos antipsicóticos son un ejemplo de compuestos eficaces que se caracterizan por unirse a varios receptores simultáneamente (principalmente a receptores unidos a proteína G, GPCR). El trabajo de la presente tesis se ha centrado en el estudio de los mecanismos moleculares que determinan el perfil de afinidad de unión por múltiples receptores de los fármacos antipsicóticos.En primer lugar se construyeron modelos de homología para todos los receptores potencialmente implicados en la actividad farmacológica de dichos fármacos, usando una metodología adecuada para construir complejos fármaco-receptor consistentes. La estructura de estos complejos fue analizada y se llevó a cabo una comparación mediante métodos estadísticos multivariantes, que permitió la identificación de asociaciones entre la actividad farmacológica de los fármacos antipsicóticos y diferencias estructurales de los receptores diana. Los resultados obtenidos tienen interés para ser explotados en el diseño de fármacos antipsicóticos con un perfil farmacológico óptimo, más seguros y eficaces. Receptor 5-HT2A Receptor D3 Receptor D2 Ligando Clozapina Derivados Benzofuranonas Risperidona Olanzapina esquizofrenia métodos de regresión campos de interacción Molecular (MIF) Perfil Multireceptorial modelado por homología Docking sitio de unión interacciones moleculares selectividad afinidad de unión Diana Meta-Diana efectos secundarios fármaco antipsicótico típico fármaco antipsicótico atípico agonista antagonista membrana receptoroma rhodopsina estructura de rayos X descriptores moleculares farmacología análisis multivariante procedimiento integrado Computer-aided drug design Integrated approach Multivariate analysis Pharmacology Molecular descriptors X-ray structure Rhodopsin Receptorome Membrane Antagonist Agonist Atypical antipsychotic drug Typical antipsychotic drug Side effects Off-target Target Selectivity Binding affinity Molecular interactions Binding site Homology modeling Docking Multireceptor profile Molecular interaction Field (MIF) Partial Least Squares (PLS) Principal Component Analysis (PCA) Schizophrenia Benzolactam Derivatives Benzofuranone Derivatives Risperidone Olanzapine Clozapine Ligand Adrenergic receptors Muscarinic receptors Histamine receptors Serotonin receptors Dopamine receptors beta2-Adrenergic receptor D2 receptor D3 receptor 5-HT2A receptor G protein-coupled receptors (GPCR) 57

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