Úloha adrenergního systému v genetické hypertenzi / The role of adrenergic system in genetic hypertension

Loučková, Anna

January 2013

The adrenergic system plays an important role in the regulation of blood pressure. In the spontaneously hypertensive rat, the most studied model of essential hypertension, many components of the adrenergic system are altered. Changes in expression level of any catecholamine biosynthetic enzymes or any adrenergic receptor subtypes could be one of the causes of hypertension development. In this work, the expression of adrenergic system genes was measured in adrenal gland, renal cortex and renal medulla of the spontaneously hypertensive (SHR), Wistar-Kyoto and Brown Norway rats at the age of thirteen weeks. In adrenal gland of SHR, all four catecholamine biosynthetic enzymes (tyrosine hydroxylase, DOPA decarboxylase, dopamine β-hydroxylase and phenylethanolamine-N- methyltransferase) and almost all subtypes of adrenergic receptors (with the exception of Adra1a and Adra1d) were underexpressed. This generally decreased expression in adrenal gland of SHR suggests that at least a part of regulation of adrenergic system gene expression is common. The mechanism of this downregulation in SHR could be a negative feedback through adrenergic receptors stimulated by high plasma noradrenaline concentration. In the kidney of SHR, there were no differences in the expression of most of adrenergic receptor subtypes with the...

Homology modeling and structural analysis of the antipsychotic drugs receptorome

López Muñoz, Laura

22 June 2010

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)

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