Efeitos neuroprotetores do 4'-clorodiazepam em modelos experimentais de Doença de Alzheimer in vitro e sobre o desenvolvimento neuronal

Arbo, Bruno Dutra

January 2016

O aumento da expectativa de vida da população mundial tem se associado com uma maior prevalência de doenças neurodegenerativas. A Doença de Alzheimer (DA) é a doença neurodegenerativa mais comum e a principal causa de demência em indivíduos com mais de 60 anos, sendo caracterizada por um declínio progressivo na memória e função mental dos pacientes. Esses sintomas são acompanhados por alterações histopatológicas no cérebro desses indivíduos, incluindo a presença de uma grande quantidade de placas senis, formadas pela deposição do peptídeo beta-amiloide (Aβ), e de emaranhados neurofibrilares formados pela hiperfosforilação da proteína Tau. Estudos indicam que a deposição do Aβ é uma das principais responsáveis pelo desenvolvimento da DA, causando dano neuronal através da ativação de várias vias pró-apoptóticas e dando origem aos sintomas de demência típicos dessa doença. Até o momento, não existem tratamentos eficazes para o combate à DA, de forma que a maior parte das intervenções farmacológicas é destinada apenas ao tratamento de alguns de seus sintomas. A proteína translocadora (TSPO) se localiza em pontos de contato entre as membranas mitocondriais interna e externa e está relacionada com o transporte de colesterol para o interior da mitocôndria e com a regulação da esteroidogênese e da apoptose. Estudos mostram que ligantes da TSPO apresentam efeitos neuroprotetores em diferentes modelos experimentais de lesão cerebral e doenças neurodegenerativas. Especificamente em relação à DA, um estudo indicou que o 4’-clorodiazepam (4’-CD), um ligante da TSPO, apresenta efeitos neuroprotetores em um modelo animal dessa doença, sendo um possível candidato para o seu tratamento. Dessa forma, o objetivo desse estudo foi verificar o efeito neuroprotetor do 4’-CD em diferentes modelos in vitro de toxicidade induzida pelo Aβ, além de seus efeitos sobre o desenvolvimento de neurônios hipocampais. Inicialmente, demonstramos que o 4’-CD reduziu a morte celular de células SH-SY5Y expostas a um modelo de toxicidade induzida pela administração de Aβ. Esses efeitos estiveram associados com a redução da expressão da proteína pró-apoptótica Bax e com um aumento da expressão da survivina, uma proteína anti-apoptótica. A expressão das proteínas Bcl-xl e procaspase-3, por outro lado, não foi alterada pelos tratamentos. Posteriormente, estudamos os efeitos neuroprotetores do 4’-CD contra a toxicidade induzida pela administração do Aβ em culturas organotípicas de hipocampo. Nesses experimentos, foi demonstrado que o 4’-CD reduz a morte celular de culturas organotípicas de hipocampo expostas ao Aβ através de um aumento na expressão da enzima SOD, sem alterar, no entanto, a expressão das proteínas Akt e procaspase-3. Por fim, foi avaliado o efeito do 4’-CD sobre o desenvolvimento de culturas primárias de neurônios hipocampais de camundongos machos e fêmeas. Foi observado que as culturas de neurônios hipocampais das fêmeas apresentaram um desenvolvimento mais rápido do que as dos machos. O 4’-CD acelerou a maturação e aumentou a ramificação neurítica dos neurônios hipocampais dos machos, mas não exerceu qualquer efeito sobre os neurônios das fêmeas. Em suma, foi observado que o 4’-CD apresenta efeitos neuroprotetores contra o Aβ em células SH-SY5Y e em culturas organotípicas do hipocampo, apresentando-se como um fármaco em potencial para o tratamento da DA. Além disso, foi observado que o 4’-CD exerceu um efeito dependente do sexo sobre o desenvolvimento de culturas primárias de neurônios hipocampais, estimulando o desenvolvimento e a ramificação neurítica de neurônios hipocampais de machos, mas não de fêmeas. / The increase in life expectancy of the world population has been associated with a higher prevalence of neurodegenerative diseases. The Alzheimer’s Disease (AD) is the most common neurodegenerative disorder and the main cause of dementia among people over 60 years, being characterized by a progressive decline in the memory and mental function of the patients. These symptoms are associated with histopathological changes in the brain of these patients, including the presence of senile plaques, formed by the deposition of amyloid-beta (Aβ), and neurofibrillary tangles, which are related to the hyperphosphorylation of Tau protein. Studies indicate that Aβ deposition is a major contributor to AD progression, promoting neuronal damage through the activation of different pro-apoptotic pathways and giving rise to the typical dementia symptoms of this disease. To date, there are no effective treatments for AD, so that most of the pharmacological intervention is intended for the treatment of some of its symptoms. The translocator protein (TSPO) is located in contact sites between the outer and the inner mitochondrial membranes and is involved in the cholesterol transport into the mitochondria and in the regulation of steroidogenesis and apoptosis. Studies show that TSPO ligands present neuroprotective effects in different experimental models of brain injury and neurodegenerative diseases. Specifically regarding AD, a study indicated that 4’-chlorodiazepam (4’-CD), a TSPO ligand, is neuroprotective in an animal model of this disease, being a possible candidate for its treatment. Therefore, the aim of this study was to evaluate the neuroprotective effect of 4’-CD in different experimental models of Aβ- induced neurotoxicity in vitro, as well as its effects on the development of hipocampal neurons. First, it was demonstrated that 4’-CD decreased the cell death of SH-SY5Y cells exposed to the Aβ. This effect was associated with the inhibition of the Aβ-induced upregulation of Bax, a pro-apoptotic protein, and downregulation of survivin, a prosurvival protein. On the other hand, the expression of Bcl-xl and procaspase-3 was not change by the treatments. After, it was studied the neuroprotective effects of 4’-CD against Aβ in organotypic hipocampal cultures. In these experiments, it was shown that 4’-CD decreases the cell death of organotypic hippocampal slices exposed to the Aβ by increasing the protein expression of SOD, but without changing the expression of Akt and procaspase-3. Finally, due to the importance of the processes of neuronal development and maturation in the regeneration of CNS after injury, it was evaluated the effect of 4’-CD on the development of primary hippocampal neurons of male and female mice. It was observed that female primary hippocampal neurons presented an increased rate of development than male neurons. 4’-CD stimulated the development and increased the neuritic branching of male but not from female neurons. In summary, it was observed that 4’-CD presented a neuroprotective effect against Aβ in SH-SY5Y cells and in rat organotypical hippocampal slices, presenting itself as a promising agent for the treatment of AD. Also, it was observed that 4’-CD modulates the development of hippocampal neurons in a sex-dependent manner, stimulating the development of male but not from female cells.

Doenças neurodegenerativas

Doença de Alzheimer

Peptídeos beta-amilóides

Translocases mitocondriais de ADP e ATP

Diazepam

Neurônios

Hipocampo

Neuroproteção

Translocator protein (TSPO)

4’-CD

Neuroprotection

Amyloid-beta

Hippocampus

Neuritogenesis

Efeitos neuroprotetores do 4'-clorodiazepam em modelos experimentais de Doença de Alzheimer in vitro e sobre o desenvolvimento neuronal

Arbo, Bruno Dutra

January 2016

O aumento da expectativa de vida da população mundial tem se associado com uma maior prevalência de doenças neurodegenerativas. A Doença de Alzheimer (DA) é a doença neurodegenerativa mais comum e a principal causa de demência em indivíduos com mais de 60 anos, sendo caracterizada por um declínio progressivo na memória e função mental dos pacientes. Esses sintomas são acompanhados por alterações histopatológicas no cérebro desses indivíduos, incluindo a presença de uma grande quantidade de placas senis, formadas pela deposição do peptídeo beta-amiloide (Aβ), e de emaranhados neurofibrilares formados pela hiperfosforilação da proteína Tau. Estudos indicam que a deposição do Aβ é uma das principais responsáveis pelo desenvolvimento da DA, causando dano neuronal através da ativação de várias vias pró-apoptóticas e dando origem aos sintomas de demência típicos dessa doença. Até o momento, não existem tratamentos eficazes para o combate à DA, de forma que a maior parte das intervenções farmacológicas é destinada apenas ao tratamento de alguns de seus sintomas. A proteína translocadora (TSPO) se localiza em pontos de contato entre as membranas mitocondriais interna e externa e está relacionada com o transporte de colesterol para o interior da mitocôndria e com a regulação da esteroidogênese e da apoptose. Estudos mostram que ligantes da TSPO apresentam efeitos neuroprotetores em diferentes modelos experimentais de lesão cerebral e doenças neurodegenerativas. Especificamente em relação à DA, um estudo indicou que o 4’-clorodiazepam (4’-CD), um ligante da TSPO, apresenta efeitos neuroprotetores em um modelo animal dessa doença, sendo um possível candidato para o seu tratamento. Dessa forma, o objetivo desse estudo foi verificar o efeito neuroprotetor do 4’-CD em diferentes modelos in vitro de toxicidade induzida pelo Aβ, além de seus efeitos sobre o desenvolvimento de neurônios hipocampais. Inicialmente, demonstramos que o 4’-CD reduziu a morte celular de células SH-SY5Y expostas a um modelo de toxicidade induzida pela administração de Aβ. Esses efeitos estiveram associados com a redução da expressão da proteína pró-apoptótica Bax e com um aumento da expressão da survivina, uma proteína anti-apoptótica. A expressão das proteínas Bcl-xl e procaspase-3, por outro lado, não foi alterada pelos tratamentos. Posteriormente, estudamos os efeitos neuroprotetores do 4’-CD contra a toxicidade induzida pela administração do Aβ em culturas organotípicas de hipocampo. Nesses experimentos, foi demonstrado que o 4’-CD reduz a morte celular de culturas organotípicas de hipocampo expostas ao Aβ através de um aumento na expressão da enzima SOD, sem alterar, no entanto, a expressão das proteínas Akt e procaspase-3. Por fim, foi avaliado o efeito do 4’-CD sobre o desenvolvimento de culturas primárias de neurônios hipocampais de camundongos machos e fêmeas. Foi observado que as culturas de neurônios hipocampais das fêmeas apresentaram um desenvolvimento mais rápido do que as dos machos. O 4’-CD acelerou a maturação e aumentou a ramificação neurítica dos neurônios hipocampais dos machos, mas não exerceu qualquer efeito sobre os neurônios das fêmeas. Em suma, foi observado que o 4’-CD apresenta efeitos neuroprotetores contra o Aβ em células SH-SY5Y e em culturas organotípicas do hipocampo, apresentando-se como um fármaco em potencial para o tratamento da DA. Além disso, foi observado que o 4’-CD exerceu um efeito dependente do sexo sobre o desenvolvimento de culturas primárias de neurônios hipocampais, estimulando o desenvolvimento e a ramificação neurítica de neurônios hipocampais de machos, mas não de fêmeas. / The increase in life expectancy of the world population has been associated with a higher prevalence of neurodegenerative diseases. The Alzheimer’s Disease (AD) is the most common neurodegenerative disorder and the main cause of dementia among people over 60 years, being characterized by a progressive decline in the memory and mental function of the patients. These symptoms are associated with histopathological changes in the brain of these patients, including the presence of senile plaques, formed by the deposition of amyloid-beta (Aβ), and neurofibrillary tangles, which are related to the hyperphosphorylation of Tau protein. Studies indicate that Aβ deposition is a major contributor to AD progression, promoting neuronal damage through the activation of different pro-apoptotic pathways and giving rise to the typical dementia symptoms of this disease. To date, there are no effective treatments for AD, so that most of the pharmacological intervention is intended for the treatment of some of its symptoms. The translocator protein (TSPO) is located in contact sites between the outer and the inner mitochondrial membranes and is involved in the cholesterol transport into the mitochondria and in the regulation of steroidogenesis and apoptosis. Studies show that TSPO ligands present neuroprotective effects in different experimental models of brain injury and neurodegenerative diseases. Specifically regarding AD, a study indicated that 4’-chlorodiazepam (4’-CD), a TSPO ligand, is neuroprotective in an animal model of this disease, being a possible candidate for its treatment. Therefore, the aim of this study was to evaluate the neuroprotective effect of 4’-CD in different experimental models of Aβ- induced neurotoxicity in vitro, as well as its effects on the development of hipocampal neurons. First, it was demonstrated that 4’-CD decreased the cell death of SH-SY5Y cells exposed to the Aβ. This effect was associated with the inhibition of the Aβ-induced upregulation of Bax, a pro-apoptotic protein, and downregulation of survivin, a prosurvival protein. On the other hand, the expression of Bcl-xl and procaspase-3 was not change by the treatments. After, it was studied the neuroprotective effects of 4’-CD against Aβ in organotypic hipocampal cultures. In these experiments, it was shown that 4’-CD decreases the cell death of organotypic hippocampal slices exposed to the Aβ by increasing the protein expression of SOD, but without changing the expression of Akt and procaspase-3. Finally, due to the importance of the processes of neuronal development and maturation in the regeneration of CNS after injury, it was evaluated the effect of 4’-CD on the development of primary hippocampal neurons of male and female mice. It was observed that female primary hippocampal neurons presented an increased rate of development than male neurons. 4’-CD stimulated the development and increased the neuritic branching of male but not from female neurons. In summary, it was observed that 4’-CD presented a neuroprotective effect against Aβ in SH-SY5Y cells and in rat organotypical hippocampal slices, presenting itself as a promising agent for the treatment of AD. Also, it was observed that 4’-CD modulates the development of hippocampal neurons in a sex-dependent manner, stimulating the development of male but not from female cells.

Doenças neurodegenerativas

Doença de Alzheimer

Peptídeos beta-amilóides

Translocases mitocondriais de ADP e ATP

Diazepam

Neurônios

Hipocampo

Neuroproteção

Translocator protein (TSPO)

4’-CD

Neuroprotection

Amyloid-beta

Hippocampus

Neuritogenesis

Énergétique mitochondriale et vieillissement musculaire : de l’in vivo vers le moléculaire / Mitochondrial energetics and skeletal muscle aging : from in vivo to the molecular level

Gouspillou, Gilles

25 October 2010

Le vieillissement musculaire est caractérisé par des pertes progressives de masse et de fonction. Des altérations de l’énergétique mitochondriale pourraient être impliquées dans ce processus. Dans cette thèse, l’analyse modulaire du contrôle métabolique a été appliquée chez le rat à différents niveaux d’intégration pour caractériser les effets du vieillissement sur la fonction mitochondriale. Combinée à la spectroscopie RMN du 31P, cette approche a permis de montrer in vivo dans le muscle gastrocnemius une diminution de la réponse de phosphorylation oxydative mitochondriale face à des variations de concentration des intermédiaires énergétiques chez les rats âgés (21 mois vs. 6 mois). Suivant les principes de l’analyse Top-Down, les propriétés de la phosphorylation oxydative ont été étudiées sur des mitochondries isolées à partir du muscle gastrocnemius. La capacité maximale de production d’ATP est réduite chez les rats âgés, alors que le rendement maximal (rapport ATP/O) de la phosphorylation oxydative reste inchangé. L’application de l’analyse modulaire in vitro a révélé chez les rats âgés une augmentation de la réponse (élasticité) du module phosphorylation face à des variations du potentiel de membrane. Cette élasticité plus élevée explique la modification du schéma de contrôle de la phosphorylation oxydative pour des activités de phosphorylation compatibles avec celles étudiées in vivo. Elle explique également le plus faible potentiel de membrane généré par les mitochondries de rats âgés pour un même niveau d’activité de phosphorylation. De nombreux processus pourraient de fait être affectés : production de radicaux libres, homéostasie calcique, voies de signalisation impliquées dans le contrôle de la masse musculaire. Les modifications des propriétés fonctionnelles de l’ANT démontrées dans cette thèse sont en mesure d’expliquer, au moins en partie, les modifications de l’énergétique mitochondriale révélées à la fois in vitro et in vivo chez les rats âgés. / Skeletal muscle aging is characterized by a progressive loss of muscle mass and function. Involvement in this process of an impaired mitochondrial bioenergetics was proposed but is still extensively debated. The aim of this thesis was to take adventage of the capabilities of modular control analysis approach to get better insights in the effects of aging on mitochondrial function. We first studied the integrated muscle energetics in adult (6 months) and aged (21 months) rats using the modular control analysis approach combined with non-invasive 31P NMR spectroscopy measurements of energetic intermediates. The in vivo activation of mitochondrial oxidative phosphorylation in response to an increase in ATP demand was markedly decreased in the gastrocnemius muscle of aged rats. To further define the effects of aging on mitochondrial energetics, we thus studied the oxidative phosphorylation in mitochondria isolated from the gastrocnemius muscle. Maximal oxidative phosphorylation capacity is clearly reduced in aged rats, while mitochondrial efficiency is unaffected. Application of modular control analysis to the study of oxidative phosphorylation revealed an increased sensitivity (elasticity) of the phosphorylation module in response to changes in membrane potential in aged rats. This increased elasticity is responsible for a modified control pattern of oxidative phosphorylation under low phosphorylation activities. Interestingly these low activities certainly correspond to those we studied in vivo. This increased elasticity of the phosphorylation module is responsible for a modified mitochondrial response toward changes in cellular ATP demand, leading to a decreased membrane potential, which may in turn affect many cellular processes such as ROS production, calcium homeostasis and some signaling pathways involved in the control of muscle mass. The modified ANT properties evidenced in this thesis certainly explain, at least in part, the modified mitochondrial energetics reaveled both in vitro and in vivo in aged rats.

Énergétique mitochondriale

Vieillissement

Muscle Squelettique

Échangeur ATP/ADP

Mitochondrial energetics

Aging

Skeletal Muscle

Modular Control Analysis

Adenine nucleotide translocator

L’accumulation du cholestérol et des oxystérols mitochondriaux lors de la reperfusion du myocarde ischémique : mécanismes et implication dans la cardioprotection / The mitochondrial cholesterol and oxysterol accumulation during the reperfusion of the ischemic myocardium : mechanisms and implication in cardioprotection

Musman, Julien

07 November 2017

L’infarctus du myocarde représente un problème de santé publique dont le traitement de choix consiste à restaurer le flux sanguin (reperfusion) à travers le tissu ischémié dans les plus brefs délais, cependant cette procédure s’accompagne de lésions supplémentaires dont les mécanismes ne sont pas totalement connus. Notre laboratoire a observé que la reperfusion du myocarde s’accompagne d’une accumulation de cholestérol et d’oxystérols dans les mitochondries qui sont impliquées dans l’apparition de ces lésions. L’objectif de ce projet de thèse a donc été d’identifier les mécanismes responsables de cette accumulation. L’utilisation de stratégies cardioprotectrices (statines, exercice physique, ligand de la protéine translocatrice (TSPO)), visant à réduire la concentration cellulaire ou mitochondriale de cholestérol ou le stress oxydant, a tout d’abord permis de mettre en évidence une relation entre l’effet cardioprotecteur et l’inhibition de l’accumulation des stérols mitochondriaux. Cette relation persiste en présence d’une hypercholestérolémie. Par ailleurs, nous avons montré que l’accumulation mitochondriale de cholestérol et d’oxystérols est due à la translocation de la protéine StAR (Steroidogenic Acute Regulatory protein) du cytosol à la mitochondrie dans les premières minutes de la reperfusion et que ce phénomène est modulé par le TSPO. L’inhibition de l’expression mitochondriale de la protéine StAR pourrait représenter une stratégie intéressante afin de protéger le myocarde ischémié de la reperfusion et ce notamment en cas d’hypercholestérolémie. / Myocardial infarction represents a serious public health issue which requires the restoration of the blood flow (reperfusion) in the ischemic tissue as soon as possible; however cardiac reperfusion also induces additional injuries whose mechanisms are not completely established. Our laboratory showed that myocardial infarction induces the accumulation of cholesterol and oxysterols in the mitochondria which are involved in the induction of reperfusion injury. The objective of this thesis project was to identify the mechanisms responsible for this accumulation. The use of cardioprotective strategies (statin, physical exercise, translocator protein (TSPO) ligand), aiming at reducing the cellular and mitochondrial cholesterol concentrations or the oxidative stress, showed the relation between the cardioprotective effect and the inhibition of the mitochondrial sterol accumulation. This relation persists in hypercholesterolemic animals. Furthermore, we showed that the mitochondrial cholesterol and oxysterol accumulation is caused by the translocation of StAR (Steroidogenic Acute Regulatory protein) from cytosol to mitochondria during the first minutes of the reperfusion and this phenomenon is regulated by the TSPO. The inhibition of the mitochondrial expression of StAR could be an interesting approach in order to protect the ischemic myocardium from reperfusion injury, especially in a hypercholesterolemic context.

Cardioprotection

Mitochondrie

Cholestérol

Oxystérols

Steroidogenic Acute Regulatory protein

Protéine translocatrice

Cardioprotection

Mitochondria

Cholesterol

Oxysterols

Steroidogenic Acute Regulatory protein

Translocator protein

611.1

The Molecular Control of Zebrafish Isotocin Cell Development: A Potential Model for the Neurodevelopmental Causes of Autism and Prader-Willi Syndrome

Eaton, Jennifer Lynn

10 July 2006

No description available.

oxytocin

isotocin

vasopressin

vasotocin

Hypothalamo-Neurohypophysial System

hypothalamus

development

autism

Prader-Willi Syndrome

Single-minded

Orthopedia

Arylhydrocarbon Nuclear Translocator

Brn2

POU

zebrafish

behavior

Molecular genetic studies of pollutant response in the European flounder, Platichthys flesus (L.)

Dixon, Thomas James

January 2003

Effects of man made pollutants on an ecosystem are initiated at the cellular level where a prime determinant for survival of an organism is its ability to metabolise and excrete toxic chemicals or their metabolites, thereby preventing cellular toxicity or damage to germ cell DNA. Cytochrome P450 (CYP) enzymes are responsible (in concert with the remainder of the Ah battery enzymes) for the metabolism of numerous xenobiotics and endogenous compounds, including the metabolic activation of most environmental toxic chemicals and carcinogens. Genetic polymorphisms which affect performance of these enzymatic detoxification systems may alter tolerance to pollutants and thus survival in polluted environments. Alterations in the susceptibility of individuals and the development of resistant populations has arisen by forced selection of populations with variant genes, resulting in increased detoxification capacity. There is evidence for such scenarios of variations in activities of pollutant biotransforming enzymes of fish contributing to survival in polluted estuarine environments and several chemically resistant populations have been identified in the USA and Europe. In fish it has been demonstrated that CYP1A enzyme activity is required to activate some carcinogenic xenobiotics to a metabolic state in which they can form DNA adducts. The mechanism of reduced CYP1A expression in highly contaminated populations may therefore represent resistance to chemical stressors. European flounder (Platichthys flesus) from some waterways which have a long history of severe sedimentary contamination do not show elevated levels of CYP1A. The aim of the current study was to investigate whether any heritable differences were apparent between offspring from parents inhabiting long-term polluted and pristine areas. Flounder were obtained from a highly polluted estuary in the UK and crossed with fish from a relatively pristine environment. Offspring were raised in communal tanks in order to standardise environmental conditions, and allow investigations into the genetic variation of CYP1A. To allow identification of offspring to parental fish, polymorphic microsatellite loci were isolated and characterised for the flounder. Novel cDNA probes to transcription factors in the detoxification pathway (AhR2 and ARNT2) were cloned for flounder, and RT-PCR / Southern blot methods were developed for quantitation of gene transcript levels. A novel method of CYP1A quantification using real-time PCR was developed. PAH and PCB exposure trials were carried out on mixed batch offspring, and CYP1A gene transcript levels assessed using Northern blot and real-time PCR techniques. Offspring were genotyped to their parents using the microsatellites obtained, and CYP1A transcript levels were correlated with clean and polluted areas. CYP1A was further correlated to transcription factor expression, and data are presented. Following exposure to the commercial PCB mixture, Aroclor 1254, CYP1A transcript levels were found to be significantly lower in families whose parents originated from a polluted area. This observation indicates that there is a possible genetic component to variation in CYP1A levels, and that these fish may have acquired a heritable tolerance to polluted areas. The lack of induction, or correlation with CYP1A levels, of AhR2 and ARNT2 expression indicates a possible AhR independent pathway for the metabolism of PCBs in the flounder. © Tom Dixon 2003 http://www.tomdixon.org

577.7

Transcriptional regulation of the hepatic cytochrome <em>P450 2a5</em> gene

Arpiainen, S. (Satu)

25 September 2007

Abstract Cytochrome P450 (CYP) enzymes are the major metabolizers of xenobiotics, e.g. drugs, and environmental toxins. Thus, changes in CYP expression have an important impact on drug metabolism and susceptibility to chemical toxicity. In the present study, the transcriptional mechanisms of both constitutive and inducible regulation of the Cyp2a5 gene in mouse liver were investigated. Mouse primary hepatocyte cultures were used as the main model system together with cell and molecular biology methods. The key activation regions of the Cyp2a5 5' promoter were determined using reporter gene assays. Two major transcription activation sites of the Cyp2a5 5' promoter, called the proximal and the distal, were found. Transcription factors hepatocyte nuclear factor-4 (HNF-4) and nuclear factor I were shown to bind to the proximal promoter. Aryl hydrocarbon receptor nuclear translocator (ARNT) and upstream stimulatory factor bound to a common palindromic E-box element in the distal promoter region. All three response elements were shown to be essential for constitutive expression of CYP2A5 in murine hepatocytes. ARNT appeared to control Cyp2a5 transcription without a heterodimerization partner suggesting active involvement of the ARNT homodimer in mammalian gene regulation. Aryl hydrocarbon receptor (AHR) ligands were shown to induce Cyp2a5 transcriptionally by an AHR-dependent mechanism, and established Cyp2a5 as a novel AHR-regulated gene. The AHR response element and the E-box, identified in these studies, were located near to each other and close to a separately defined nuclear factor (erythroid-derived 2)-like 2 binding site in the distal region of the Cyp2a5 promoter, suggesting cooperation between these elements. Peroxisome proliferator-activated receptor gamma coactivator-1α was shown to up-regulate Cyp2a5 transcription through coactivation of HNF-4α. This indicates that xenobiotic metabolism can be regulated by modification of co-activation. The present results show that CYP2A5 is regulated by several different cross-regulatory pathways. The regulatory mechanisms involved in the transcription of the Cyp2a5 gene may also control other CYP genes, especially the human ortholog CYP2A6, and may explain some of the individual variations in the metabolism of xenobiotics.

CYP2A5

aryl hydrocarbon receptor

cytochrome P450 enzyme system

hepatocyte nuclear factor 4

nuclear factor I

upstream stimulatory factors

Study of the aryl hydrocarbon receptor as a target for rational drug design

Xie, Jinghang

01 January 2014

The aryl hydrocarbon receptor (AhR) heterodimerizes with the aryl hydrocarbon receptor nuclear translocator (Arnt) for transcriptional regulation. We generated three N-terminal deletion constructs of the human AhR of 12-24 KDa in size—namely D1 (aa 84-295), D2 (aa 84-192) and D3 (aa 191-295)—to suppress the Arnt function. We observed that all three constructs interact with the human Arnt with similar affinities. D2, which contains part of the AhR PAS-A domain and interacts with the PAS-A domain of Arnt, inhibits the formation of the AhR gel shift complex. D2 suppresses the 3-methylcholanthrene-induced, dioxin response element (DRE)-driven luciferase activity in Hep3B cells and exogenous Arnt reverses this D2 suppression. D2 suppresses the induction of CYP1A1 at both the message and protein levels in Hep3B cells; however, the CYP1B1 induction is not affected. D2 suppresses the recruitment of Arnt to the cyp1a1 promoter but not to the cyp1b1 promoter, partly because the AhR/Arnt heterodimer binds better to the cyp1b1 DRE than to the cyp1a1 DRE. Interestingly, D2 has no effect on the cobalt chloride-induced, hypoxia inducible factor-1 (HIF-1)-dependent expression of vegf, aldolase c, and ldh-a messages. Our data reveal that the flanking sequences of the DRE contribute to the binding affinity of the AhR/Arnt heterodimer to its endogenous enhancers and the function of AhR and HIF-1 can be differentially suppressed by the D2 inhibitory molecule. In chapter 2, a Pichia Pastoris expression system was constructed expressing codon optimized human full length AhR. This codon optimization is necessary for overexpression of huAhR. RT-PCR data showed that the codon optimized mRNA was more stably expressed than wild types. Overexpressed huAhR protein was degraded by proteinase when using a regular P. Pastoris strain yJC100 whereas the proteinase deficient ySMD1163 maintained a much higher level of huAhR. P. Pastoris expressed huAhR was natively purified and analyzed. Coimmunopricipitation assay shows its interaction with endogenous Arnt. A ligand-dependent gel shift was also observed. In addition, we performed an in vitro coprecipitation assay to study its binding to endogenous cyp1b1 DREs. The result shows that the DRE3, known as a critical DRE for cyp1b1 transcriptional activity, has the highest binding affinity to AhR/Arnt complex. Taking together, we constructed a novel P. Pastoris expression system to overexpress human full length AhR. Purified huAhR is a good reagent for studing its ligand and DNA binding. In chapter 3, an adeno-associated virus (AAV) expression system was constructed to express an AhR deletion contruct CΔ553 (aa1-295) for tumor injection. Western blot shows the expression of CΔ553 (aa1-295) in hela cells infected by AAV-553, but the low yield of AAV-553 limited its application on tumor treatment. Possible solutions were discussed for future work.

Pharmacology

Health and environmental sciences

AHR deletion constructs

Aryl hydrocarbon receptor

CYP1A1

Dioxin response element binding

Hypoxia inducible factor-1

Chemicals and Drugs

Chemistry

Medical Pharmacology

Medicinal-Pharmaceutical Chemistry

Medicine and Health Sciences

Pharmaceutical Preparations

Pharmacy and Pharmaceutical Sciences

Physical Sciences and Mathematics