From Variants to Pathways: Interrogating the Genetic Architecture of Age-Related Macular Degeneration

Waksmunski, Andrea Rose

02 June 2020

No description available.

Genetics

Bioinformatics

Biomedical Research

age-related macular degeneration

genetics

Amish

bioinformatics

pathway analysis

database

heritability

epistasis

genome-wide association study

genetic linkage

complement factor H

phospholipase C gamma 2

statistical driver gene

A novel molecular relationship between PARN and PLD that, when deregulated, contributes to the aggressive phenotype of breast cancer cell lines.

Miller, Taylor Elaine

09 May 2017

No description available.

Biochemistry

Cellular Biology

Molecular Biology

PARN

polyA-specific ribonuclease

deadenylase

phospholipase D

PLD

breast cancer

MDA-MB-231

microRNA

miR

miR-203

mRNA decay

post-transcriptional regulation

miR-dependent deadenylation

Avaliação longitudinal de alterações microestruturais cerebrais estado-dependentes em indivíduos com primeiro episódio psicótico, associadas à atividade da enzima fosfolipase A2 / Longitudinal evaluation of state-dependent microstructural brain abnormalities in first-episode psychosis patients, associated to the activity of phospholipase a2 enzyme

Serpa, Mauricio Henriques

10 March 2017

INTRODUÇÃO: Os transtornos mentais psicóticos são condições frequentes na população geral e estão associados a grande morbidade e disfuncionalidade. Apesar disso, as bases fisiopatológicas destes transtornos ainda estão em investigação. Estudos neuropatológicos post-mortem e de neuroimagem in vivo sugerem haver comprometimento da microestrutura de substância branca (SB) cerebral nestas condições clínicas, associado a alterações da conectividade cerebral. No entanto, nenhuma investigação prévia de neuroimagem avaliou especificamente se tais anormalidades microestruturais podem ser dependentes do estado clínico do paciente, i.e., se tais alterações podem variar de acordo com a fase da doença. Outra linha de investigação biológica em psicoses aponta para alterações na atividade da fosfolipase A2 (PLA2), uma enzima essencial a diversas funções na homeostase cerebral, incluindo manutenção de membrana celular, mielinização e atividade inflamatória. Estudos prévios sugerem haver relação entre alterações na atividade desta enzima e as fases da esquizofrenia. Entretanto, não há estudos translacionais que tenham avaliado como tais alterações se relacionam com anormalidades microestruturais de SB em pacientes psicóticos. OBJETIVOS: Investigar a hipótese de que alterações de microestrutura de SB presentes em pacientes em fase aguda do primeiro episódio psicótico (PEP) sejam potencialmente reversíveis após estabilização clínica; investigar também possíveis alterações estado-dependentes da atividade de PLA2 no PEP; e examinar interações entre manifestações clínicas, microestrutura de SB cerebral e atividade de PLA2 na fisiopatologia do PEP. METODOLOGIA: Pacientes em PEP não afetivo foram avaliados em dois períodos no tempo: durante a fase aguda da doença (T0); após remissão estável de sintomas (T1). Um grupo controle de voluntários saudáveis (CS) também foi avaliado longitudinalmente. Para investigar alterações de microestrutura de SB estado-dependentes, análises voxel-a-voxel de mapas cerebrais de índices de anisotropia (fractional anisotropy, FA) e difusividade (trace, TR) foram conduzidas, assim como o cálculo de correlações entre tais índices de DTI, variáveis clínicas e atividade de PLA2. A atividade dos três principais subgrupos de PLA2 em plaquetas foi estimada através de um método radioenzimático. RESULTADOS: 25 pacientes PEP e 51 CS foram avaliados em T0, com coleta de dados clínico-demográficos, ressonância magnética (RM) e amostra de sangue. Destes, 21 PEP e 36 CS realizaram a segunda aquisição de RM. No baseline (T0), os pacientes PEP apresentaram redução difusa de FA (p < 0,05, FDR), afetando principalmente SB fronto-límbica e fascículos associativos, projetivos e comissurais. As análises longitudinais demonstraram que a remissão clínica se associou a aumentos de FA em tratos de SB acometidos em T0 (p < 0,001, não corrigido), além de robustas correlações inversas entre aumentos de FA e redução sintomas ao longo do tempo (p < 0,05, FDR). As análises de PLA2 não demostraram efeitos estado-dependentes ou correlações consistentes com os índices de DTI. CONCLUSÃO: Alterações da microestrutura de SB afetando tratos cerebrais essenciais para a integração de informação perceptual, cognição e emoções são detectáveis logo após o início do PEP e podem ser parcialmente revertidas em relação direta com a remissão de sintomas psicóticos agudos. Nossos achados reforçam a visão de que anormalidades de SB de tratos cerebrais são um componente neurobiológico central nos transtornos psicóticos agudos, e que a recuperação de tal patologia de SB pode levar à melhora clínica. Por outro lado, a atividade de PLA2 não parece ter associação direta com o estado de doença ou moderar as alterações microestruturais dinâmicas de SB aqui observadas. Estudos com amostras maiores e com um maior número de avaliações ao longo do tempo são necessários para confirmar e ampliar os resultados aqui apresentados / INTRODUCTION: Psychotic disorders are frequent conditions in the general population and are associated to severe morbidity and functional impairment. Notwithstanding, the pathophysiological basis of such disorders is still under investigation. Post-mortem neuropathologic investigations and in vivo neuroimaging studies have pointed to the occurrence of abnormalities in the microstructure of brain white matter (WM) in such clinical conditions, which are associated to changes in brain connectivity. However, no previous neuroimaging investigation has specifically examined whether such microstructural abnormalities would be state-dependent, i.e., whether such changes could relate to the illness phase. Another field of biological investigation in psychosis points to changes in the activity of phospholipase A2 enzyme (PLA2), which is essential to several functions implicated in brain homeostasis, such as the maintenance of cellular membrane, myelination and inflammatory activity. Previous studies suggest the existence of a relationship between changes on PLA2 activity and schizophrenia phase. Nonetheless, no translational study to date has examined the potential interplay between PLA2 activity and WM microstructural abnormalities in psychotic patients. OBJECTIVES: To investigate the hypothesis that WM microstructural changes observed in patients during the acute first-episode psychosis (FEP) are potentially reversible following clinical remission; to investigate possible state-dependent changes in PLA2 activity in FEP; and to examine interactions between clinical manifestations, brain WM microstructure and PLA2 activity in the pathophysiology of FEP. METODOLOGY: Patients with non-affective FEP were evaluated in two time points: during the acute phase (T0) and following sustained remission (T1). A control group of healthy volunteers (HC) was also longitudinally studied. In order to investigate state-dependent WM microstructure changes, voxelwise analyses of brain maps of anisotropy (fractional anisotropy, FA) and diffusivity (trace, TR) indexes were conducted, as well as correlations between such DTI metrics, clinical variables and PLA2 activity. The activity of the three main PLA2 subgroups was assessed in platelets using a radioenzymatic method. RESULTS: 25 FEP and 51 HC were evaluated at T0 (clinical and demographic data, MRI scanning, and blood collection). Out of these, 21 FEP and 36 HC also underwent a second MRI acquisition. At baseline (T0), FEP patients presented widespread reduction of FA (p < 0.05, FDR), affecting mainly fronto-limbic WM and associative, projective and commissural fasciculi. Longitudinal analyses showed that clinical remission was associated with FA increase in WM tracts that were affected at T0 (p < 0.001, uncorrected), besides robust inverse correlations between FA increase and symptoms reduction over time (p < 0.05, FDR). PLA2 analyses failed to show state-dependent effects or consistent correlations to DTI indexes. CONCLUSION: WM changes affecting brain tracts critical to the integration of perceptual information, cognition and emotions are detectable soon after the onset of FEP and may partially reverse in direct relation to the remission of acute psychotic symptoms. Our findings reinforce the view that WM abnormalities are a key neurobiological feature of acute psychotic disorders, and that recovery from such WM pathology can lead to amelioration of symptoms. In the other hand, it seems that PLA2 activity has no direct relationship to the disease state or modulatory effects on the dynamic WM changes observed herein. Studies with larger samples and with more time points evaluations are necessary to confirm and expand the findings reported herein

Brain

Diffusion magnetic resonance imaging

Encéfalo

Esquizofrenia

Estudos longitudinais

First-episode psychosis

Fosfolipases A2

Fosfolipídeos

Imagem por ressonância magnética

Longitudinal studies

Magnetic resonance imaging

Phospholipase A2

Phospholipids

Primeiro episódio psicótico

Psychotic disorders

Schizophrenia

Substância branca

Transtornos psicóticos

White matter

Avaliação longitudinal de alterações microestruturais cerebrais estado-dependentes em indivíduos com primeiro episódio psicótico, associadas à atividade da enzima fosfolipase A2 / Longitudinal evaluation of state-dependent microstructural brain abnormalities in first-episode psychosis patients, associated to the activity of phospholipase a2 enzyme

Mauricio Henriques Serpa

10 March 2017

INTRODUÇÃO: Os transtornos mentais psicóticos são condições frequentes na população geral e estão associados a grande morbidade e disfuncionalidade. Apesar disso, as bases fisiopatológicas destes transtornos ainda estão em investigação. Estudos neuropatológicos post-mortem e de neuroimagem in vivo sugerem haver comprometimento da microestrutura de substância branca (SB) cerebral nestas condições clínicas, associado a alterações da conectividade cerebral. No entanto, nenhuma investigação prévia de neuroimagem avaliou especificamente se tais anormalidades microestruturais podem ser dependentes do estado clínico do paciente, i.e., se tais alterações podem variar de acordo com a fase da doença. Outra linha de investigação biológica em psicoses aponta para alterações na atividade da fosfolipase A2 (PLA2), uma enzima essencial a diversas funções na homeostase cerebral, incluindo manutenção de membrana celular, mielinização e atividade inflamatória. Estudos prévios sugerem haver relação entre alterações na atividade desta enzima e as fases da esquizofrenia. Entretanto, não há estudos translacionais que tenham avaliado como tais alterações se relacionam com anormalidades microestruturais de SB em pacientes psicóticos. OBJETIVOS: Investigar a hipótese de que alterações de microestrutura de SB presentes em pacientes em fase aguda do primeiro episódio psicótico (PEP) sejam potencialmente reversíveis após estabilização clínica; investigar também possíveis alterações estado-dependentes da atividade de PLA2 no PEP; e examinar interações entre manifestações clínicas, microestrutura de SB cerebral e atividade de PLA2 na fisiopatologia do PEP. METODOLOGIA: Pacientes em PEP não afetivo foram avaliados em dois períodos no tempo: durante a fase aguda da doença (T0); após remissão estável de sintomas (T1). Um grupo controle de voluntários saudáveis (CS) também foi avaliado longitudinalmente. Para investigar alterações de microestrutura de SB estado-dependentes, análises voxel-a-voxel de mapas cerebrais de índices de anisotropia (fractional anisotropy, FA) e difusividade (trace, TR) foram conduzidas, assim como o cálculo de correlações entre tais índices de DTI, variáveis clínicas e atividade de PLA2. A atividade dos três principais subgrupos de PLA2 em plaquetas foi estimada através de um método radioenzimático. RESULTADOS: 25 pacientes PEP e 51 CS foram avaliados em T0, com coleta de dados clínico-demográficos, ressonância magnética (RM) e amostra de sangue. Destes, 21 PEP e 36 CS realizaram a segunda aquisição de RM. No baseline (T0), os pacientes PEP apresentaram redução difusa de FA (p < 0,05, FDR), afetando principalmente SB fronto-límbica e fascículos associativos, projetivos e comissurais. As análises longitudinais demonstraram que a remissão clínica se associou a aumentos de FA em tratos de SB acometidos em T0 (p < 0,001, não corrigido), além de robustas correlações inversas entre aumentos de FA e redução sintomas ao longo do tempo (p < 0,05, FDR). As análises de PLA2 não demostraram efeitos estado-dependentes ou correlações consistentes com os índices de DTI. CONCLUSÃO: Alterações da microestrutura de SB afetando tratos cerebrais essenciais para a integração de informação perceptual, cognição e emoções são detectáveis logo após o início do PEP e podem ser parcialmente revertidas em relação direta com a remissão de sintomas psicóticos agudos. Nossos achados reforçam a visão de que anormalidades de SB de tratos cerebrais são um componente neurobiológico central nos transtornos psicóticos agudos, e que a recuperação de tal patologia de SB pode levar à melhora clínica. Por outro lado, a atividade de PLA2 não parece ter associação direta com o estado de doença ou moderar as alterações microestruturais dinâmicas de SB aqui observadas. Estudos com amostras maiores e com um maior número de avaliações ao longo do tempo são necessários para confirmar e ampliar os resultados aqui apresentados / INTRODUCTION: Psychotic disorders are frequent conditions in the general population and are associated to severe morbidity and functional impairment. Notwithstanding, the pathophysiological basis of such disorders is still under investigation. Post-mortem neuropathologic investigations and in vivo neuroimaging studies have pointed to the occurrence of abnormalities in the microstructure of brain white matter (WM) in such clinical conditions, which are associated to changes in brain connectivity. However, no previous neuroimaging investigation has specifically examined whether such microstructural abnormalities would be state-dependent, i.e., whether such changes could relate to the illness phase. Another field of biological investigation in psychosis points to changes in the activity of phospholipase A2 enzyme (PLA2), which is essential to several functions implicated in brain homeostasis, such as the maintenance of cellular membrane, myelination and inflammatory activity. Previous studies suggest the existence of a relationship between changes on PLA2 activity and schizophrenia phase. Nonetheless, no translational study to date has examined the potential interplay between PLA2 activity and WM microstructural abnormalities in psychotic patients. OBJECTIVES: To investigate the hypothesis that WM microstructural changes observed in patients during the acute first-episode psychosis (FEP) are potentially reversible following clinical remission; to investigate possible state-dependent changes in PLA2 activity in FEP; and to examine interactions between clinical manifestations, brain WM microstructure and PLA2 activity in the pathophysiology of FEP. METODOLOGY: Patients with non-affective FEP were evaluated in two time points: during the acute phase (T0) and following sustained remission (T1). A control group of healthy volunteers (HC) was also longitudinally studied. In order to investigate state-dependent WM microstructure changes, voxelwise analyses of brain maps of anisotropy (fractional anisotropy, FA) and diffusivity (trace, TR) indexes were conducted, as well as correlations between such DTI metrics, clinical variables and PLA2 activity. The activity of the three main PLA2 subgroups was assessed in platelets using a radioenzymatic method. RESULTS: 25 FEP and 51 HC were evaluated at T0 (clinical and demographic data, MRI scanning, and blood collection). Out of these, 21 FEP and 36 HC also underwent a second MRI acquisition. At baseline (T0), FEP patients presented widespread reduction of FA (p < 0.05, FDR), affecting mainly fronto-limbic WM and associative, projective and commissural fasciculi. Longitudinal analyses showed that clinical remission was associated with FA increase in WM tracts that were affected at T0 (p < 0.001, uncorrected), besides robust inverse correlations between FA increase and symptoms reduction over time (p < 0.05, FDR). PLA2 analyses failed to show state-dependent effects or consistent correlations to DTI indexes. CONCLUSION: WM changes affecting brain tracts critical to the integration of perceptual information, cognition and emotions are detectable soon after the onset of FEP and may partially reverse in direct relation to the remission of acute psychotic symptoms. Our findings reinforce the view that WM abnormalities are a key neurobiological feature of acute psychotic disorders, and that recovery from such WM pathology can lead to amelioration of symptoms. In the other hand, it seems that PLA2 activity has no direct relationship to the disease state or modulatory effects on the dynamic WM changes observed herein. Studies with larger samples and with more time points evaluations are necessary to confirm and expand the findings reported herein

Encéfalo

Esquizofrenia

Estudos longitudinais

Fosfolipases A2

Fosfolipídeos

Imagem por ressonância magnética

Primeiro episódio psicótico

Substância branca

Transtornos psicóticos

Brain

Diffusion magnetic resonance imaging

First-episode psychosis

Longitudinal studies

Magnetic resonance imaging

Phospholipase A2

Phospholipids

Psychotic disorders

Schizophrenia

White matter

Localization and regulation of trpv4 channels in CILIATED epithelia

Lorenzo Moldero, Ivan

24 July 2008

La neteja del moc i dels patògens dels pulmons, i el transport de gàmets i embrions en els òrgans reproductius de les femelles són funcions clau en els epitelis ciliats, tals com aquells que es troben presents en les vies respiratòries i l'oviducte. La taxa de transport mucociliar és funció de la freqüència de batut ciliar (CBF) i aquesta freqüència és augmentada per increments en la concentració de Ca2+ intracelul·lar. El canal catiònic "transient potential vanilloid 4" (TRPV4) intervé en l'entrada de Ca2+ en resposta a estímuls mecànics i osmòtics. L'expressió del TRPV4 en l'epiteli ciliat de les vies respiratòries i de l'oviducte és confirmada mitjançant la localització per immunofluorescència del canal iònic a la membrana apical de l'epiteli ciliat i polaritzat, allà on la senyalització de Ca2+ és requerida per la regulació de la CBF. Cèl·lules ciliades de la tràquea de ratolins TRPV4-/- no expressen el canal TRPV4, no responen a l'activador específic del TRPV4, el 4&#945;-phorbol 12,13-didecanoate (4&#945;-PDD) i presenten respostes de Ca2+ reduïdes a temperatures mitjanes (~25ºC- 8ºC), un altre estímul dels canals TRPV4. L'activació dels canals TRPV4 per solucions altament viscoses i per hypotonicitat depèn de l'activació de la via de la fosfolipasa A2(PLA2)i la subseqüent producció de àcid epoxieicosatrienoic (EET). En condicions de baixa activació de la PLA2, estímuls mecànics i hipotònics alliberen ATP per a l'activació de la via de la fosfolipasa C (PLC)-inositol trifosfat (IP3) per contribuir a l'activació dels canals TRPV4. Descrivim que el metabòlit IP3 sense ser un agonista per ell mateix, sensibilitza el TRPV4 per a l'activació de EET, essent aquest un mecanisme general. L'acoblament funcional entre els canals TRPV4 de la membrana plasmàtica i els receptors de IP3 (IP3R) és necessari tant per iniciar com mantenir la senyalització oscil·latòria del Ca2+ desencadenada per estímuls viscosos i hipotònics. Un dels principals activadors de la CBF, la adenosina-5'-trifosfat (ATP), desencadena una resposta cel·lular mediada per Ca2+ en la que es desencadena tant l'alliberament de Ca2+ des dels dipòsits intracel·lulars com l'entrada de Ca2+. És destacable la contribució de el TRPV4 en l'augment de la CBF mediada per ATP. És més, el nostre treball implica als canals TRPV4 exclusivament en l'entrada de Ca2+ activada per receptor (ROCE). Tot plegat, aquesta tesi doctoral mostra el paper dels canals TRPV4 en l'acoblament d'estímuls fisiològics tipus mecànic, osmòtic i químic a la regulació de la CBF en l'epiteli ciliat destinat al transport mucociliar. / Clearance of mucus and pathogenic agents from lungs and the transport of gametes and embryos in the female reproductive organs are key functions of ciliated epithelia such as those present in the airways and the oviduct. The rate of mucociliary transport is a function of ciliary beat frequency (CBF) and this, in turn, is increased by increases in intracellular calcium. Transient potential vanilloid 4 (TRPV4)cation channel mediates Ca2+ influx in response to mechanical and osmotic stimuli. TRPV4 expression in ciliated epithelia from airways and oviduct is confirmed by immunofluorescence localization of the channel at the apical membrane of the polarized ciliated epithelia, where the Ca2+ signalling is required for CBF regulation. Ciliated tracheal cells from TRPV4-/-mice show no TRPV4 expression, neither increases in intracellular Ca2+ and CBF in response to the TRPV4-specific activator 4&#945;- phorbol 12,13- idecanoate (4&#945;-PDD), and reduced responses to mild temperatures (~25ºC - 38ºC), another TRPV4-activating stimulus. TRPV4 gating by high viscous loads and hypotonicity depends on phospholipase A2 (PLA2) pathway activation and subsequent production of epoxyeicosatrienoic acid (EET). Under conditions of low PLA2 activation, mechanical and hypotonic stimuli use extracellular ATP release-mediated activation of phospholipase C (PLC)-inositol triphosphate(IP3)signalling to support TRPV4 gating. We describe that IP3, without being an agonist itself, sensitizes TRPV4 to EET activation. Besides, the functional coupling between plasma membrane TRPV4 channels and IP3 receptors (IP3R) is required to initiate and maintain the cellular oscillatory Ca2+ signal triggered by high viscous loads and hypotonic stimuli. One of the main CBF activators, adenosine-5'-triphosphate (ATP), triggers both Ca2+ release from intracellular Ca2+ stores and Ca2+ entry. Interestingly, TRPV4 contributes to ATP-induced increase in CBF. Furthermore, our work implicates TRPV4 channel exclusively in receptor-operated Ca2+ entry. Collectively, this PhD thesis shows the role of TRPV4 channels coupling physiologically relevant mechanical, hypotonic and chemical stimuli to CBF regulation in motile ciliary epithelia.

hypotonicity

viscosity

ATP

TRPV4

receptor operated-calcium entry

ion channel

TRP superfamily

inositol-1 4 5-triphosphate

phospholipase A2

ciliary cell culture

patch-clamp

immunofluorescence

calcium imaging

cell volume regulation

ciliary beat frequency

ciliated epithelia

mucus transport

cilia

oviduct

airways

61

616.2

Amyloid beta induces cPLA2 activation by an NADPH oxidase-dependent mechanism in neurons

Shelat, Phullara B., Sun, Grace Y.

January 2008

The entire dissertation/thesis text is included in the research.pdf file; the official abstract appears in the short.pdf file (which also appears in the research.pdf); a non-technical general description, or public abstract, appears in the public.pdf file. Title from PDF of title page (University of Missouri--Columbia, viewed on April 29, 2010). Vita. Thesis advisor: Grace Y. Sun. "May 2008" Includes bibliographical references.

Mise en évidence du rôle de Sar1b et PLD1 dans le transport et le métabolisme des lipides dans l’intestin : impact sur la formation et la sécrétion des chylomicrons

Auclair, Nickolas

12 1900

Les chylomicrons (CM) sont des vésicules produites et sécrétées par les entérocytes de l'intestin grêle pour permettre le transport des lipides et des vitamines liposolubles de l'alimentation vers la circulation sanguine. Les mécanismes de transport, de formation et de sécrétion des CM sont très complexes et des défauts dans ces mécanismes peuvent affecter de manière significative la qualité de vie d'un individu. Il est clair qu'il existe des lacunes dans notre compréhension des protéines qui régulent ces processus puisque certains patients atteints de malabsorptions intestinales ne présentent pas de mutations pour des protéines connues et d’autres patients présentant des mutations connues ont des caractéristiques cliniques incompréhensibles. La phospholipase D(PLD) 1 et la Sar1b GTPase sont deux protéines dont le rôle dans l'homéostasie lipidique intestinale reste à mieux préciser. La PLD1 est une enzyme dont le rôle principal est de catalyser la formation d'acide phosphatidique à partir de la phosphatidylcholine. Son produit permet de réguler de nombreux processus cellulaires tels que l’endocytose, l’exocytose et le traffic vésiculaire. Cependant, sa fonction dans l'homéostasie lipidique intestinale était jusqu'à présent inconnue. La Sar1b GTPase, quant à elle, régule la formation des vésicules COPII du réticulum endoplasmique (RE) et sa mutation a été associée à la maladie de rétention du CM (MRC), l'une des trois principales maladies qui provoquent une malabsorption des lipides intestinaux. Cependant, nos connaissances scientifiques sur cette enzyme sont assez limitées et même sa relation de cause à effet reste à définir dans un organisme complexe tel qu'un mammifère. Par conséquent, l'objectif général de cette thèse est de mettre en évidence le rôle de la PLD1 et de la Sar1b GTPase dans le transport et le métabolisme des lipides intestinaux. Pour atteindre ces objectifs, nous avons soit administré des inhibiteurs de l'activité des différents isoformes de PLD à des cellules entérocytaires Caco2/15, ou utilisé des cellules présentant une diminution de l’expression du gène de PLD1. En outre, pour la Sar1b GTPase, nous avons utilisé des souris présentant soit une mutation ponctuelle, soit une délétion de Sar1b. Nos résultats ont montré que la diminution de l'expression protéique de PLD1 réduit la sécrétion de CM et modifie l'expression protéique de facteurs importants impliqués dans la β-oxydation et la lipogenèse. En ce qui concerne la Sar1b GTPase, nous avons pu observer que les souris homozygotes avec une mutation ou une délétion de Sar1b ne sont pas viables et sembleraient mourir juste après la naissance étant donné le développement embryonnaire normal de ces souris. Avec les souris hétérozygotes, nous avons quand même pu confirmer la relation de cause à effet entre le gène et la MRC puisque ces souris récapitulaient plusieurs anomalies gastro-intestinales retrouvées chez les patients. En outre, nous avons observé que la gravité des caractéristiques observées chez les souris peut dépendre du régime alimentaire et du génotype. De plus, nous avons observé que les mâles présentant une mutation ponctuelle reflétaient d’avantage la maladie. Par ailleurs, les lipoprotéines de ces animaux avaient une composition chimique et protéique altérée avec une diminution de la quantité d’ApoB-100 dans les fractions de VLDL et LDL, ainsi qu’une augmentation des ratios cholestérol ester/phospholipides et des ratios lipides estérifiés/lipides non-estérifiés. Enfin, nous avons observé que l'altération du gène Sar1b dans l'intestin affecte son homéostasie lipidique et modifie l'expression génique et protéique de plusieurs facteurs importants dans le stress du RE, la β-oxydation, la lipogenèse et le métabolisme du cholestérol. En conclusion, même si cette thèse comporte plusieurs limites, nous avons pu établir le rôle de la PLD1 et de la Sar1b GTPase dans l'homéostasie lipidique. En effet, nous sommes les premiers à avoir démontré que l'altération du gène PLD1 affecte la sécrétion de CM et le métabolisme des lipides dans les cellules intestinales. De plus, nous avons pu confirmer in vivo la relation de cause à effet entre la MRC et la protéine Sar1b, tout en ayant une meilleure compréhension de son impact sur le métabolisme des lipides qui peut varier en fonction de différents facteurs tels que le génotype et la diète. Une meilleure compréhension de ces protéines permettrait d'augmenter les cibles possibles pour le développement de traitements ciblant la sécrétion de CM et de mieux comprendre les conséquences que la mutation de ces gènes peut avoir chez les patients. / Chylomicrons (CMs) are vesicles produced and secreted by enterocytes in the small intestine to transport lipids and fat-soluble vitamins from the diet into the bloodstream. The mechanisms of CM transport, formation and secretion are very complex and defects in these mechanisms can significantly affect the quality of life of an individual. It is clear that there are gaps in our understanding of the proteins that regulate these processes since some patients with intestinal malabsorptions do not have mutations for known proteins and other patients with known mutations have incomprehensible clinical features. Phospholipase D (PLD) 1 and Sar1b GTPase are two proteins whose role in intestinal lipid homeostasis remains to be better defined. PLD1 is an enzyme whose main role is to catalyze the formation of phosphatidic acid from phosphatidylcholine. Its product regulates many cellular processes such as endocytosis, exocytosis and vesicular trafficking. However, its function in intestinal lipid homeostasis was unknown until now. Sar1b GTPase, on the other hand, regulates COPII vesicle formation in the endoplasmic reticulum (ER) and its mutation has previously been associated with CM retention disease (CRD), one of the three major diseases that cause intestinal lipid malabsorption. However, our scientific knowledge about this enzyme is quite limited and even its cause and effect relationship remains to be defined in a complex organism such as a mammal. Therefore, the overall goal of this thesis is to highlight the role of PLD1 and the Sar1b GTPase in intestinal lipid transport and metabolism. To achieve these objectives, we either administered inhibitors of the activity of different PLD isoforms to Caco2/15 enterocyte cells or used cells with protein depletion of PLD1. In addition, for the Sar1b GTPase, we used mice with either a point mutation or a deletion of Sar1b. Our results showed that decreased protein expression of PLD1 reduces CM secretion and alters the protein expression of important factors involved in β-oxidation and lipogenesis. With regard to the Sar1b GTPase, we could observe that homozygous mice with a mutation or deletion of Sar1b are not viable and would appear to die just after birth given the normal embryonic development of these mice. With the heterozygous mice, we were still able to confirm the causal relationship between the gene and CRD since these mice recapitulated several gastrointestinal abnormalities found in patients. In addition, we observed that the severity of the features observed in the mice may depend on diet and genotype. In addition, we observed that males with a point mutation reflected the most the disease. Also, the lipoproteins of these animals had an altered chemical and protein composition, with a decrease in the amount of ApoB-100 in the VLDL and LDL fractions, as well as an increase in choesteryl ester/phospholipids ratios and esterified/nonesterified lipid ratios. Finally, we observed that alteration of the Sar1b gene in the gut affects its lipid homeostasis and alters the gene and protein expression of several factors important in ER stress, β-oxidation, lipogenesis, and cholesterol metabolism. In conclusion, although this thesis has several limitations, we were able to establish the role of PLD1 and the Sar1b GTPase in lipid homeostasis. Indeed, we are the first to have demonstrated that alteration of the PLD1 gene affects CM secretion and lipid metabolism in intestinal cells. Furthermore, we were able to confirm in vivo the causal relationship between MRC and the Sar1b protein, while having a better understanding of its impact on lipid metabolism which can vary according to different factors such as genotype and diet. A better understanding of these proteins would increase the possible targets for the development of treatments targeting CM secretion and better understand the consequences that mutation of these genes may have in patients.

Souris transgéniques

Caco-2/15

Intestin

Lipoprotéines

Syndrome métabolique

Maladie de rétention des chylomicrons

Phospholipase D

Sar1b GTPase

malabsorption intestinale

Dyslipidémies

Métabolisme lipidique

Métabolisme du cholestérol

Transgenic mice

Intestine

Liver

Lipoproteins

Metabolic syndrome

Chylomicron retention disease

intestinal malabsorption

The signalling role of superoxide anion in vascular smooth muscle cells

Wu, Lingyun

05 1900

Thèse numérisée par la Direction des bibliothèques de l'Université de Montréal. / L'anion superoxyde peut agir comme une molécule de signalisation ou comme un facteur préjudiciable selon sa concentration, l'organe cible, et selon la présence ou non d'antioxydants neutralisants. Actuellement, dans les cellules musculaires lisses (CMLs) vasculaires, les effets de l'anion superoxyde sur les différentes voies de transduction du signal et sur les interactions croisées entre ces voies ne sont pas encore définies. Par conséquent, une meilleure connaissance des effets de l'anion superoxyde sur les différentes voies de signalisation pourrait fournir une meilleure compréhension des mécanismes sous-jacents aux fonctions altérées des CMLs vasculaires observées dans des conditions pathologiques. L'objectif général de cette étude était de caractériser et d'évaluer le rôle modulateur de l'anion superoxyde, produit par la réaction de l'hypoxanthine avec la xanthine oxidase, sur les activités de différentes voies de signalisation dans les CMLs vasculaires, et de déterminer si la sensibilité de différentes voies de signalisation à l'anion superoxyde était altérée dans l'hypertension artérielle. Le projet de ce programme de recherche était basé sur les principaux postulats suivants : (1) l'anion superoxyde pourrait affecter sélectivement la production d'inositol 1,4,5-triphosphates (IP3), de GMPc, ou d'AMPc dans les CMLs vasculaires; (2) le rôle modulateur de l'anion superoxyde pourrait être dû à une altération des interactions croisées entre différentes voies de signalisation; et (3) les anomalies observées dans les CMLs vasculaires chez le rat spontanément hypertendu (SHR) pourraient être reliées à des altérations des différentes voies de signalisation induites par l'anion superoxyde. Une production augmentée d'1P3induite par l'anion superoxyde dans les CMLs d'aorte de rat ou d'artère mésentérique en culture a été démontrée pour la première fois dans cette étude. L'anion superoxyde a augmenté la formation d'IP3d'une manière concentration-dépendante et temps-dépendante. La superoxyde dismutase (SOD), mais non la catalase, a inhibé significativement la formation d'IP3 induite par l'anion superoxyde. L'inhibition de la phospholipase C (PLC) a aboli l'effet de l'anion superoxyde sur la formation d'1P3. La génistéine et la tyrphostine A25, deux inhibiteurs de la tyrosine kinase, ont aussi inhibé significativement la formation d'IP3induite par l'anion superoxyde. L'utilisation d'anticorps anti-PLCy a atténué significativement la formation d'1P3induite par l'anion superoxyde. De plus, le taux d'expression des protéines de la PLCy a été augmenté après l'exposition des CMLs à l'anion superoxyde. Ces observations suggèrent donc que dans les CMLs vasculaires la formation d'1P3 induite par l'anion superoxyde pourrait être en grande partie secondaire à une augmentation de l'activité de la tyrosine kinase liée aux voies de signalisation de la PLCy. En ce qui concerne la voie du GMPc, l'anion superoxyde a diminué significativement les niveaux de base de GMPc et supprimé aussi l'augmentation des niveaux de GMPc induite par des stimulateurs de la guanylyl cyclase, le nitroprussiate de sodium (NPS) ou la s-nitroso-nacétylpénicillamine (SNAP). La formation d'1P3stimulée par l'anion superoxyde a été significativement inhibée par le NPS ou la SNAP, mais potentialisée de façon importante par un inhibiteur de la guanylyl cyclase l'ODQ ou par le KT5823 (un inhibiteur de la protéine kinase dépendant du GMPc). Cependant, l'anion superoxyde n'a pas eu d'effet sur les niveaux de base d'AMPc ou sur la production d'AMPc induite par la forskoline et de plus, l'inhibition de l'adénylyl cyclase ou de la protéine kinase dépendante de l'AMPe n'a pas affecté la formation d'lP3stimulée par l'anion superoxyde. Ces données, par conséquent, suggèrent que l'inhibition de la formation de GMPc par l'anion superoxyde contribue probablement à l'activation de la formation d'1P3induite par l'anion superoxyde en atténuant le rétrocontrôle inhibiteur du GMPc sur les voies de signalisation liées à la PLC, tandis que la voie de signalisation de l'AMPc ne serait pas impliquée dans la formation d'EP3induite par l'anion superoxyde. Dans les CMLs vasculaires de rat SHR, les effets de l'anion superoxyde ont été plus puissants que dans les CMLs de rat WKY, en ce qui concerne l'augmentation de formation d'1P3, la diminution des taux de GMPc et la facilitation induite par l'anion superoxyde des interactions croisées entre les voies du GMPc et de 1'IP3. Dans les CMLs vasculaires des deux souches de rat, la formation d'IP3induite par l'anion superoxyde a été inhibée par une variété d'antioxydants, dont la N-acétylcystéine, l'acide a-lipoïque, la mélatonine et la SOD. Il apparaît donc vraisemblable que l'hypersensibilité à l'anion superoxyde des voies de 1'IP3et du GMPc puissent contribuer à l'augmentation du tonus vasculaire et de la réactivité des CMLs dans l'hypertension artérielle. Nous avons aussi investigué si l'effet de la mélatonine était dû à ses propriétés antioxydantes. Un effet inhibiteur plus important de la mélatonine sur la contraction aortique induite par la norépinéphrine (NE) a été observé chez les rats SHR en comparaison avec les rats Wistar-Kyoto (WKY). L'inhibition par la mélatonine de la formation d'IP induite par la NE a été aussi plus importante dans les CMLs aortiques de rat SHR que dans celles de rat WKY. Les effets plus puissants de la mélatonine chez le rat SHR, qui ont été aussi observés avec la SOD, mais non avec la catalase, ne sont pas dûs à l'activation des récepteurs à la mélatonine ou des récepteurs a-adrénergiques. Ces résultats indiquent que les effets anti-hypertenseurs de la mélatonine sont largement dûs à l'inactivation de l'anion superoxyde, et que les niveaux endogènes d' antioxydants ne parviennent pas à contrecarrer les niveaux accrus d'anion superoxyde produits chez le rat SHR. En conclusion, cette étude révèle une variété de nouveaux mécanismes de signalisation de l'anion superoxyde. Pour la première fois, il a été démontré que l'anion superoxyde active l'hydrolyse des phosphoinositides et augmente les taux d'IP3dans les CMLs vasculaires, principalement par la stimulation de la tyrosine kinase liée à la voie de signalisation de la PLCy. Il a aussi été observé que l'anion superoxyde réduit la formation de GMPc et supprime l'inhibition croisée de 1'1P3par le GMPc, facilitant ainsi la formation d'1P3. Les effets sélectifs de l'anion superoxyde sur les voies de 1'IP3et du GMPc, ainsi que l'existence d'une inhibition croisée de la formation d'1P3par la voie du GMPc, révèlent des mécanismes nouveaux pour expliquer le rôle modulateur de l'anion superoxyde sur les voies de signalisation dans les CMLs. Par conséquent, les effets plus puissants de l'anion superoxyde sur la signalisation de la voie de 1'IP3et de la voie du GMPc dans les CMLs vasculaires de rat SHR, effets qui ont été démontrés pour la première fois dans cette étude, pourraient être responsables des altérations des mécanismes de transduction du signal cellulaire chez le rat SHR et ainsi contribuer au développement et/ou au maintien de l'hypertension artérielle. Ces observations permettent donc d'imaginer de nouvelles orientations pour le développement de nouvelles stratégies pour la prévention ou le traitement de l'hypertension artérielle. / Superoxide anion can act as a signalling molecule or a detrimental factor depending on its concentration, the targeted organ, and the presence of counteracting antioxidants. The effects of superoxide on different signal transduction pathways and on the cross-talk interactions among these pathways in vascular smooth muscle cells (SMCs) are presently still unsettled. Therefore, a better knowledge on the effects of superoxide on different signalling pathways may provide a better understanding of the mechanisms underlying the altered functions in vascular SMCs observed in pathological conditions. The general objective of this study was to characterize and evaluate the modulating role of superoxide generated by the hypoxanthine and xanthine oxidase reaction on the activities of different signalling pathways in vascular SMCs and to investigate whether the sensitivities of different signalling pathways to superoxide were altered in hypertension. The design of the present research program was based on the following major postulates. (1) superoxide might selectively affect the generation of inositol 1,4,5-triphosphates (IP3), cGMP, or cAMP in vascular SMCs; (2) the modulating role of superoxide might be mediated by alteration in the cross-talk interactions among different signalling pathways; and (3) the abnormalities observed in vascular SMCs from spontaneously hypertensive rats (SHR) might be related to the alterations induced by superoxide on different signalling pathways. An enhanced production of 1P3induced by superoxide in cultured SMCs from rat aorta or mesenteric artery was demonstrated, for the first time, in this study. Superoxide increased 1P3 formation in a concentration- and time-dependent manner. Superoxide dismutase (SOD), but not catalase, significantly inhibited the superoxide-increased 1P3formation. The inhibition of phospholipase C (PLC) abolished the effect of superoxide on IP3formation. Genistein and tyrphostin A25, two tyrosine kinase inhibitors, also significantly inhibited the superoxideinduced IP3formation. The application of antibody against PLCI, significantly attenuated the superoxide-induced 1P3formation. Moreover, the expression level of PLC7proteins was increased after exposing SMCs to superoxide. These observations thus suggest that superoxideinduced IP3 formation may be in a great part secondary to an increase in the activity of tyrosine kinase-link PLCy signalling pathways in vascular SMCs. Concerning the cGMP pathway, superoxide significantly decreased the basal levels of cGMP and also suppressed the rise in cGMP levels induced by guanylyl cyclase stimulator sodium nitroprusside (SNP) or s-nitroso-n-acetylpenicillamine (SNAP). The superoxide-induced IP3 formation was significantly inhibited by SNP or SNAP, but markedly potentiated by a guanylyl cyclase inhibitor ODQ or KT5823 (a cGMP-dependent protein kinase inhibitor). However, superoxide had no effect on the basal levels of cAMP or the forskolin-induced cAMP production and moreover, the inhibition of adenylyl cyclase or cAMP-dependent protein kinase did not affect the superoxide-enhanced IP3formation. These data, therefore, suggest that the reduced cGMP formation by superoxide probably contributes to the superoxide induced activation of 1P3 formation by lifting the inhibitory feedback of cGMP on the PLC pathway(s), whereas, the cAMP pathway may not be involved in the superoxide-induced IP3formation. In vascular SMCs from SHR, the effects of superoxide were more potent than in SMCs from WKY, including the increase in 1P3 formation, the decrease in cGMP levels, and the superoxide-induced facilitation of the cross-talk interaction between cGMP and IP3pathways. The superoxide-induced 1P3formation was inhibited by a variety of antioxidants, including nacetylcysteine, cc-lipoic acid, melatonin and SOD, in vascular SMCs from both strains. It thus appears that the hypersensitivity of 1P3and cGMP pathways to superoxide is likely to contribute to the increased vascular tone and reactivity of SMCs in hypertension. Whether the effect of melatonin is due to its antioxidant properties was also explored. A greater inhibitory effect of melatonin on the norepinephrine (NE)-induced aortic contraction was observed in SHR than in Wistar-Kyoto rats (WKY). The inhibition of the NE-induced IP formation by melatonin was also greater in aortic SMCs from SHR than that from WKY. The enhanced effects of melatonin in SHR, which were found to be similarly enhanced with SOD but not with catalase, were not mediated by melatonin receptors or oc-adrenoceptors. These results indicate that the anti-hypertensive effects of melatonin are largely due to the scavenging of superoxide, and that the levels of endogenous antioxidants may not counteract the levels of overproduced superoxide in SHR. In conclusion, this study reveals a variety of novel signalling mechanisms for superoxide. For the first time, it was demonstrated that superoxide activates the hydrolysis of phosphoinositides and increases IP3levels in vascular SMCs mainly through the stimulation of tyrosine kinase-link PLCy signal pathway. It was also found that superoxide reduces cGMP formation and suppresses the cross-inhibition of IP3by cGMP, thus facilitating 1133formation. The selective effects of superoxide on 1133and cGMP pathways as well as the existence of a cross-inhibition of IP3formation by cGMP pathway provide novel mechanisms for the signalling role of superoxide in vascular SMCs. Therefore, the altered signalling effects of superoxide on the IP3pathway and the cGMP pathway, which were demonstrated in vascular SMCs from SHR for the first time in this study, could thus be responsible for the alterations in cellular signal transduction mechanisms in SHR and might contribute to the development and/or maintenance of hypertension. These observations could provide new avenues for the development of new strategies for the prevention or treatment of hypertension.

Anion superoxyde

Signalisation cellulaire

Hypertension artérielle

Voies de signalisation

Inositol 1,4,5-triphosphates (IP3)

GMPc (guanosine monophosphate cyclique)

AMPc (adénosine monophosphate cyclique)

Phospholipase C (PLC)

Réactivité vasculaire

Superoxide anion

Signalling pathways

Vascular smooth muscle cells (SMCs)

Hypertension

Inositol 1,4,5-triphosphates (IP3)

cGMP

cAMP

Tyrosine kinase

Antioxidants

Biology / Biologie (UMI : 0306)