Étude et applications du réarrangement sigmatropique [3,3] d'allyl cyanates pour la synthèse de molécules d'intêret biologique / Study and applications of [3,3] sigmatropic rearrangement of allyl cyanates for the synthesis of molecules of biological interest.

Henrion, Sylvain

19 December 2017

De nos jours, parmi toutes les transformations chimiques dont disposent les chimistes organiciens, le réarrangement sigmatropique [3,3] constitue un outil puissant afin de créer une liaison C-C ou encore C-hétéroatome. Le réarrangement d’allyl cyanate en allyl isocyanate, jusqu’ici peu utilisé, est en train d’émerger, comme une nouvelle méthode efficace de préparation d’allylamines substituées. C’est dans ce contexte que s’inscrit mon travail de thèse qui a pour objectif d’étudier et d’utiliser le réarrangement sigmatropique [3,3] d’allyl cyanates diversement substitués pour la synthèse de molécules d’intérêt biologique. Dans une première partie, l’emploi d’allyl cyanates borylés nous a permis de synthétiser, de façon stéréocontrôlée, des ènecarbamates et des ènehydroxyurées cycliques à 7 chainons ainsi que des γ-butyrolactones. Cette méthodologie a été appliquée à la première synthèse totale de la (-)-Galbacin. Les ènecarbamates cycliques ont fait l’objet, en seconde partie, d’une étude structure-activité en tant qu’inhibiteur du protéasome humain. Dans une troisième partie, nous avons étudié le réarrangement d’allyl cyanates silylés ce qui nous a permis d’accéder à des α-amino allylsilanes énantioenrichis. En dernière partie, nous avons mis en évidence un oxo-réarrangement à partir d’allyl carbamates substitués par un groupement aryle. / Nowadays, among all chemical transformations in the organic chemist’s toolbox, [3,3] sigmatropic rearrangements represent a powerful method to create carbon-carbon or even carbon-heteroatom bonds. The allyl cyanate to allyl isocyanate rearrangement, underused so far, is becoming an attractive method to prepare substituted allylamines. In this context, I studied and applied in my thesis this [3,3] rearrangement on diversely substituted allyl cyanates for the synthesis of molecules of biological interest. First, we used borylated allyl cyanates to prepare, stereoselectively, cyclic seven membered enecarbamates and enehydroxyureas as well as γ-butyrolactones. This methodology was applied to the first total synthesis of (-)-Galbacin. Then, a library of cyclic enecarbamates was performed to study the structure-activity relationship on the human proteasome. Next, the study of silylated allyl cyanates allowed us to prepare some new enantioenriched α-amino allylsilanes. Finally, we brought to light an unexpected oxo-rearrangement from aryl substituted allyl carbamates.

Réarrangement sigmatropique

Isocyanate

Allylboronate

Enecarbamate

Γ-Butyrolactone

Galbacin

Protéasome

Allylsilane

Amino allylsilane

Oxo-Réarrangement

Sigmatropic rearrangement

Isocyanate

Allylboronate

Enecarbamate

Γ-Butyrolactone

Galbacin

Proteasome

Allylsilane

Amino allylsilane

Oxo-Rearrangement

Biomass derivatives in heterogeneous catalysis : adsorption, reactivity and support from first principles / Dérivés de la biomasse en catalyse hétérogène : adsorption, réactivité et support depuis les premiers principes

Reocreux, Romain

13 July 2017

L’abandon progressif des ressources fossiles s’accompagne de l’exploitation croissante de la biomasse. Cette transition nécessite de développer de nouveaux procédés notamment en catalyse hétérogène. Les chimistes se heurtent alors à deux défis majeurs : (i) désoxygéner la biomasse (cellulose/lignine) pour revenir à la chimie maîtrisée des grands intermédiaires (ii) rendre les catalyseurs résistants à l’eau, omniprésente en biomasse. En collaboration avec des expérimentateurs de l’Université d’Ottawa, nous nous sommes d’abord intéressés à la désoxygénation d’aromatiques de type lignine. Les calculs ab initio (DFT) nous ont permis de dresser les caractéristiques d’adsorption de ces composés sur Pt(111) en termes de descripteurs moléculaires simples. Nous avons ensuite étudié le mécanisme de décomposition de l’anisole et du 2-phénoxyéthanol, molécules modèles. Nos études ont montré l’importance de l’hydrogène et des fragments carbonés sur la réaction de désoxygéna6on de ces composés. En parallèle nous nous sommes intéressés à la stabilité, dans l’eau, d’un des supports catalytiques majeurs : l’alumine-γ. Ce sujet clé pose des défis considérables en modélisation, puisqu’il nécessite d’utiliser des méthodes de dynamiques moléculaires ab initio. Celles-ci nous ont permis de caractériser la structuration de l’eau au contact de l’alumine et l’importance de la solvatation sur les aluminols de surface. À l’aide de méthodes d’événements rares (dynamique contrainte, métadynamique) nous avons enfin abordé la réactivité d’alcools et de l’eau avec l’alumine hydratée. Ces simulations ont permis d’identifier les premières étapes d’hydratation et de mieux comprendre comment les limiter. / Moving away from fossil ressources is currently being accompanied by the increasing exploitation of biomass.This shift requires the development of new processes, in particular in heterogeneous catalysis. Chemists are nowfacing two major challenges: (i) deoxygenate biomass (cellulose/lignin) to produce platform intermediates with aeel-known chemistry (ii) make catalysts resistant to water, ubiquitous within the context of biomass.Within a collaboration with experimentalists at the University of Ottawa, we have first studied the deoxygenationof lignin-like aromatics. From an ab initio (DFT) inspection, we have characterized and described the adsorptionof such aromatic oxygenates on Pt(111) with simple molecular descriptors. We have then investigated thedecomposition mechanism of anisole and 2-phenoxyethanol. For these two model compounds, we have showedthe significance of hydrogen and carbonaceous species to have the deoxygenation reaction proceed properly.Meanwhile, we have examined the stability, in water, of γ-alumina, a major support in heterogeneous catalysis.The necessity to perform ab initio molecular dynamics simulations makes the modeling of such a systemparticularly challenging computationally. The simulations have nevertheless enabled us to characterize thestructuration of liquid water in contact with alumina and the significance of solvation on surface aluminol groups.Using rare-event methods (constrained dynamics, metadynamics) we have eventually been able to probe thereactivity of alcohols and water with hydrated alumina. We have then identified the first steps of hydration andgained insights on how to limit them.

Mécanismes réactionnels

DFT

Lignine

Métadynamique

Alumine γ

Dynamique moléculaire

Pt(111)

Interfaces

Reaction mechanisms

DFT

Lignin

Metadynamics

Alumina γ

Molecular dynamics

Pt(111)

Interfaces

Ação farmacológica do 3-alquinil selenofeno em modelos de convulsão em ratos jovens / Pharmacological action of 3-alkynyl selenophene on models of seizures in rat pups

Wilhelm, Ethel Antunes

02 March 2012

Conselho Nacional de Desenvolvimento Científico e Tecnológico / Seizures have important consequences in terms of mortality and quality of life of the affected population, being a risk factor for the development of cognitive and behavioral abnormalities. Considering the promising pharmacological properties of molecules containing selenium, in article 1, we evaluated the anticonvulsant action of 1-(2,5-diphenylselenophen-3-yl)-3-methylpent-1-yn-3-ol, generically called 3-alkynyl selenophene (3-ASP) against seizures induced by pilocarpine (PC), pentylenetetrazole (PTZ) and kainate (KA) in 21-days-old rats. Animals were pre-treated with 3-ASP (10, 25 or 50 mg/kg; per oral, p.o.) or vehicle, 30 minutes before of intraperitoneally administration of PC (400 mg/kg), PTZ (80 mg/kg) or KA (45 mg/kg). 3-ASP pre-treatment (50 mg/kg) abolished seizures and the death induced by PC administration. 3-ASP (50 mg/kg) increased the latency to the first convulsive episode, as well as decreased the mortality and incidence of seizures caused by PTZ and KA. In article 1, the antioxidant activity of 3-ASP (10, 25 or 50 mg/kg; p.o.) against the oxidative stress induced by PC (400 mg/kg, i.p.) in 21-days-old rats was evaluated. Our results demonstrated that 3-ASP pre-treatment was effective in protecting against the inhibition of cerebral activity of superoxide dismutase, decreased ascorbic acid levels, stimulation of catalase activity and increase of reactive species levels caused by PC. Additionally, 3-ASP protected against the inhibition of acetylcholinesterase and Na+, K+-ATPase activities resulting from convulsions induced by PC. The involvement of glutamatergic and GABAergic systems in the anticonvulsant action of 3-ASP was investigated (Articles 1 and 2). The combination of sub-effective doses of 3-ASP (10 mg/kg, p.o.) and diazepam (GABA agonist; 0,5 mg/kg, i.p.), 5S,10R-(+)-5-methyl-10,11-dihydro- 5H-dibenzo[a,d]cyclohepten-5,10-imine maleate (MK-801, a non-competitive N-methyl-D-aspartate (NMDA) receptor antagonist; 0.1mg/kg, i.p.) or 6,7-dinitroquinoxaline-2,3-dione (DNQX, a non-NMDA receptor antagonist; 5 mg/kg, i.p.) was effective in increasing the latency to the first convulsive episode, as well as, in decreasing the incidence of convulsions induced by PC. On the other hand, the combination of 3-ASP and 2-methyl-6-phenylethynyl pyridine hydrochloride (MPEP, an antagonist of metabotropic glutamate receptor mGluR5; 0,5 mg/kg, i.p.) did not protect against convulsions. The oral administration of 3-ASP (50 mg/kg) caused an inhibition of 64% and 58% of GABA uptake in the cortex and hippocampus, respectively. However, no change in glutamate uptake after 3-ASP administration (50 mg/kg) was found. Additionally, in article 2, we investigated the possible interaction between sub-effective doses of 3-ASP and GABA uptake or GABA transaminase (GABA-T) inhibitors against PC-induced seizures in 21-days-old rats. To this, sub-effective doses of 3-ASP (10 mg/kg; p.o.) and DL-2,4-diamino-n-butyric acid hydrochloride (DABA, an inhibitor of GABA uptake; 2 mg/kg; i.p.) or aminooxyacetic acid hemihydrochloride (AOAA; a GABA-T inhibitor; 10 mg/kg, i.p.) were co-administrated in 21-days-old rats before of PC administration (400 mg/kg). The treatment with 3-ASP and DABA abolished the PC-induced seizures. Similar results were found when sub-effective doses of 3-ASP and AOAA were administrated in 21-days-old rats. Finally, in the article 3 we investigated the effect of 3-ASP or diazepam against convulsions, the increased susceptibility to the development of seizures and long term memory impairment resulting from febrile seizures induced by hyperthermia. 21-Days-old rats were pre-treated with 3-ASP (25, 50 or 100 mg/kg; p.o), diazepam (1 or 5 mg/kg; i.p.) or vehicle. After the treatment, animals were exposed to a stream of heated air to approximately 41°C. Thirty days after the exposure to hyperthermia, the susceptibility to the development of seizures and long term memory impairment were evaluated. We verified that the pre-treatment with 3-ASP or diazepam did not protect against stereotyped behavior, facial automatisms and body flexion induced by hyperthermia. The protective effect of 3-ASP (100 mg/kg) against the increased susceptibility to the development of seizures and long term memory impairment resulting from febrile seizures induced by hyperthermia was demonstrated. Diazepam (1 or 5 mg/kg) did not protect against long term memory impairment caused by febrile seizures. In addition, diazepam (1 mg/kg) treatment caused a significant cognitive impairment in animals kept at room temperature. These results suggest that 3-ASP had anticonvulsant action in 21-days-old rats and that this action appears to be mediated by glutamatergic and GABAergic systems. In addition, the anticonvulsant action of 3-ASP seems to be associated with its antioxidant activity. Finally, 3-ASP can represent an important tool to protect against increased susceptibility to seizures and cognitive impairment resulting from febrile seizures. / As convulsões têm conseqüências importantes em termos de mortalidade e qualidade de vida da população afetada, sendo um fator de risco para o desenvolvimento de alterações cognitivas e anormalidades comportamentais. Tendo em vista as promissoras propriedades farmacológicas das moléculas contendo selênio, no artigo 1 avaliamos a ação anticonvulsivante do (1-(2,5-difenilselenofeno-3-il)-3-metilpent-1-in-3-ol, que foi genericamente denominado de 3-alquinil selenofeno (3-ASP) frente as convulsões induzidas por pilocarpina (PC), pentilenotetrazole (PTZ) e cainato (KA) em ratos de 21 dias de vida. Os animais foram pré-tratados com 3-ASP (10, 25 ou 50 mg/kg; per oral, p.o.) ou veículo, 30 minutos antes da administração intraperitoneal (i.p.) de PC (400 mg/kg), PTZ (80 mg/kg) ou KA (45 mg/kg). Verificamos que o pré-tratamento com 3-ASP (50 mg/kg) aboliu as convulsões e a morte induzidas pela administração de PC. O 3-ASP (50 mg/kg) aumentou a latência para o primeiro episódio convulsivo, bem como, diminuiu a mortalidade e a incidência das convulsões causadas por PTZ e KA. Ainda no artigo 1, consideramos importante o estudo da ação antioxidante do 3-ASP (10, 25 e 50 mg/kg; p.o.) frente ao estresse oxidativo induzido pela PC (400 mg/kg, i.p.) em ratos de 21 dias de vida. Os resultados demonstraram que o pré-tratamento com 3-ASP mostrou-se eficaz na proteção contra a inibição da atividade cerebral da superóxido dismutase, diminuição dos níveis de ácido ascórbico, estimulação da atividade da catalase e aumento dos níveis de espécies reativas causadas pela PC. Adicionalmente, o 3-ASP protegeu contra a inibição da atividade da acetilcolinesterase e da Na+,K+-ATPase resultantes das convulsões induzidas pela PC. Em um segundo momento, o envolvimento dos sistemas glutamatérgico e GABAérgico na ação anticonvulsivante do 3-ASP foi verificado (Artigos 1 e 2). A combinação de doses sub-efetivas de 3-ASP (10 mg/kg, p.o.) e diazepam (agonista GABAérgico; 0,5 mg/kg, i.p.), 5S,10R (+)-5-metil-10,11-dihidro-5H-dibenzo [a,d] ciclohepteno -5,10- imina maleato (MK-801; antagonista não-competitivo do receptor NMDA; 0.1mg/kg, i.p.) ou 6,7-dinitroquinoxalina-2,3-diona (DNQX; antagonista de receptores não-NMDA; 5 mg/kg, i.p.) aumentou a latência para o primeiro episódio convulsivo, bem como diminuiu a incidência de convulsões induzidas pela PC. Por outro lado, a combinação de 3-ASP e 2-metil-6-feniletinil piridina hidroclorada (MPEP; antagonista do receptor glutamatérgico metabotrópico do tipo 5; 0,5 mg/kg, i.p.) não apresentou efeito protetor contra os episódios convulsivos. A administração oral de 3-ASP (50 mg/kg) causou uma inibição de 64% e 58% da captação de GABA no córtex e no hipocampo, respectivamente. Entretanto, nenhuma alteração na captação de glutamato após a administração de 3-ASP (50 mg/kg) foi observada. Adicionalmente, no artigo 2 investigamos a possível interação entre doses sub-efetivas de 3-ASP e inibidores da captação de GABA ou da GABA transaminase (GABA-T) frente às convulsões induzidas por PC em ratos de 21 dias de vida. Para isto, doses sub-efetivas de 3-ASP (10 mg/kg; p.o.) e ácido DL-2,4-diamino-n-butírico hidroclorado (DABA - um inibidor da captação de GABA; 2 mg/kg; i.p.) ou ácido aminooxiacético hemihidroclorado (AOAA um inibidor da GABA-T; 10 mg/kg, i.p.) foram co-administrados em ratos de 21 dias de vida antes da administração de PC (400 mg/kg; i.p.). A presença de episódios convulsivos foi avaliada. Verificamos que o tratamento com o 3-ASP e DABA aboliu as convulsões induzidas por PC, corroborando com nossos resultados neuroquímicos. O mesmo foi observado quando foram administradas doses sub-efetivas de 3-ASP e AOAA. Por fim, no artigo 3 investigamos o efeito do 3-ASP ou diazepam frente as convulsões, aumento da susceptibilidade ao desenvolvimento de convulsões e prejuízo na memória a longo prazo resultantes da convulsão febril induzida pela hipertermia. Os ratos de 21 dias de vida foram pré-tratados com 3-ASP (25, 50 ou 100 mg/kg; p.o), diazepam (1 ou 5 mg/kg; i.p.) ou veículo. Após o pré-tratamento, os animais foram expostos a uma temperatura de 41°C. Trinta dias após a exposição à hipertermia, avaliamos o aumento da susceptibilidade ao desenvolvimento de convulsões e prejuízo na memória a longo prazo. Verificamos que o pré-tratamento com 3-ASP ou diazepam não foi capaz de proteger contra o comportamento estereotipado, automatismos faciais e flexão corporal induzidos pela hipertermia. O efeito protetor do 3-ASP (100 mg/kg) contra o aumento da susceptibilidade ao desenvolvimento de convulsões e prejuízo na memória a longo prazo resultantes da convulsão febril induzida pela hipertermia foi verificado. O diazepam (1 ou 5 mg/kg) não protegeu contra o prejuízo na memória a longo prazo causado pela convulsão febril. Além disso, o tratamento com diazepam (1 mg/kg) nos animais mantidos a temperatura ambiente causou um significativo prejuízo cognitivo. Estes resultados sugerem que o 3-ASP apresenta ação anticonvulsivante em ratos de 21 dias de vida e que essa ação parece ser mediada pelos sistemas glutamatérgico e GABAérgico. Além disso, a ação anticonvulsivante do 3-ASP parece estar associada à sua atividade antioxidante. Por fim, o 3-ASP pode representar uma importante ferramenta para a proteção contra o aumento à susceptibilidade às convulsões e o prejuízo cognitivo resultantes das convulsões febris.

3-alquinil selenofeno

Selênio

Anticonvulsivante

Hipertermia

Estresse oxidativo

Ácido γ-aminobutírico

Glutamato

3-alkynyl selenophene

Selenium

Anticonvulsant

Hiperthermia

Oxidative stress

γ-aminobutyric acid

Glutamate

CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA

Infecção intratorácica com Paracoccidioides brasiliensis em modelo experimental murino / Intrathoracic infection with Paracoccidioides brasiliensis in experimental murine model

Alves, Caio Cesar de Souza

30 August 2007

Submitted by Renata Lopes (renatasil82@gmail.com) on 2017-02-03T13:11:46Z No. of bitstreams: 1 caiocesardesouzaalves.pdf: 1872262 bytes, checksum: f03fadd9407262d508f6744a7f73820f (MD5) / Approved for entry into archive by Adriana Oliveira (adriana.oliveira@ufjf.edu.br) on 2017-02-03T13:14:01Z (GMT) No. of bitstreams: 1 caiocesardesouzaalves.pdf: 1872262 bytes, checksum: f03fadd9407262d508f6744a7f73820f (MD5) / Made available in DSpace on 2017-02-03T13:14:01Z (GMT). No. of bitstreams: 1 caiocesardesouzaalves.pdf: 1872262 bytes, checksum: f03fadd9407262d508f6744a7f73820f (MD5) Previous issue date: 2007-08-30 / A Paracoccidioidomicose é uma micose sistêmica humana causada pelo fungo dimórfico, Paracoccidioides brasiliensis, que acomete, principalmente, indivíduos adultos do sexo masculino. O presente estudo propôs a padronização do modelo de infecção com P. brasiliensis pela via intratorácica em camundongos BALB/c. Este estudo foi monitorado pela detecção do P. brasiliensis através da contagem de unidades formadoras de colônia e pela presença de DNA do fungo nos pulmões dos animais infectados em diferentes pontos pósinfecção (2o, 7o, 15o, 30o, 45o, 60o e 90o dias) e a taxa de sobrevida dos camundongos. Além disto, foram avaliados alguns parâmetros imunológicos como a produção de óxido nítrico, TNF-alpha, IFN-gama, e IL-10 por células presentes no lavado intratorácico, contagem total e diferencial do número de células do lavado intratorácico, o estudo histopatológico dos pulmões e a detecção de anticorpos específicos anti-P. brasiliensis nos pulmões e no soro. Os resultados mostram um aumento gradual do número de colônias e de DNA de P. brasiliensis nos pulmões. Até o 15o dia após a infecção pode ser observado um aumento na produção de óxido nítrico e IFN-gama pelas células do lavado intratorácico, bem como um aumento do número total de células e da porcentagem de leucócitos mononucleares. A partir do 30o dia após a infecção observa-se um aumento de anticorpos específicos (IgG1) no soro e no pulmão, um aumento da produção de IL-10 e TNF-alpha pelas células do lavado intratorácico e conseqüente diminuição da produção de IFN-gama e óxido nítrico. Além disso, observa-se um aumento da porcentagem de células polimorfonucleares no lavado. No estudo histopatológico pode ser constatado um aumento gradual no tamanho e complexidade dos granulomas presentes nos cortes histológicos. Os camundongos utilizados no estudo de sobrevida começaram a morrer no 60o dia após a infecção. Os resultados mostram uma resposta inicial do hospedeiro com um perfil Th1 mudando durante a infecção para uma resposta Th2 que leva ao óbito dos camundongos BALB/c. / Paracoccidioidomycosis or South American blastomycosis, is a chronic granulomatous human male infection caused by the Paracoccidioides brasiliensis. The present study it considered the standardization of the model of infection with P. brasiliensis for the intrathoracic route in BALB/c mice. This study was monitored by the detection of the P. brasiliensis through the counting of colony forming units and by the presence of DNA of fungi in the lungs of the infected animals in different points (2, 7, 15, 30, 45, 60 and 90 days) and the survival rate of the mice. Moreover, some immune parameters had been evaluated as the nitric oxide production, TNF-alpha, IFN-gamma, and IL-10 for cells in the intrathoracic washed, total and distinguishing counting of cells of the intrathoracic washed, the lung histopathology and the detection of specific antibodies anti-P. brasiliensis in the lungs and serum. The results show a gradual increase of the number of colonies and P. brasiliensis DNA in the lungs. Until 15 day after the infection can be observed an increase in the nitric oxide production and IFN-gamma for the cells of the washed, as well as an increase of the total number of cells and the percentage of mononuclear. From 30 day after the infection observes an increase of specific antibodies (IgG1) in the serum and the lung, an increase of the production of IL-10 and TNF-alpha for the cells of the washed and consequent reduction of the IFN-gamma production and nitric oxide. Moreover, observed an increase of the percentage of cells polimorphonuclear in the washed. In the histopathology it can be evidenced a gradual increase in the size and complexity of granulomas in the cuts. The mice used in the survival study had started to die in 60 day after the infection. The results show an initial reply of the host with a Th1 profile moving during the infection for a Th2 reply that leads to the death of the BALB/c mice.

CNPQ::CIENCIAS DA SAUDE::MEDICINA

Paracoccidioides brasiliensis

BALB/c

Intratorácico

IFN-γ

IL-10

TNF-α

Granuloma

Paracoccidioides brasiliensis

BALB/c

Intrathoracic

IFN-γ

IL-10

TNF-α

Granuloma

Role of Immunity-Related GTPases (IRGs) for maintaining virulent Toxoplasma gondii in wild rodents

Torelli, Francesca

24 April 2020

Toxoplasma gondii ist ein weltweit verbreiteter Parasit. In Europa ernährt sich der Endwirt (Katzen) hauptsächlich von kleinen Säugetieren wie Myodes glareolus und Microtus spp. (Wühlmäusen) und Apodemus spp., seltener von Mus spp. Erstere zeigen gegenüber Mus spp. erhöhte Prävalenzen von T. gondii und überleben diese eher als Mus spp. Daher wird vermutet, dass Wühlmäusen und Apodemus spp. eine größere Rolle als Zwischenwirte besitzen, als Mus spp. Der Schutz wird auf das IFN-γ-induzierte IRGb2-b1 zurückgeführt, die den zentralen parasitären Virulenzfaktor ROP5 inhibiert. Daher liegt der Fokus meiner Arbeit auf der protektiven Rolle von IRGb2-b1 bei der Infektion mit T. gondii in Wühlmäusen und Apodemus spp. Mit dieser Arbeit trage ich nützliche Werkzeuge zur Erforschung von Wühlmäusen bei, wie ein rekombinantes M. glareolus IFN-γ Zytokin und neuartige Zellsysteme. Alle untersuchten Wühlmaus-Systeme besaßen einen Phänotyp bei Infektion mit in vivo Resistenz beschrieben wurde: einem IFN-γ-vermittelten Reduktion der Parasitenbürde (mit Wirtszelltod für Typ I Parasiten, ohne für Typ II). Darüber hinaus bestätigen vorläufige Resultate aus Wühlmäusen und Apodemus spp. in Deutschland hohe genetische Vielfalt der IRGb2 Untereinheit zeigen, insbesondere an der vermuteten Grenzfläche zum ROP5, was auf eine Rolle dieses Proteins bei der Infektion hindeutet. Um die Funktion der IRGb2-b1 Proteine zu untersuchen, habe ich ein Zellkultur System, entwickelt, welches erlaubt wild-derived Gene stabil zu exprimieren. Dieses Setup gestattet es, die Auswirkungen von Polymorphismen in Irg Genen bei der Infektion mit T. gondii zu evaluieren. Insgesamt habe ich Werkzeuge erarbeitet, um den Ansatz der Öko-Immunologie in eine Labor-Umwelt zu bringen, wodurch die molekulare Untersuchung ökologisch relevanter Arten möglich wird. Durch Anwendung dieser Werkzeuge stütze ich die Hypothese, dass nicht-Mus Nagetiere, insbesondere M. glareolus, ein bedeutendes Reservoir für T. gondii darstellen. / Toxoplasma gondii is an ubiquitous parasite grouped in three main clonal lineages, type I-III. In Europe, felids, definitive hosts for the parasite, mostly prey on small mammals of Myodes glareolus and Microtus spp. (voles), and Apodemus spp., rather than Mus spp. Voles and Apodemus spp. also display higher T. gondii prevalence and survive infection to a larger extent than Mus spp., although tolerant Mus subspecies exist. This suggests that voles and Apodemus spp. are more relevant intermediate hosts than Mus spp.. Resistance to infection relies on the IFN-γ-induced IRGb2-b1, which inhibits the major parasite virulence factor ROP5. Thus, this work focuses on the protective role of IRGb2-b1 during T. gondii infection in voles and Apodemus spp. With this project I contribute with valuable tools for research on voles, such as the supply of the recombinant M. glareolus IFN-γ cytokine and novel cell systems. All vole systems show a phenotype to type I infection which is associated with in vivo resistance in Mus spp: IFN-γ-mediated host cell death and a decrease in parasite burden. The latter without cell death was observed for type II parasites, suggesting novel protective mechanisms. Further, preliminary results from voles and Apodemus spp. in Germany confirm the expected high diversity in the IRGb2-like subunit, especially at the putative interface with ROP5, which suggests a role of the protein during infection. To assess the role of IRGb2-b1-like in this phenotype, I developed a system which allows establishment of cell lines stably expressing wild-derived Irg-like genes. This setup allows evaluation of the effect of polymorphisms of Irg-like genes during infection. Taken together, I have provided tools to bring eco-immunology into a lab setting to perform molecular investigations of ecologically relevant species. Using these tools, I offer support for the hypothesis that non-Mus rodents, especially M. glareolus, constitutes a relevant T. gondii reservoir in Germany.

Toxoplasma gondii

Wühlmäusen

Angeborene Immunität

IFN-γ

Toxoplasma gondii

Voles

Innate immunity

IFN-γ

570 Biowissenschaften; Biologie

WI 3918

YD 9412

YD 9418

ddc:570

Pistes pour une meilleure compréhension et de nouvelles modalités de traitement de la toxoplasmose / Insights towards a better understanding and novel treatment modalities of Toxoplasmosis

Hamie, Maguy

22 November 2019

Toxoplasma gondii est un parasite répandu, ayant un impact médical et vétérinaire. Chez les hôtes intermédiaires, les tachyzoïtes et les bradyzoïtes sont responsables de la toxoplasmose aiguë (TA) et chronique (TC), respectivement. Sous la réponse immunitaire, la TA évolue en TC, se manifestant par des kystes latents dans le cerveau et les muscles squelettiques. De plus, une forte corrélation existe entre la TC et plusieurs neuropathologies et cancers. Chez les patients immunodéprimés, la TC peut être réactivée et conduire à une maladie potentiellement fatale. Les traitements actuels ciblent principalement les TA, et présentent plusieurs effets secondaires. Nous nous sommes concentrés sur la TC et la compréhension de ses mécanismes moléculaires. Nous avons d’abord étudié l’efficacité de l’imiquimod contre la TA et la TC. Au cours de la TA, l'imiquimod a entraîné le recrutement de cellules T dans le péritoine et la rate de souris traitées et a considérablement diminué le nombre de kystes cérébraux lors de l'établissement de la TC. Remarquablement, le gavage de souris avec les kystes cérébraux restants chez des souris traitées à l'imiquimod n'a pas pu induire de TC. Après l'établissement de la TC, nous avons démontré que l'imiquimod réduisait considérablement le nombre de kystes cérébraux chez les souris chroniquement infectées et augmentait les récepteurs Toll-Like 11 et 12, qui se lient à une protéine du tachyzoïte, la profiline. Parallèlement, l’expression de TLR-7 augmentait, probablement par son agoniste, l'imiquimod. L'imiquimod induit une interconversion, comme l'indiquent la diminution du taux de protéine P21 et l'augmentation du taux de protéine P30, exprimées exclusivement et respectivement chez les bradyzoïtes et les tachyzoïtes. Les voies en aval de TLR-11/12 ont été activées via la voie MyD88 de signalisation, entraînant une induction ultérieure de la réponse immunitaire. In vitro, l'imiquimod n’affecte pas la souche Toxoplasma dépourvue de profiline, suggérant un rôle via le complexe Profilin/TLR-11/12. Enfin, le traitement par l'imiquimod a régulé positivement les transcrits des ligands 9 (CXCL9) et 10 (CXCL10), connus pour induire le recrutement de lymphocytes T dans des foyers réactivés du Toxoplasme afin d'éliminer l'infection.Ensuite, nous nous sommes concentrés sur les mécanismes moléculaires impliqués dans la TA et particulièrement dans la TC. Nous avons caractérisé P18, un membre de la superfamille SRS. Lorsque nous avons supprimé P18, la virulence était atténuée au cours de la TA, dû à un échappement plus rapide des tachyzoïtes du péritoine de souris, parallèle à un recrutement significatif de cellules dendritiques. De manière concomitante, moins de tachyzoïtes étaient détectés dans la rate, tandis que plus de parasites ont atteint le cerveau de souris infectées. L’élimination de P18 a augmenté le nombre de kystes de bradyzoïtes in vitro et dans le cerveau de souris infectées. Une expression induite de cytokines, notamment CXCL9 et 10, a également été observée. L’immunosuppression de souris KO P18 infectées a retardé la réactivation. L’infection orale de souris immunodéficientes ayant des macrophages fonctionnels a montré un prolongement de survie, contrairement aux souris n’ayant pas de macrophage, soulignant un rôle de l'IFN-g dans l’interconversion. Collectivement, ces données confirment le rôle de P18 dans la modulation de la réponse immunitaire, facilitant le passage des tachyzoïtes dans le cerveau et favorisant la formation de kystes. P18 joue également un rôle central dans la réactivation et la dissémination de parasites de manière dépendante de l'IFN-g. Dans l'ensemble, nous avons montré le potentiel thérapeutique prometteur de l'imiquimod contre la toxoplasmose et caractérisé le rôle de P18 dans l'immunomodulation afin de contrôler la dissémination et l'interconversion. Notre étude ouvre la voie à de nouvelles approches thérapeutiques contre la toxoplasmose, sa persistance et sa réactivation. / Toxoplasma gondii is a prevalent parasite of medical and veterinary impact. In intermediate hosts, tachyzoïtes and bradyzoïtes are responsible for acute and chronic toxoplasmosis (AT and CT), respectively. In immunocompetent patients, AT evolves, due to the host immunity, into a persistent CT, which manifests as latent tissue cysts in the brain and skeletal muscles. CT correlates with several neuro-pathologies and cancers. In immunocompromised patients, CT may reactivate and poses a life threatening condition. Current treatments primarily target AT, are limited to general anti-parasitic/anti-bacterial drugs, and associate with several limitations. Here, we focused on targeting CT and understanding its molecular mechanisms. First, we explored the efficacy of Imiquimod against AT and CT. During AT, Imiquimod led to recruitment of T cells to peritoneum and spleen of treated mice and significantly decreased the number of brain cysts upon establishment of CT. Remarkably, gavage of mice with the remaining brain cysts from Imiquimod treated mice, failed to induce CT. Post-establishment of CT, we demonstrated that Imiquimod sharply reduced the number of brain cysts in chronically infected mice, and significantly increased Toll-Like Receptors 11 and 12. These TLRs are usually expressed by dendritic cells and monocytes, and bind a tachyzoïte actin-binding protein, profilin. Concomitantly, TLR-7 was upregulated, likely by its agonist Imiquimod. Imiquimod induced interconversion as documented by the decreased protein levels of P21, and increased protein levels of P30, exclusively expressed in bradyzoïtes and tachyzoïtes respectively. Pathways downstream from TLR-11/12 were activated, through MyD88 dependent TLR signaling, which resulted in subsequent immune response induction. In vitro, Toxoplasma strain lacking profilin, does not respond to Imiquimod, suggesting a role through Profilin/TLR-11/12. Finally, Imiquimod treatment upregulated the transcript expression levels of Chemokine (C-X-C motif) ligand 9 (CXCL9) and 10 (CXCL10), known to induce T cell recruitment to reactivated Toxoplasma foci to clear the infection.Then, we focused on molecular mechanisms involved in AT and notably CT. We characterized P18, a Surface-Antigen 1 (SAG-1) Related Sequence (SRS) superfamily member. When we deleted P18, the virulence was attenuated during AT. Indeed, P18 depletion led to a faster clearance of the parasites from the peritoneum of mice, paralleled by a substantial recruitment of dendritic cells, presumably a vehicle for tachyzoïte dissemination. Concomitantly, a lower number of tachyzoïtes was detected in the spleens while a higher number of parasites reached the brains of infected mice. P18 depletion increased the number of bradyzoïte cysts, in vitro and in the brains of infected mice. An induced expression of cytokines/chemokines, including CXCL9 and 10 was also observed. Immunosuppression of infected mice with KO P18, delayed reactivation. Oral infection of Severe Combined Immunodeficiency (SCID) (with IFN-g secreting macrophages), and NOD/Shi-scid/IL-2Rgnull (NSG) mice (lacking IFN-g), showed a significant prolonged survival in infected SCID but not NSG mice. This underlines a role for IFN-g in the conversion from bradyzoïtes to tachyzoïtes. Collectively, these data support a role of P18 in orchestrating the immune response, which ultimately facilitates tachyzoïte trafficking to the brain and favors cyst formation. P18 plays also a central role in parasite reactivation and dissemination in an IFN-g dependent fashion.Altogether, we showed the promising therapeutic potential of Imiquimod against toxoplasmosis and characterized P18 role in immunomodulation to control dissemination and interconversion. Our study paves the path towards new therapeutic approaches against toxoplasmosis. It tackled key questions pertaining to establishment, maintenance and reactivation of CT and should result in a comprehensive solution to this endemic disease.

Toxoplasmose chronique

Récepteurs Toll-Like 11. 12. 7

Interféron-Γ

Réactivation

Imiquimod

P18

Chronic toxoplasmosis

Toll-Like receptors 11. 12. 7

Interferon-Γ

Reactivation

Imiquimod

P18

Studium statistických vlastností rozpadu jader / Study of statistical decay in well deformed rare-earth nuclei

Valenta, Stanislav

January 2018

The γ decay of highly excited nuclear levels can be described within the statistical model of nucleus in terms of the level density and a set of photon strength functions. The knowledge of these quantities enables more accurate calculations of reaction rates in many different reactions which are important especially in nuclear astrophysics and in the development of advanced nuclear reactors. Despite the fact that the photon strength functi- ons have been studied for decades, there are still contradicting experimental results regarding the low energy behavior of dipole strength. One of these ca- ses is the shape of electric dipole photon strength function and the strength of the scissors mode in well-deformed rare-earth nuclei. In this thesis the ana- lyses of γ-ray spectra measured by two different experimental setups are pre- sented. The two-step γ cascades measurements with odd gadolinium targets were performed at the research reactor LVR-15 at the Research Centre Řež. In the multi-step γ cascades experiments the γ rays following resonance ne- utron capture on 161−163 Dy targets were measured with the highly-segmented γ-ray calorimeter Detector for Advanced Neutron Capture Experiments in the Los Alamos Neutron Science Center at Los Alamos National Labora- tory. Experimental spectra were compared...

Biosyntéza propylprolinové stavební jednotky linkomycinu / Biosynthesis of propylproline building unit of lincomycin

Jirásková, Petra

January 2020

The clinically used antibiotic lincomycin consists of an amino-sugar and an amino-acid moiety. The incorporated amino-acid 4-propyl-L-prolin (PPL) is very important for the linomycin bioactivity, as evidenced by the lower activity of the related antibiotic celesticetin, which incorporates proteinogenic L-prolin instead. Gene clusters for the biosynthesis of both lincosamides are published and reflect a common basis - biosynthesis of amino-sugar precursor and condensation reactions. Additionally, in the biosynthetic gene cluster for lincomycin there is a sub-cluster of genes encoding the biosynthesis of PPL, the alkylated proline derivative (APD). PPL has a common biosynthetic origin with other APDs that are part of the structures of antitumor pyrrolobenzodiazepines and the signal molecule hormaomycin, which is also reflected in the presence of homologous genes in their gene clusters. The acquired knowledge on PPL biosynthesis thus can be applied to a larger group of natural products. The first overall concept of APD biosynthesis was published forty years ago. The milestone was the year 1995 when the gene cluster for lincomycin biosynthesis was published and specific gene products have been proposed for individual biosynthetic steps. The functional proof of proteins has been performed so far just...

Homogenization of Rapidly Oscillating Riemannian Manifolds

Hoppe, Helmer

12 April 2021

In this thesis we study the asymptotic behavior of bi-Lipschitz diffeomorphic weighted Riemannian manifolds with techniques from the theory of homogenization. To do so we re-interpret the problem as different induced metrics on one reference manifold. Our analysis is twofold. On the one hand we consider second-order uniformly elliptic operators on weighted Riemannian manifolds. They naturally emerge when studying spectral properties of the Laplace-Beltrami operator on families of manifolds with rapidly oscillating metrics. We appeal to the notion of H-convergence introduced by Murat and Tartar. In our first main result we establish an H-compactness result that applies to elliptic operators with measurable, uniformly elliptic coefficients on weighted Riemannian manifolds. We further discuss the special case of locally periodic coefficients and study the asymptotic spectral behavior of Euclidean submanifolds with rapidly oscillating geometry. On the other hand we study integral functionals featuring non-convex integrands with non-standard growth on the Euclidean space in a stochastic framework. Our second main result is a Γ-convergence statement under certain assumptions on the statistics of their integrands. Such functionals provide a tool to study the Dirichlet energy on non-uniformly bi-Lipschitz diffeomorphic manifolds. We show Mosco-convergence of the Dirichlet energy and deduce conditions for the spectral behavior of weighted Riemannian manifolds with locally oscillating random structure, especially in the case of Euclidean submanifolds.:Introduction Outline Notation I. Preliminaries 1. Convergence of Riemannian Manifolds 1.1. Hausdorff-Convergence 1.2. Gromov-Hausdorff-Convergence 1.3. Spectral Convergence 1.4. Mosco-Convergence 2. Homogenization 2.1. Periodic Homogenization 2.2. Stochastic Homogenization II. Uniformly bi-Lipschitz Diffeomorphic Manifolds 3. Uniformly Elliptic Operators on a Riemannian Manifold 3.1. Setting 3.2. Main Results 3.3. Strategy of the Proof and Auxiliary Results 3.4. Identi cation of the Limit via Local Coordinate Charts 3.5. Examples 3.6. Proofs 4. Application to Uniformly bi-Lipschitz Diffeomorphic Manifolds 4.1. Setting and Results 4.2. Examples 4.3. Proofs III. Rapidly Oscillating Random Manifolds 5. Integral Functionals with Non-Uniformal Growth 5.1. Setting 5.2. Main Results 5.3. Strategy of the Proof and Auxiliary Results 5.4. Proofs 6. Application to Rapidly Oscillating Riemannian Manifolds 6.1. Setting and Results 6.2. Examples 6.3. Proofs Summary and Discussion Bibliography List of Figures

info:eu-repo/classification/ddc/510

ddc:510

Multivariable (φ,Γ)-modules and representations of products of Galois groups

Pupazan, Gheorghe

22 October 2021

Für eine Primzahl p, sei L eine endliche Erweiterung von $QQ_p$ mit Ganzheitsring $O_L$ und Restklassenk\"{o}rper $kk_L$. Sei ferner n eine positive ganze Zahl. In dieser Arbeit beschreiben wir die Kategorie der endlich erzeugten stetigen Darstellungen der n-ten direkten Potenz der absoluten Galoisgruppe $G_L$ von L mit Koeffizienten in $O_L$, unter Verwendung einer verallgemeinerten Version der $(phi, Gamma)$-Moduln von Fontaine. In Kapitel 4 beweisen wir, dass die Kategorie der stetigen Darstellungen der n-ten direkten Potenz von $G_L$ auf endlichen dimensionalen $kk_L$-Vektorräumen und die Kategorie étaler $(phi, Gamma)$-Moduln über einem n-variablen Laurentreihenring über $kk_L$ äquivalent sind. In Kapitel 5 erweitern wir diese Äquivalenz, um zu beweisen, dass die Kategorie der stetigen Darstellungen der n-ten direkten Potenz von $G_L$ auf endlich erzeugten $O_L$-Moduln und die Kategorie étaler $(phi, Gamma)$-Moduln über einem n-variablen Laurentreihenring über $O_L$ äquivalent sind. Einerseits erhalten wir, wenn wir n=1 und L willkürlich lassen, die Verfeinerung von Fontaine ursprünglicher Konstruktion gemäß Kisin, Rin und Schneider, die Lubin-Tate Theorie verwenden. Wenn wir andererseits n willkürlich lassen und $L=QQ_p$, erhalten wir die Theorie von Zábrádi von multivariablen zyklotomischen $(phi, Gamma)$-Moduln, die Fontaines Verwendung einer einzelnen freien Variablen verallgemeinert. Daher bietet unsere Arbeit einen gemeinsamen Rahmen für diese beiden Verallgemeinerungen. / For a prime number p, let L be a finite extension of $QQ_p$ with ring of integers $O_L$ and residue field $kk_L$. We also let n be a positive integer. In this thesis we describe the category of finitely generated continuous representations of the n-th direct power of the absolute Galois group $G_L$ of L with coefficients in $O_L$ using a generalized version of Fontaine's $(phi, Gamma)$-modules. In Chapter 4 we prove that the category of continuous representations of the n-th direct power of $G_L$ on finite dimensional $kk_L$-vector spaces is equivalent to the category of étale $(phi, Gamma)$-modules over a n-variable Laurent series ring over $kk_L$. In Chapter 5 we extend this equivalence to prove that the category of continuous representations of the n-th direct power of $G_L$ on finitely generated $O_L$-modules is equivalent to the category of étale $(phi, Gamma)$-modules over a n-variable Laurent series ring over $O_L$. On the one hand, if we let n=1 and $L$ be arbitrary, we obtain the refinement of Fontaine's original construction due to Kisin, Rin and Schneider, which uses Lubin-Tate theory. On the other hand, if we let n be arbitrary and $L=QQ_p$, we recover Zábrádi's theory of multivariable cyclotomic $(phi,Gamma)$-modules that generalizes Fontaine's use of a single free variable. Therefore, our thesis provides a common framework for both of these generalizations.

p-adische Darstellung

(φ,Γ)-Moduln

Lubin-Tate Gruppe

Lokaler Körper

p-adic representation

(φ,Γ)-Modules

Lubin-Tate group

local fields

510 Mathematik

SK 260

ddc:510