Benzo- et naphtopyranes annelés par des éthers couronnes : synthèse, photochromisme et pouvoir complexant vis-à-vis des cations métalliques et des acides aminés / Crown ether annelated benzo- and naphtopyrans : synthesis, photochromism, and coordination ability towards metal cations and amino acids

Paramonov, Sergey

19 November 2010

Les chromènes photochromiques sont largement utilisés dans les technologies modernes en raison de leur capacité à changer les propriétés sous irradiation UV. Les chromènes présentés dans ce travail possèdent en outre des fragments pouvant participer à la coordination avec des cations métalliques, acides aminés, ou de l'ADN. Pour ce type de molécule, l'interdépendance éventuelle entre les propriétés photochromiques et complexantes permet d'envisager soit le photo-contrôle de la complexation, soit la modulation du photochromisme par le biais de coordination.Ce travail est divisé en deux parties : la première est consacrée à la préparation des molécules cibles et la seconde à l'étude de la complexation. Les approches synthétiques élaborées ont permis d'obtenir une série de nouveaux chromènes annelés par des éthers couronnes de taille et de composition hétéroatomique différentes. Le processus de complexation de certains dérivés a été étudié en détail par spectroscopie RMN et absorptionUV-Visible. Il a été établi que la nature des cations métalliques détermine la stoechiométrie du complexe formé ainsi que la structure spatiale. Pour tous les composés étudiés, la complexation affecte les paramètres photochromiques notamment la vitesse de décoloration. En ce qui concerne la complexation des chromènes synthétisés avec les acides aminés protonés, il a été établi qu'en fonction de la longueur de chaine de ces acides, la formation de complexe mono- ou ditopique est favorisée.De plus, l'interaction d'un nouveau chromène cationique avec l'ADN a été étudiée. Il a été constaté que contrairement à la forme initiale, la forme colorée de ce composé générée sous irradiation UV permet l'intercalation au sein de l'ADN / Photochromic chromenes are widely used in modern technologies due to their abilityto change their properties upon UV irradiation. The chromenes presented in this work alsopossess fragments able to participate to the coordination with metal cations, amino acids, orDNA. These properties may sustain mutual influence on each other resulting in either photocontrolof complexing ability or photochromism tunable by complex formation.This work is divided in two parts, one devoted to the synthesis of the targetcompounds and the second to study on the complexing ability of the substances,respectively. Thus, the synthetic approaches to photochromic benzo- and naphthopyrans,annelated to the crown ether moieties of different size and heteroatomic composition, weredeveloped. The complex formation of several chromenes with metal cations wasinvestigated by means of UV-Vis absorption and NMR spectroscopies. The metal cationnature was found to determine the stoichiometry of the complexes as well as their spatialstructure. The complex formation was found to affect the photochromic properties of thecompounds, especially the bleaching rate. Investiga.on of complexation of the chromeneswith protonated amino acids revealed that, depending on the length of the carbon chain ofthe acid used, mono- or ditopic complexes may be formed.The interaction of the new chromene, possessing a positively charged group, with DNAwas also studied. In contrast to the initial form, the photo-induced colored form was foundto intercalate with DNA.

Chromènes

Photochromisme

Éthers couronnes

Complexation

Acides aminés

Cations métalliques

Chromenes

Photochromism

Crown ethers

Complex formation

Amino acids

Metal cations

Mn(III)porfirinas sintéticas como modelos químicos do Citocromo P-450: a O-desalquilação oxidativa de aril éteres substituídos como modelos de drogas por iodosilbenzeno / Synthetic Mn(III)porphyrins as cytochrome P-450 mimic: oxidative O-dealkylation of aryl substituted ethers by iodosylbenzene as drug models

Felipucci Neto, Carlos Alberto

03 October 2007

Reações de O-desmetilação oxidativa estão entre as várias oxidações realizadas pelas enzimas do citocromo P-450. Entretanto, poucos estudos de O-desmetilação catalisadas por enzimas do citocromo P-450 ou modelos químicos baseados em metaloporfirinas sintéticas têm resultado em dúvidas acerca do mecanismo da O-desmetilação destes compostos orgânicos. Neste trabalho, foi estudada a O-desmetilação oxidativa, com PhIO, do benzil metil éter e alguns de seus derivados para substituídos (com os grupos doadores de elétrons -OCH3 e -CH3 e os grupos retiradores -NO2 e -Cl) catalisada pelas Mn(III)P [Mn(TPP)]Cl, [Mn{T(4-N-MePy)P}](PF6)5, [Mn(TMP)]Cl, [Mn(TDCSPP)]Cl e [Mn(TFPP)]Cl para verificar o efeito destes diferentes catalisadores na conversão e seletividade de produtos da O-desmetilação oxidativa e avaliar o efeito dos diversos substituintes citados no mecanismo de O-desalquilação. Inicialmente, realizou-se o estudo das oxidações catalíticas do metil benzil éter. Todas as reações catalisadas pelas MnP se mostram seletivas, sendo que o benzaldeído foi o produto comum a todas as oxidações. A melhor condição encontrada foi 1:50:1224 (catalisador/oxidante/substrato). Em relação às reações com os substratos contendo os substituintes na posição -para, as reações de oxidações catalíticas do p-metóxibenzil metil éter por PhIO não se mostraram tão seletivas quanto as do metil benzil éter, mostrando claramente que o grupo metóxi alterou a reatividade do aril éter original. Mesmo assim, o p-metoxibenzaldeído ainda foi o produto principal, sendo a conversão ao álcool p-metoxibenzílico observada em escala menor. Já com o substrato p-nitrobenzil metil éter, novamente o efeito provocado pelo substituinte na posição para no anel benzênico pôde ser percebida na distribuição final dos produtos, sendo que houve seletividade total para a formação de p-nitrobenzaldeído em detrimento ao álcool p-nitrobenzóico. Em relação aos dois últimos substratos da série proposta, metil p-metilbenzil éter e metil p-clorobenzil éter, de um modo geral, as reações realizadas com o p-clorobenzil metil éter não se mostraram tão seletivas quanto as do metil p-nitrobenzil éter, mostrando que o grupo cloro aumentou a reatividade do cloroéter em relação ao éter com o substituinte nitro- original. Mesmo assim, o p-clorobenzaldeído foi o produto principal, sendo a conversão ao álcool p-clorobenzílico observada em menor escala. Em relação às reações de oxidação do p-metilbenzil metil éter, observou-se que os resultados experimentais são semelhantes aos encontrados para o metil benzil éter. Esses resultados corroboram o principal mecanismo proposto para os sistemas modelo do citocromo P-450 que envolve abstração inicial do átomo de hidrogênio, o mecanismo por recombinação de oxigênio. / O-dealkylation oxidative reactions are among the several oxidations accomplished by the cytochrome P-450 enzymes. However, few studies on O-dealkylation catalyzed by such enzymes or chemical models based on synthetic metalloporphyrins have resulted in doubts concerning the mechanism of these reactions involving organic compounds. In this work, we studied the oxidative O-dealkylation by PhIO of benzyl methyl ether and some of its para-substituted derivatives (with the electron donor groups -OCH3 and -CH3 and the electronwithdrawing groups -NO2 and -Cl) catalyzed by the following Mn(III)P: [Mn(TPP)]Cl, [Mn{T(4-N-MePy)P}] (PF6)5, [Mn(TMP)]Cl, [Mn(TDCSPP)] Cl, and [Mn(TFPP)]Cl. Our aim was to verify the effect of these different catalysts on the conversion yields and product selectivity, as well as evaluate the effect of the several substituents on the ether on the O-dealkylation mechanism. We initially studied the catalytic oxidation of methyl benzyl ether. All the reactions catalyzed by the various MnPs were selective, and benzaldehyde was the product common to all oxidations. The best reaction condition was catalyst/oxidant/substrate molar ration = 1:50:1224. As for the reactions with the substituted substrates, the catalytic oxidation of p-methoxybenzyl methyl ether by PhIO was not as selective as the ones of methyl benzyl ether, clearly showing that the methoxy group affects the reactivity of the original aryl ether. Nevertheless, p-methoxybenzaldehyde was still the main product, being the conversion to p-methoxybenzylic alcohol observed in minor amount. With the substrate p-nitrobenzyl methyl ether, the effect of the electronwithdrawing substituent in the para- position of the aromatic ring could be observed in the final product distribution once again, and total selectivity toward the formation of p-nitrobenzaldehyde to the detriment of p-nitrobenzoic alcohol was observed. In relation to the two last substrates of the proposed series, the methyl p-methylbenzyl and methyl p-chlorobenzyl ethers, the reactions accomplished with p-chlorobenzyl methyl ether were not as selective as the ones carried out with methyl p-nitrobenzyl ether, showing that the chloro group increased the reactivity of the chloro-ether in relation to the ether with the original nitro- substituent. Even so, p-chlorobenzaldehyde was the main product, being the conversion to the p-chlorobenzylic alcohol observed in smaller amount. Concerning the oxidation reactions of p-methylbenzyl methyl ether, the experimental results were similar to those obtained in the case of methyl benzyl ether. These results corroborate the main mechanism proposed for the cytochrome P-450 model systems, which involves initial hydrogen atom abstraction, followed by oxygen rebound.

Avaliação dos congêneres BDE-100 e BDE-153 de éteres difenílicos polibromados sobre a linhagem celular HepG2 e linfócitos humanos: efeitos citotóxicos, genotóxicos e mutagênicos / Evaluation of the effects of polybrominated diphenyl ethers congeners, BDE-100 and BDE-153, on the HepG2 cell line

Pereira, Lílian Cristina

28 July 2016

Os retardantes de chama bromados são substâncias utilizadas em bens de consumo para aumentar sua resistência ao fogo e/ou altas temperaturas. Para este fim os Éteres Difenílicos Polibromados (PBDEs do inglês polybrominated diphenyl ether) representam a classe mais utilizada tendo em vista sua eficiência no controle da propagação da chama e baixo custo. Estes compostos são considerados persistentes, bioacumuláveis, podem ser transportados para longas distâncias e apresentam toxicidade podendo causar desregulação endócrina, entretanto os mecanismos de toxicidade ainda não foram bem estabelecidos. Desta forma, o presente projeto utilizou linhagens celulares de Hepatoblastoma Humano (HepG2), HeLa, Hepatócitos e linfócitos humanos a fim de elucidar seus mecanismos de toxicidade. Os resultados significativos demonstram a capacidade destes compostos em induzir dano primário no DNA (0,5 ?mol/L para o BDE-153 e 5 ?mol/L para o BDE-100) monitorado pelo teste do cometa, que não foi reparado após 24 horas de exposição. No entanto, não se observou um aumento de micronúcleos em HepG2 e linfócitos após exposição aos congêneres (0,1 - 25 ?mol/L) nem mesmo mutagenicidade no ensaio de Salmonella typhimurium. Contudo, os compostos apresentam capacidade de diminuir a redução do brometo de 3-(4,5 dimetiltiazol-2il)-2,5 difenil tetrazólio (MTT), proliferação e interferem no ciclo celular nos cultivos celulares avaliados. Estes efeitos de citotoxicidade estão relacionados com a disfunção mitocondrial, uma vez que ambos PBDEs geram dissipação do potencial de membrana mitocondrial, formação e acúmulo de espécies reativas, culminando em morte celular apoptótica, demonstrada pela manutenção da fosfatidil serina na face externa da membrana celular, pela condensação e fragmentação nuclear, presença de fatores pró-apoptóticos no citosol da célula, tais como citocromo C e AIF além da ativação de caspases 3 e 9. Estes dados corroboram com o fato de não ter liberação de lactato desidrogenase intracelular, excluindo a morte celular por necrose. E por fim, foi possível observar que a exposição aos compostos ativa o processo autofágico, a princípio como um mecanismo de citoproteção observado pela conversão de LC3I em LC3II e acúmulo de p62 (marcadores autofágicos) além de marcações imunicitoquímicas para LC3II e co-localização de lisossomos no padrão pontuado, indicanto acúmulos da proteína LC3 e lisossomos, formando os autofagossomos. Em conjunto nossos resultados apresentam a capacidade de induzir instabilidade genômica e citotoxicidade desta classe de compostos, reforçando a idéia de que os PBDEs representam risco à população exposta / The brominated flame retardants are substances used in consumer goods to increase its fire resistance and/or high temperatures. Due to, the polybrominated diphenyl ethers (Polybrominated diphenyl ether) are the most commonly used class in view of its efficiency in controlling the spread of flame and low cost. These compounds are considered persistent, bioaccumulative, can be transported over long distances and have toxicity. However the toxic mechanisms of action have not been well established. Thus, this project held cytotoxic, genotoxic and mutagenic assays in HepG2, HeLa, hepatocytes and human lymphocytes cells in order to elucidate the mechanisms of toxicity. The results demonstrate the ability of these compounds to induce primary DNA damage (0.5 ?M for BDE-153 and 5 ?M for BDE-100) monitored by the comet assay, it was not repaired after 24 hours of exposure. However, there was not observed nether increase in micronuclei in HepG2 cells and lymphocytes after exposure to the congeners (0.1 - 25 ?M) even in the Salmonella typhimurium mutagenicity assay. However, the compounds show the ability to reduce MTT reduction, proliferation, and interfere with cell cycle evaluated in cell cultures. These cytotoxic effects are related to mitochondrial dysfunction, since both PBDE generate dissipation of the mitochondrial membrane potential, accumulation of reactive oxygen species, resulting in apoptotic cell death, demonstrated by the maintenance of serine phosphatidyl on the external surface of the cell membrane, by condensation and nuclear fragmentation, the presence of pro-apoptotic factors in the cytosol of the cell, such as cytochrome c and AIF plus activating caspase 3 and 9. These data corroborate the fact of not having to intracellular lactate dehydrogenase release, excluding death cell necrosis. Finally, it was observed that exposure to the active compounds the autophagic process, at first as a cytoprotective mechanism observed by LC3I conversion in LC3II and accumulation of p62 (autophagic markers) plus imunicitoquímicas markings for LC3II and co-location lysosomes in dotted pattern, indicanto accumulations of LC3 protein and lysosomes, forming autophagosomes. Together our results show the ability to induce genomic instability and cytotoxicity of this class of compounds, reinforcing the idea that PBDEs pose a risk to the exposed population

Citotoxicidade

Cytotoxicity

Flame retardants

Genotoxicidade e Autofagia

Genotoxicity and Autophagy

Polybrominated difenilas Ethers (PBDEs)

Retardantes de chama

An investigation of the phototoxicity of decabromodiphenyl ether and triclosan

Suh, Yang-Won

01 December 2010

Decabromodiphenylether (deca-BDE) and triclosan (2,4,4'-trichloro-2'-hydroxydiphenylether) are used in consumer products as flame retardant and bactericide, respectively. Dermal contact is a major human exposure pathway. Deca-BDE and triclosan are known to be photolytically degraded to compounds like lower-BDEs and dioxins. My hypothesis is that photolysis of deca-BDE and triclosan generates free radicals and degradation products which cause toxic effects including cytotoxicity, growth inhibition, oxidative stress and genotoxicity in skin. To test this hypothesis radical formation and photolytic products of deca-BDE and toxic effects of deca-BDE and triclosan alone/with UV-exposure were determined using immortal human keratinocytes (HaCaT) and primary human skin fibroblasts (HSF). My electron paramagnetic resonance and GC-MS studies indicate that deca-BDE is photoreactive and UV irradiation of deca-BDE in organic solvents generates free radicals and lower-BDEs. The free radical formation is wavelength-dependent and positively related to the irradiation time and deca-BDE concentration. In structure-activity relationship studies with deca-BDE, octa-BDE, PBB 209, PCB 209 and diphenyl ether, the presence of halogen atoms (Br > Cl), and/or an ether bond enhance free radical formation. Debromination and hydrogen abstraction from the solvents are the mechanism of radical formation with deca-BDE, which raises concerns about possible toxic effects in UV-exposed skin. In cell culture experiments high levels of triclosan plus UV irradiation and repetitive deca-BDE and UV exposures caused synergistic cytotoxicity in HaCaT. However, neither triclosan nor deca-BDE can be regarded as a phototoxicant following the OECD test and evaluation guidelines. In HSF, no synergistic cytotoxicity was observed, although HSF were more sensitive to deca-BDE and triclosan alone than HaCaT. Contrary to expectations, the photodegradation products of triclosan were less toxic than triclosan itself to HaCaT. However, UV irradiation of triclosan-exposed cells produced a dose dependent increase in intracellular oxidative stress (dichlorofluorescein formation). Comet experiments did not show consistent results of genotoxicity in HaCaT. Overall, deca-BDE and triclosan had no or weak phototoxic potential in cells with the experimental conditions employed. To my knowledge, my research is the first prove of free radical formation during UV irradiation of deca-BDE and the first investigation of phototoxicity of deca-BDE and triclosan in human skin cells.

Electron paramagnetic resonance (EPR)

Free radicals

Phototoxicity

Polybrominated diphenyl ethers (PBDEs)

Skin cells

Triclosan

Conception, Synthèse et Caractérisation de Nouveaux Systèmes de Guidage et de Vectorisation pour la Cancérologie

GARANGER, Elisabeth

27 June 2005

Sur-exprimée par les cellules endothéliales des néo-vaisseaux tumoraux, l'intégrine alphaV béta3 (aVb3) constitue une cible judicieuse pour atteindre les foyers tumoraux et empêcher la vascularisation des tumeurs. À ces fins, nos travaux ont été consacrés à la conception, la synthèse et la caractérisation biologique de nouveaux vecteurs synthétiques ciblant l'intégrine aVb3. Le squelette du vecteur est un cyclodécapeptide RAFT, présentant deux faces d'adressage indépendantes, permettant la séparation dans l'espace du domaine des ligands, assurant le ciblage du vecteur, de celui supportant les molécules à vectoriser. La fonction de ciblage est assurée par la présentation de quatre motifs cyclopentapeptidiques c[-RGDfK-], ligands de l'intégrine aVb3, greffés sur la face supérieure du RAFT. L'architecture multivalente a été synthétisée de manière convergente par formation de liens éthers d'oxime, stables in vitro et in vivo, grâce à des réactions chimiosélectives hautement efficaces. La conjugaison du vecteur RAFT(c[-RGDfK-])4 à diverses molécules de détection a permis d'étudier ses propriétés biologiques in vitro et in vivo. Son interaction avec les cellules HEK293(b3) induit le clustering des intégrines aVb3 et conduit à un phénomène d'endocytose récepteur-dépendante. Chez un modèle animal murin, le vecteur (Cy5)RAFT(c[-RGDfK-])4, administré par voie systémique, détecte des tumeurs localisées ou métastatiques. Pour accroître son efficacité anti-tumorale, nous avons conjugué notre vecteur à différentes drogues cytotoxiques. Le peptide (KLAKLAK)2, la doxorubicine et la chaîne A de la ricine ont été couplés par des liens disulfures favorisant leur libération intracellulaire.

[CHIM:OTHE] Chemical Sciences/Other

Néo-angiogenèse tumorale

Vectorisation non-virale

Cyclodécapeptide RAFT

Ligand -RGD-

Multivalence

Liaisons Ethers d'oxime

Liaisons disulfures

Dietary intake estimations of brominated flame retardants for Swedish children

Lindström, Jonna

January 2008

<p>The dietary intake of polybrominated diphenyl ethers (PBDEs) and hexabromocyclododecane (HBCD) have been estimated for Swedish children. A dietary survey performed in 2003, including 4, 8-9 and 11-12 year olds, and concentrations in individual food items were combined. The food included in the study was mainly of animal origin, consisting of fish and shellfish, dairy products, meat products, eggs, animal and vegetable fats and fats from miscellaneous food products. The medium-bound intake of PBDEs (9 congeners) were estimated to 23.0 ng/day, 30.9 ng/day and 27.7 ng/day for 4, 8-9 and 11-12 years olds respectively. The corresponding estimations for HBCD were 7.94 ng/day 10.7 ng/day and 9.46 ng/day for 4, 8-9 and 11-12 years olds respectively. These results show a higher daily intake for 8-9 year olds compared with the other age groups. However, when estimating the daily intake per kg bw, the intake decreases with age. BDE-47 contributed the most to the total intake of PBDEs, with approximately 40%. The food group contributing the most to the intake of PBDEs and HBCD was fish and shellfish, of which non-Baltic fatty fish was the largest contributor. There were no considerable differences between boys and girls in any of the aspects examined. The result from this study show a lower intake of PBDEs and HBCD in Swedish children compared with children in other studies made in Europe and the United States.</p> / <p>Bromerade flamskyddsmedel används för att skydda brännbara material från att fatta eld, till exempel skyddas textilier och plaster i bland annat elektronik, fordon och möbler. Två typer av bromerade flamskyddsmedel är polybromerade difenyletrar (PBDE) och hexabromocyklododekan (HBCD). Dessa är additiva flamskyddsmedel och blandas i materialet som ska skyddas men binder inte in i produkten och kan därför lätt läcka ut i miljön, vilket också har skett. Halter har påträffats i miljön och i biota långt från plaster där ämnena produceras eller används.</p><p>PBDE och HBCD har visats ha hormonstörande och neurotoxiska effekter i studier på råtta och mus. Thyroxinnivåerna sjunker vid exponering av PBDE och HBCD, vilket skulle kunna leda till sköldkörtelproblem och störd utveckling av bland annat hjärnan om exponering sker perinatalt. De neurotoxiska effekterna inkluderar inlärnings- och minnessvårigheter och ett förändrat beteende med hyper- och hypoaktivitet som följd.</p><p>Human exponering för PBDE och HBCD sker främst via födan och speciellt via animaliska produkter då dessa ämnen är lipofila, bioackumulerande och ofta biomagnifierande vilket gör att de påträffas i högre koncentrationer högre upp i trofinivåerna. Studier från bland annat Sverige och Finland visar att fisk och skaldjur är den största källan till intag av PBDE.</p><p>De flesta intagsberäkningar av PBDE och HBCD baseras på livsmedelskonsumtionen hos vuxna och visar följaktligen endast hur intaget ser ut för den delen av populationen. För barn, som är en av de känsligaste grupperna i populationen, finns inte många studier att tillgå, varken från Sverige eller andra delar av världen. I den här studien har därför intaget av PBDE (summan av 9 kongener) och HBCD beräknats för barn i Sverige.</p><p>I en rikstäckande kostundersökning utförd 2003 deltog barn i åldrarna 4, 8-9 och 11-12 år. De fick i en matdagbok ange sin konsumtion under fyra på varandra följande dagar. Data från denna undersökning kombinerades sedan med haltdata från olika livsmedel för att räkna ut intaget av PBDE och HBCD på individbasis. Undersökningen innefattade främst animaliska livsmedel och innehöll därför fisk och skaldjur, mejeriprodukter, köttprodukter, ägg, animaliskt och vegetabiliskt fett och fett från övriga livsmedel.</p><p>Resultaten visar att födointaget av PBDE var 23,0 ng/dag, 30,9 ng/dag och 27,7 ng/dag för 4, 8-9 respektive 11-12 åringar. Intaget av HBCD beräknades till 7,94 ng/dag, 10,7 ng/dag och 9,46 ng/dag för 4, 8-9 respektive 11-12 åringar. Detta visar att 8-9 åringar har det högsta dagliga intaget av PBDE och HBCD. När intaget beräknas på kroppsvikt däremot, har de yngsta barnen det högsta intaget som sedan sjunker med åldern. Fisk och skaldjur var den största källan till intaget av PBDE och HBCD, trots att konsumtionen av dessa livsmedel var relativt lågt. Det fanns ingen större skillnad mellan pojkar och flickor, varken i intag av PBDE eller av HBCD. Jämfört med de få studier som gjorts i andra länder, är det tydligt att svenska barn har ett lägre intag av PBDE och HBCD.</p><p>Undersökningen tyder också på att intaget av PBDE och HBCD hos svenska barn, utifrån de kunskaper vi har idag, inte utgör någon risk med avseende på de effekter av PBDE och HBCD som påträffats i toxikologiska studier. Däremot är barn i ett känsligt skede i livet och upprepad exponering samt exponering för flera miljögifter samtidigt skulle kunna påverka deras utveckling negativt.</p>

Polybrominated diphenyl ethers (PBDEs)

Hexabromocyclododecane (HBCD)

Dietary intake

Children

Toxicology

Endocrine disruptor

Neurotoxicity

Sweden

Biology

Biologi

Toxicology

Toxikologi

Neonatal Developmental Neurotoxicity of Brominated Flame Retardants, the Polybrominated Diphenyl Ethers (PBDEs)

Viberg, Henrik

January 2004

<p>This thesis examines developmental neurotoxic effects of polybrominated diphenyl ethers (PBDEs), PBDE 99, PBDE 153, and the fully brominated PBDE 209, after exposure during the newborn period in rodents.</p><p>Our environment contains vast numbers of contaminants, including the flame retardants, PBDEs. The PBDEs are widely found in the environment and are increasing in human milk. Individuals can be exposed to PBDEs during their whole lifetime, and especially during the lactation period. The neonatal period, coinciding with the lactation period, is characterized in many mammalian species by rapid growth and development of the immature brain. It has been shown that numerous toxicants can induce permanent disorders in brain function when administered to the neonatal mouse during the brain growth spurt (BGS). In mice and rats this period is postnatal, spanning over the first 3-4 weeks of life, while in humans, BGS begins during the third trimester of pregnancy and continues throughout the first two years of life.</p><p>The present studies identified a defined critical period during BGS in mice when the brain is vulnerable to insults of low doses of PBDEs and that it is the presence of PBDEs or their metabolites in the brain during this critical period that is crucial to evoking neurotoxic effects. The effects observed are permanent altered spontaneous behavior, reduced habituation, deficits in learning and memory, and disturbances in the cholinergic system. These effects worsen with age.</p><p>The ability of PBDEs to induce neurotoxic effects does not appear to be gender-, strain- or species-specific, because the neurotoxic effects are induced in rats and male and female mice of different strains.</p><p>The developmental neurotoxic effects of PBDEs are similar to those observed for polychlorinated biphenyls (PCBs) and possible interactive effects of PBDEs and other environmental contaminants are therefore of concern.</p>

Biology

brominated flame retardants

polybrominated diphenyl ethers

PBDE

neonatal

development

neurotoxicity

behaviour

cholinergic system

Biologi

Biology

Biologi

Self Assembly at the Liquid Air Interface

Petru, Niga

January 2010

The aim of this work is to study the interfacial properties of amphiphilic compounds at the liquid–air interface in an attempt to develop a comprehensive understanding of their orientation as well as the influence of their interaction with the solvent on the interfacial layer properties. Using Vibrational Sum Frequency Spectroscopy (VSFS) as the main tool, the molecular structure of the amphiphilic layer and the amphiphile–solvent relation can be illuminated in great detail – it is arguably the most sensitive surface spectroscopy currently available. Due to its second order nature, the VSFS technique is capable of distinguishing molecules at the interface even in the presence of a vast excess of similar molecules in the bulk.Ionic liquids (Ils) form a class of solvent which are increasingly receiving attention as ``green solvents´´. Some of these, such as ethyl ammonium nitrate (EAN), a protic IL, have the capacity to hydrogen bond extensively which is one of the important features they share with water. Since the interaction with solvent is an important consideration for self assembly and it is known that surfactant self assembly in the EAN bulk is analogous to in water, it was considered of interest to probe self assembly at EAN–air interface. To this end the interfacial structure of the pure EAN interface was probed, as was the conformation and ordering of nonionic surfactants. These studies reveal that EAN is highly ordered at the interface, exposing the ethyl moiety to the gas phase. Additionally, polarization studies have enabled the average orientation of the ethyl group to be determined. Adsorption of nonionic surfactants at the interface appears to significantly displace the EAN from the interface. The headgroup of the surfactant, a linear ethylene oxide group, appears to be highly disordered.The disorder of the linear ethylene oxide groups has led to difficulties in their surface spectroscopic fingerprinting in this and other works. In an attempt to study the interfacial behaviour of ethylene oxide and the temperature dependence of its hydration, closed loop structures of PEO attached to hydrophobic groups were also probed. This essentially locks their conformation. Such molecules are known as crown ethers and display interesting interfacial behaviour and also the ability to bind cations. The presence of even small amounts of adsorbed crown ethers at the water interface is shown to considerably perturb the water structure. The NO, CN, COC and CH vibrational modes of these compounds at the air-water interface as well as OH vibrational modes of the surface water hydrating this compound have been targeted in order to obtain molecular information about arrangement and conformation. The CH2 vibrational modes of crown ethers have been identified and found to be split due to their interaction with ether oxygen. The spectra provide evidence for the existence of a protonated crown complex moiety at the surface leading to the appearance of strongly ordered water species. The orientation of Nitrobenzo crown (NB15C5) was monitored as a function of solution concentration, by targeting the ratio of peak intensities of the CN and NO2 vibrational modes. The water of hydration has also been probed as a function of crown concentration, salt concentration, and temperature. The latter study strongly suggests that the surface can be treated as a charged interface, and that the associated ordered water decreases with increasing ionic strength of the bulkFinally, insoluble monolayers of fatty acids spread on a water surface have also been studied in an effort to further understand the relationship between molecular architecture and film structure. Fatty acid (Arachidic Acid – AA and Eicosenoic Acid – EA) monolayers are compared to investigate the effect on the monolayer structure of introducing unsaturation into the alkyl chain. For AA, at very large area per molecule, floating domains of crystalline nature exist rather than any classical gaseous phase. The measured conformational disorder in EA decreases continuously with monolayer compression and no crystalline domains are observed at low density. Addition of NaCl to the subphase does not affect the monolayer order for either of the compounds; instead, a dramatic increase in the signal of the water hydrating the headgroups is observed. The effect of introducing further unsaturations (up to three) was also studied in order to probe the resulting interfacial structure. Remarkably the double bonds appear to adopt the same orientation, irrespective of how many they are in the chain. By monitoring the vinyl CH stretch it was possible to study the film stability towards oxidative degradation and it was found that all three unsaturated species studied showed rapid degradation. The rate of degradation could be controlled by adjusting the film pressure. However, the monolayers could be stabilised by performing the experiments in an inert nitrogen atmosphere. / QC20100629

VSFS

SFG

interface

crown ethers

ethylene oxides

ionic liquids

fatty acids

domains.

Surface and colloid chemistry

Yt- och kolloidkemi

Neonatal Developmental Neurotoxicity of Brominated Flame Retardants, the Polybrominated Diphenyl Ethers (PBDEs)

Viberg, Henrik

January 2004

This thesis examines developmental neurotoxic effects of polybrominated diphenyl ethers (PBDEs), PBDE 99, PBDE 153, and the fully brominated PBDE 209, after exposure during the newborn period in rodents. Our environment contains vast numbers of contaminants, including the flame retardants, PBDEs. The PBDEs are widely found in the environment and are increasing in human milk. Individuals can be exposed to PBDEs during their whole lifetime, and especially during the lactation period. The neonatal period, coinciding with the lactation period, is characterized in many mammalian species by rapid growth and development of the immature brain. It has been shown that numerous toxicants can induce permanent disorders in brain function when administered to the neonatal mouse during the brain growth spurt (BGS). In mice and rats this period is postnatal, spanning over the first 3-4 weeks of life, while in humans, BGS begins during the third trimester of pregnancy and continues throughout the first two years of life. The present studies identified a defined critical period during BGS in mice when the brain is vulnerable to insults of low doses of PBDEs and that it is the presence of PBDEs or their metabolites in the brain during this critical period that is crucial to evoking neurotoxic effects. The effects observed are permanent altered spontaneous behavior, reduced habituation, deficits in learning and memory, and disturbances in the cholinergic system. These effects worsen with age. The ability of PBDEs to induce neurotoxic effects does not appear to be gender-, strain- or species-specific, because the neurotoxic effects are induced in rats and male and female mice of different strains. The developmental neurotoxic effects of PBDEs are similar to those observed for polychlorinated biphenyls (PCBs) and possible interactive effects of PBDEs and other environmental contaminants are therefore of concern.

Biology

brominated flame retardants

polybrominated diphenyl ethers

PBDE

neonatal

development

neurotoxicity

behaviour

cholinergic system

Biologi

Biology

Biologi

Enantioselective Synthesis Of Bio-Active Bicyclic Acetals, Cyclic Ethers And Lactones

Anbarasan, P

07 1900

The thesis entitled “Enantioselective synthesis of bio-active bicyclic acetals, cyclic ethers and lactones” demonstrates the utility of chiral pool tartaric acid as the source in the synthesis of natural products. The results are discussed in three chapters; 1) Enantioselective synthesis of bio-active bicyclic acetals, 2) Enantioselective synthesis of bio-active cyclic ethers and 3) Enantioselective synthesis of bio-active lactones. A brief introduction is provided in each chapter to keep the present work in proper perspective. Compounds (in bold) and references (in superscripts) are sequentially numbered differently for each chapter and references are given as foot notes. Experimental procedures are given differently for each chapter and placed at the end of chapter. Scanned 1H and 13C NMR spectras are given with description of signals. Chapter 1 describes the enantioselective synthesis of bicyclic acetal containing insect pheromones. First part of this chapter deals with the enantiodivergent synthesis of both enantiomers of hydroxy-exo-brevicomin and 2-hydroxy-exo-brevicomin starting from a single chiral compound, bis-Weinreb amide derived from L-(+)-tartaric acid. Controlled addition of Grignard reagent to bis-Weinreb amide followed by diastereoselective reduction of the resultant ketone was employed as the key step for the enantiodivergent synthesis of hydroxy-exo-brevicomin and 2-hydroxy-exo-brevicomin. In the second part, enantioselective synthesis of exo-brevicomin, iso-exo-brevicomin and formal synthesis of frontalin comprising similar framework is demonstrated, utilizing á -benzyloxy aldehydes derived from L-(+)-tartaric acid as chiral building block. Second Chapter describes the enantioselective synthesis of bio-active cyclic ethers, disparlure, centrolobine and isolaurepan. Employing á-benzyloxy aldehydes derived from L-(+)-tartaric acid as the chiral building block, synthesis of both enantiomers of insect pheromone disparlure is achieved involving the diastereoselective addition of allyltributyl tin to the á-benzyloxy aldehyde and cross metathesis of the resultant homoallylic alcohol with 4-methyl-1-pentene. Formal synthesis of centrolobine and isolaurepan are accomplished. Pivotal step involved in the synthesis of centrolobine is iron(III) mediated cyclization of 1,5-diol derived from L-(+)-tartaric acid, while Lewis acid mediated reductive cyclization of the hydroxy ketone derived from á-benzyloxy aldehyde is the key step in the synthesis of isolaurepan. Third chapter in the thesis deals with the enantioselective synthesis of bio-active lactones muricatacin, 6-acetoxy-5-hexadecanolide and boronolide. Utilizing á-benzyloxy aldehyde as the building block, synthesis of five and six membered lactones, muricatacin and 6-acetoxy-5-hexadecanolide were accomplished via the diastereoselective addition of 3-butenylmagnesium bromide and allyltributyl tin to á-benzyloxy aldehyde, respectively. Stereoselective formal synthesis of boronolide was described, starting from D-(–)-tartaric acid. Key reaction sequence includes the elaboration of ã-hydroxy amide obtained by a combination of controlled Grignard addition and diastereoselective reduction from bis- Weinreb amide derived from D-(–)-tartaric acid.

Organic Synthesis

Ethers

Lactones

Bio-Active Bicyclic Acetals

Natural Products - Synthesis

Enantioselective Synthesis

Enantiospecific Synthesis

Organic Chemistry