Cristais de ácido glutâmico: crescimento, caracterização e cálculos ab initio / Crystals of glutamic acid: growth, characterization and calculations ab initio.

Pinheiro, José Auri

January 2006

PINHEIRO, José Auri. Cristais de ácido glutâmico: crescimento, caracterização e cálculos ab initio. 2006. 114 f. : Tese (Doutorado em Bioquímica) - Universidade Federal do Ceará, Centro de Ciências, Fortaleza-CE, 2006. / Submitted by Eric Santiago (erichhcl@gmail.com) on 2016-07-20T14:46:59Z No. of bitstreams: 1 2006_tese_japinheiro.pdf: 1742642 bytes, checksum: ea49b7e21bdd91f790bdc04ac6f5f777 (MD5) / Approved for entry into archive by José Jairo Viana de Sousa (jairo@ufc.br) on 2016-08-02T20:36:49Z (GMT) No. of bitstreams: 1 2006_tese_japinheiro.pdf: 1742642 bytes, checksum: ea49b7e21bdd91f790bdc04ac6f5f777 (MD5) / Made available in DSpace on 2016-08-02T20:36:49Z (GMT). No. of bitstreams: 1 2006_tese_japinheiro.pdf: 1742642 bytes, checksum: ea49b7e21bdd91f790bdc04ac6f5f777 (MD5) Previous issue date: 2006 / Done the work accomplish in this thesis it seeks the crystallization of the glutamic acid, favoring the obtaining of the phase α (metastable) in relation to the polymorph β. After the obtaining of the crystals they did take place the experimental measures of fluorescence, with views the comparison with the obtained theoretical data, considering the limitations of the method of simulation used ab-initio. Were the calculations of first principles accomplished to study the properties of the crystal of the glutamic acid in the modifications α and β in what she refers to the aspect structural, electronic (structure of bands) and optical (function of the dieletric complex), everything this in relation to the polymorphism conformational. The theory of the functional of the density (TFD) is it considered using a base of plane waves, pseudo potential ultrasoft, and the correlation-change potential inside of the Generalized-Gradient Approximation (GGA). Are the net parameters in agreement with the experimental results, although in the form α is it foreseen to have an indirect gap between the points of high symmetry and X, equal to 4.69 eV, for the form β a conclusion cannot be reached on the direct gap (-), due to imprecision of the calculation. The function dieletric of both polymorph are very similar in the case of a sample polycrystal, but it differs strongly in the case of the polarization of the light of the faces of the crystal 100 and 010 / O trabalho realizado nesta tese visa a cristalização do ácido glutâmico, favorecendo a obtenção da fase α (metaestável) em relação ao polimorfo β. Após a obtenção dos cristais realizaram-se as medidas experimentais de fluorescência, com vistas a comparação com os dados teóricos obtidos, considerando as limitações do método de simulação ab-initio utilizado. Os cálculos de primeiros princípios foram realizados para estudar as propriedades do cristal do ácido glutâmico nas modificações α e β no que se refere ao aspecto estrutural, eletrônico (estrutura de bandas) e óptico (função do complexo dielétrico), tudo isto em relação ao polimorfismo conformacional. A teoria do funcional da densidade (TFD) é considerada usando uma base de ondas planas, pseudopotenciais ultramacios, e o potencial de correlação-troca dentro do Generalized-Gradient Approximation (GGA). Os parâmetros de rede estão de acordo com os resultados experimentais, embora na forma α é previsto ter um gap indireto entre os pontos de alta simetria  e X, igual a 4.69 eV, para a forma β não pode-se tirar uma conclusão sobre o gap direto (-), devido a imprecisão do cálculo. A função dielétrica de ambos os polimorfos são muito semelhantes no caso de uma amostra policristalina, mas difere fortemente no caso da polarização da luz das faces do cristal 100 e 010.

Bioquimica

Glutamic acid, ab nitio, cristalization

Cristalização

Estudo da sinalização glutamatérgica, estresse oxidativo e morte celular em cérebros de ratos durante o envelhecimento

Ureshino, Rodrigo Portes [UNIFESP]

25 June 2008

Made available in DSpace on 2015-07-22T20:50:06Z (GMT). No. of bitstreams: 0 Previous issue date: 2008-06-25. Added 1 bitstream(s) on 2015-08-11T03:25:52Z : No. of bitstreams: 1 Publico-10947.pdf: 1984469 bytes, checksum: 2cce63c3d607e63adb499e8742f10eed (MD5) / O envelhecimento é um processo multi-fatorial associado a déficits funcionais, sendo que o cérebro é um dos órgãos com maior susceptibilidade a doenças crônico-degenerativas. Dentre essas, as doenças de Alzheimer e de Parkinson apresentam maior prevalência na população global e levam à incapacitação severa do indivíduo. Assim, o entendimento dos mecanismos dessas doenças que estão relacionados com o envelhecimento é importante para a busca de alternativas de tratamento. Há evidências de que, em doenças neurodegenerativas, ocorrem alterações na homeostase do cálcio (Ca2+), o que pode contribuir para a morte celular por apoptose. No presente trabalho, buscamos investigar fenômenos envolvidos com a tríade Ca2+ -mitocondria- EROs (espécies reativas do oxigênio) (TOESCU, 2005) e a apoptose em corpo estriado de ratos no envelhecimento. Foram avaliadas a sinalização intracelular dinâmica (em tempo real) e estática (biologia molecular), a morfologia celular e ultraestrutural, a morfometria e bioenergética. Utilizando fatias cerebrais de ratos, observamos que os anmais senescentes apresentaram um aumento de Ca2+ citosólico maior que os animais jovens, após a estimulação glutamatérgica. Em seguida, utilizamos antagonistas parciais das duas classes de receptores, os metabotrópicos do grupo I e os ionotrópicos (NMDAR), para estudar os componentes desse aumento de Ca2+. Avaliamos também o aumento de Ca2+ citosólico mediado por agentes que mobilizam esse íon do retículo endoplasmático e da mitocôndria, mostrando que esses estoques de Ca2+ podem estar aumentados no envelhecimento. As medidas do ∆ψm basal mostraram que hei urna diminuição deste parâmetro no envelhecimento, sendo estas alterações condizentes com a inibição mais acentuada do complexo I da cadeia transportadora de elétrons e do aumento na produção de EROs. As alterações funcionais não implicaram em mudanças ultraestruturais da mitocôndria. Foram investigados a expressão gênica e o conteúdo proteíco de Bax e Bcl-2, mostrando um aumento da expressão de bax e uma redução de proteínas Bcl-2, o que pode ter uma relação com o aumento de apoptose encontrado no estriado dos animais senescentes. Desse modo, os resultados indicam que, no envelhecimento, existem alterações no controle intracelular de sinalização de Ca2+ e na bioenergética, que podem contribuir para o aumento de apoptose. / TEDE / BV UNIFESP: Teses e dissertações

Ácido glutâmico

Apoptose

Cálcio

Corpo estriado

Espécies de oxigênio reativas

Envelhecimento

Glutamic Acid

Apoptosis

Calcium

Corpus Striatum

Reactive Oxygen Species

Aging

Estudo do comportamento térmico de alguns aditivos alimentares por TG/DTG, DTA e DSC / Thermal behavior studies of some food additives by TG/STG, STA and DSC

Ronaldo Spezia Nunes

13 April 2009

Estudos termoanalíticos de alguns aditivos alimentares da classe dos realçadores de sabor foram desenvolvidos visando avaliar sua estabilidade e resistência durante o preparo de alimentos a quente assim como investigar os eventuais intermediários de decomposição que poderiam resultar destes processos. Os sais foram obtidos de fontes industriais ou sintetizados e submetidos à caracterização por análise elementar, espectrometria vibracional na região do infra-vermelho, termogravimetria/termogravimetria derivada, análise térmica diferencial e em alguns casos, calorimetria exploratória diferencial. Foram estudados o ácido glutâmico e seus sais de amônio, lítio e sódio mono e dissubstituídos. Em todos os casos observou-se uma conversão a piroglutamato após desidratação dos sais monossubstituídos, a qual ocorre via a a-carboxila. A estabilidade térmica destes sais foi da ordem de 190-200 °C. No caso dos sais dissubstituídos de lítio e sódio não houve conversão ao piroglutamato pois as duas carboxilas estão salificadas. Os glutamatos de magnésio, cálcio estrôncio e bário, também foram preparados e investigados quanto ao seu comportamento térmico. Os sais se formaram na estequiometria 2:1 (ligante:metal), apresentando águas de hidratação em número característico e foram estáveis até 190- 200 °C. Finalmente foram estudados os mecanismos de decomposição térmica do inosinato-monofosfato de sódio e do guanilato-monofosfato de sódio, dois nucleotídeos que apresentam a propriedade de realçar o sabor de alimentos. Ambos apresentaram elevado grau de hidratação, para o qual foi possível distinguir mecanismos característicos de desidratação. A decomposição dos sais anidros ocorreu com saída do grupo purínico, seguida da decomposição do restante da molécula e formação de pirofosfato de sódio como resíduo final. / Thermal analytical studies of some food addictives of the flavor enhancer class were developed in order to evaluate their stability and resistance to the hot cooking process, as well as to identify the intermediaries of thermal decomposition that could remain at the end of such processes. The salts were obtained from industrial sources or synthesized and characterized by elemental analysis, infra-red spectroscopy, thermogravimetry/derivative thermogravimetry, differential thermal analysis and in some opportunities to differential scanning calorimetry. The glutamic acid and its ammonium, lithium and sodium salts mono and disubstituted were investigated. In all cases a conversion to pyroglutamate has been observed in the free acid and its monosubstituted salts after dehydration. The conversion undergoes by the ?-carboxyl group. The thermal stability was observed to be as high as 190-200 °C. In the case of the lithiu m and sodium dissubstituted salts any conversions to pyroglutamates were observed, once both carboxyl groups were salified. Magnesium, calcium, strontium and barium glutamates has also been synthesized and investigated in relation to its thermal behavior. The salts were formed in the 2:1 stoichiometry (ligand:metal), presenting hydration waters in a characteristic content and showed to be stable up to 190-200 °C. Finally the thermal decomposition mechanisms of dissodium inosinatemonophosphate and dissodium guanilate-monophosphate two nucleotides with flavor enhancement properties in food were also investigated. Both presented high degree of hydration, to which it was possible to propose a water release mechanism. The decomposition of the anhydrous salts occurred with release of the purine group followed by the decomposition of the rest of the molecule generating sodium pyrophosphate as residue.

ácido glutâmico

análise térmica

glutamatos alcalino e alcalino-terrosos

guanilato

inosinato

alkalines and alkalines earth glutamates

glutamic acid

guanylate

inosinate

thermal analysis

Adsorção de aminoácidos em hidróxidos duplos lamelares: efeito da temperatura, pH e força iônica do meio / Adsorption of amino acids in layered double hydroxides: temperature, pH and ionic strength effects

Fabiano Silvério

28 January 2005

Hidróxidos Duplos Lamelares (HDLs), são materiais lamelares constituídos de camadas positivamente carregadas de um hidróxido misto de dois metais (um di e um trivalente), com ânions hidratados no domínio interlamelar. Apesar de serem potenciais adsorventes, o estudo da adsorção de aminoácidos sobre estes sólidos ainda não foi realizado. Este é importante, pois abre caminho para a aplicação de HDLs na remoção e recuperação de aminoácidos de soluções aquosas, provenientes de processos industriais. Este trabalho teve por objetivo estudar a adsorção e a sorção dos aminoácidos: Ácido Aspártico (Asp), Ácido Glutâmico (Glu) e Fenilalanina (Phe), a partir de soluções aquosas, em HDLs do sistema [Mg-Al-CO3], verificando o efeito de variáveis como temperatura, pH e força iônica (FI) do meio. O adsorvente foi preparado pelo método de coprecipitação a pH variável e caracterizado quanto à composição, organização estrutural, textura e morfologia. A adsorção de Asp, Glu e Phe no HDL não calcinado indicaram que não ocorre a substituição do ânion interlamelar (CO32-), mas sim a adsorção por interação do aminoácido com as cargas residuais na superfície do HDL. O processo mostrou uma grande dependência das variáveis estudadas. A adsorção de Asp e Glu tem comportamento semelhante, embora o aumento da força iônica, seja mais pronunciado em pH 7 para o Asp, e em pH 10 para o Glu. Sem aumento da força iônica, as isotermas atingem ou se aproximam do patamar de adsorção destes aminoácidos, e o aumento na temperatura diminui a quantidade máxima adsorvida. A adsorção de Phe apresentou comportamento similar aos anteriores, exceto pelo fato do aumento da força iônica causar uma diminuição na adsorção. Os resultados obtidos para a sorção no HDL calcinado mostraram que inicialmente o HDL é reconstituído contendo ânions OH- intercalados que são deslocados pelo aminoácido conforme a concentração deste aumenta. Neste caso, Asp e Glu também apresentaram comportamentos semelhantes: as isotermas atingem um patamar onde a sorção torna-se constante e o aumento da temperatura diminui a quantidade sorvida. Para a Phe, a quantidade sorvida é muito maior que para os demais e não se observa o patamar de sorção constante. A temperatura não causa alteração significativa na quantidade sorvida. Os resultados de remoção dos aminoácidos, obtidos para o HDL calcinado se mostraram mais eficientes do que àqueles observados no HDL não calcinado. / Layered Double Hydroxides (LDHs), are lamellar materials constituted of positively charged layers of two cations mixed hydroxide (a bi and a trivalent one), with hydrated anions in the interlayer domain. In spite of they being potential adsorbents, the study of the adsorption of amino acids on these solids has not been done yet. This is important, because it opens the perspective for the application of LDHs to remove and to recover amino acids from aqueous solutions, resultant from industrial processes. The aim of this work was to study the adsorption and the sorption of the amino acids: Aspartic Acid (Asp), Glutamic Acid (Glu) and Phenylalanine (Phe), from aqueous solutions, in [Mg-Al-CO3] LDHs, verifying the effect of the variables: temperature, pH and ionic strength of the medium. The adsorbent was prepared by the coprecipitation method and characterized with respect to their composition, structural organization, texture and morphology. The adsorption of Asp, Glu and Phe in LDH indicated that the substitution of the interlayer anion (CO32-) doesn\'t occur, but the adsorption process occurs by the interaction of the amino acid with the residual charges on the LDH surface. The process showed a dependence on the parameters studied. The adsorption of Asp and Glu presented similar behavior, although the ionic strength effect is more pronounced in pH 7 for Asp, and in pH 10 for Glu. Without the increase in ionic strength, the isotherms reach or approach a plateau, and the increasing in the temperature reduces the maximum amount adsorbed. The adsorption of Phe has similar behavior to the previous ones, except at higher ionic strength, in which a decrease in the adsorption was observed. The results for the sorption in calcined LDH showed that the LDH are reconstituted with the OH- anions intercalated at low amino acid concentrations. The intercalation of amino acid becomes important as their concentration increase. In this case, Asp and Glu also presented similar behaviors: the isotherms reach a plateau where the sorption becomes constant and the increase of the temperature reduces the amount of sorbed amino acid. For Phe, the amount sorbed is higher than those for the others amino acids and the plateau of constant sorption was not observed. The temperature doesn\'t cause any significant alteration in the sorbed amount. The results of removing the amino acids on calcined LDH showed to be more efficient than those observed for the adsorption in LDH.

Ácido Aspártico

Ácido Glutâmico

Adsorção

Fenilalanina

Hidróxidos Duplos Lamelares

Sorção

Adsorption

Aspartic Acid

Glutamic Acid

Layered Double Hidroxides

Phenylalanine

Sorption

Dubious Role Of Mycobacterium Paratuberculosis In Pathogenesis Of Type I Diabetes

Thanigachalam, Saisathya

01 January 2012

Background: Type 1 Diabetes mellitus (TIDM) is a chronic disorder in which the insulin producing beta cells are selectively self-destroyed. Although the etiology of the disease has not been determined, genetic dispositions such as SLC11A1 polymorphism in suffering patients have been reported. The role of pathogenic microorganisms such as Mycobacterium avium subspecies paratuberculosis (MAP) in TIDM has also been recently debated. MAP is already known to cause paratuberculosis in cattle and now it is a strong suspect of causing autoimmune diseases in humans such as Crohn’s disease, multiple sclerosis, autoimmune Thyroiditis, rheumatoid arthritis and autoimmune diabetes. We hypothesis that molecular mimicry between MAP Heat shock protein 65K (Hsp65) and human Glutamic Acid Decarboxylase 65K (GAD65) can be the trigger which leads to the autoimmune destruction of beta cell in patients exposed to MAP . Method: To test the hypothesis, peptide sequences of MAP Hsp65 and human GAD65 were investigated using BLAST and PyMOL bioinformatics tools. Moreover, 18 blood samples from humans with TIDM and controls, and 100 sera samples from cattle with paratuberculosis and controls were evaluated for the presence of MAP, MAP DNA and its antibodies. Glucose, insulin and GAD65 antibodies were also determined in some of the clinical samples. Results: Peptide BLAST analysis revealed 44% identity between the two proteins with 75% positive identities in a 16 amino acid region. PyMOL structural analysis identified possible shared epitope regions of the proteins in its 3D conformation. Immunoblot analysis revealed a strong cross reactivity between lysate of E.coli recombinant of MAP Hsp65 and plasma from human subject with TIDM. A weak cross reactivity was also observed between healthy rat pancreatic homogenate and rabbit anti MAP IgG. Nested PCR using IS900-specific iv oligonucleotide primers did not detect MAP DNA in peripheral blood from 18 subjects with Type I Diabetes, Type II Diabetes and non-diabetic controls. Long term culture of leukocytes from blood samples from same subjects resulted in the presence of MAP in 3/10 (30%) TIDM and 4/8 (50%) control subjects. However anti MAP IgG were detected in 5/10 (50 %) TIDM samples compared to 3/8 (37.5 %) controls. Insulin level was measured in sera from paratuberculosis cattle and controls. In MAP infected cattle, insulin level ranged from below 0.1ng/ml to 2.456 ng/ml with an average of 0.36 +/- 0.57ng/ml compared to below 0.1ng/ml to 13.47ng/ml with an average of 2.86 +/- 3.00ng/ml in healthy cattle. Conclusion: Bioinformatics analysis between MAP Hsp65 and human GAD65 through BLAST and PyMOL analysis revealed a homology of 16 amino acid motif and possible shared epitope regions; immunohistochemistry analysis revealed a cross reactivity between rabbit antiMAP IgG and pancreatic cell homogenate from a healthy rat. Moreover, plasma from patient with TIDM (TD8), who was confirmed to be positive for MAP DNA and MAP IgG, reacted strongly with MAP Hsp65 in MAP protein lysate and MAP Hsp65 recombinant clone pmptb20. Culture of MAP from human leukocytes is significant despite the lack of correlation between MAP in samples from TIDM and controls. It is worth noting that some of the control subjects have not been evaluated for other autoimmune diseases possible MAP role. Additionally, antiMAP IgG levels in TIDM subjects compared to controls have raised a suspicion on the involvement of MAP in TIDM. The poor correlation of MAP in blood versus either the antiMAP IgG or the insulin level may be related with the fastidious nature of MAP and in vitro cultivation. Since MAP is the sole causative agent of Johne’s disease, it is significant that the insulin level is 8 folds less in MAP infected cattle compared to MAP free cattle. Overall, the data v is mixed and suggest that further study is needed to investigate the intriguing question to whether MAP is involved in TIDM or not.

Type 1 diabetes

mycobacterium paratuberculosis

molecular mimicry

glutamic acid decarboxylase 65

heat shock protein 65

Molecular Biology

Synthesis and Characterization of Novel Polyethers and Polypeptides for Use in Biomedicine and Magnetic Resonance Imaging

Liang, Jue

24 January 2014

Copolymers that contain terminal or pendent functional groups have great potential in the biomedical area due to their biocompatibility and tunable properties.1-3 In this research, two vinyl functional epoxides, vinyldimethylsilylpropyl glycidyl ether (VSiGE) and ethoxy vinyl glycidyl ether (EVGE), were synthesized. These heterobifunctional monomers were polymerizable via the epoxide groups and can be functionalized via thiol-ene reactions through the pendent vinyl groups. A series of amphiphilic block copolyethers based on poly(ethylene oxide) and poly(1,2-butylene oxide) that incorporate VSiGE or EVGE were synthesized and characterized. The vinyl ether and vinyl silane functional groups were functionalized after polymerization and the functional polymers formed pH-sensitive micelles in aqueous medium. The copolyethers were loaded with ritonavir yielding well-controlled nanoparticles. Poly(L-glutamic acid) is comprised of naturally occurring L-glutamic acid repeating units that are linked together with amide bonds. In this research, we have prepared magnetic block ionomer complexes based on poly(ethylene oxide)-b-poly(L-glutamic acid) copolymers. This is of interest due to the biocompatibility and biodegradable nature of the poly(L-glutamic acid) component of the backbone. Allyl- and thiol-functional poly(ethylene oxide)-b-poly(L-glutamic acid) copolymers were also synthesized and coated onto the surface of iron oxide nanoparticles. Allyl- and thiol-tipped single particles were reacted with each other to prepare magnetic clusters. Transverse relaxivities of the clusters were found to be significantly higher than that of single particles. One major problem in commercial development of therapeutic proteins is their poor transport across cellular membranes and biological barriers such as the blood-brain barrier (BBB). One solution to this problem is to modify proteins with amphiphilic block copolymers such as PEO-b-PPO-b-PEO, Pluronics®. However, it isn't possible to independently tune the two PEO block lengths with commercial Pluronics® since a difunctional PPO macroinitator is utilized to grow both PEO blocks simultaneously (HO-EOn-b-POm-b-EOn-OH). Another challenge is introducing functional group which allows post-polymerization functionalization for specific applications. In this study, a series of heterobifunctional asymmetric amino-EOn1-b-POm-b-EOn2-OH block copolymers (APs) with different molecular weights of each block were synthesized and the amino terminal group was conjugated to an antioxidant enzyme, Cu/Zn superoxide dismutase (SOD1). The conjugates were characterized and their cellular uptake was investigated. / Ph. D.

functional polyethers

poly(glutamic acid)

iron oxide

poly(ethylene oxide)

poly(propylene oxide)

heterobifunctional polyethers

superoxide dismutase

Synthèse d'agents chélateurs bi-fonctionnels pour le marquage de peptides avec le [indice supérieur 64]Cu / Development and evaluation of bifunctional chelating agents for peptide labeling with [superscript 64]Cu

Denis, Céline

January 2015

Résumé : Grâce à des caractéristiques physiques particulières, le [indice supérieur 64]Cu (T[indice inférieur 1/2]= 12.7 h; β[indice supérieur+], 0.65 MeV [17.8 %]; β[indice supérieur −], 0.58 MeV [38.4 %]) est un candidat idéal pour l’imagerie TEP et la radiothérapie ciblée du cancer. Son utilisation est actuellement limitée par la disponibilité de chélateurs bi-fonctionnels (CBFs) offrant une résistance élevée aux réactions de transmétallation in vivo. Récemment nous avons développés deux nouveaux CBFs cycliques, DOTHA[indice inférieur 2] et NOTHA[indice inférieur 2], portant des ligands hydroxamates pour la complexation au [indice supérieur 64]Cu. Ces CBFs possèdent une cinétique de marquage rapide dans des conditions très douces, une stabilité élevée in vivo et un profil de biodistribution favorable avec une clairance rapide. Nous proposons maintenant d’étendre notre approche à la préparation de CBFs acycliques plus flexibles et compacts afin de moduler les propriétés biologiques et la pharmacocinétique des traceurs peptidiques. Le but de mon projet de maîtrise est de développer une série de chélateurs acycliques dérivés de l'histidine et de l'acide glutamique et fonctionalisés avec des groupements hydroxamates pour identifier un CBF offrant un complexe stable in vivo avec le [indice supérieur 64]Cu(II). Les CBFs ont été préparés en solution pour faciliter l’optimisation de chaque étape réactionnelle. Les groupements chélatants hydroxamates ont été sélectionnés pour leur habilité à former des complexes stables avec différents métaux et ils ont été liés en position N-terminale et sur la chaîne latérale des acides aminés grâce à des réactions de substitution nucléophile. Les groupements para-methoxy-benzyles ont été judicieusement sélectionnés pour la protection des groupements hydroxamates afin de faciliter, au besoin, une déprotection sélective sous des conditions très douces. L’optimisation du marquage a été effectuée avec l’isotope stable du cuivre et ensuite avec le [indice supérieur 64]Cu en faisant varier le contre ion métallique, le pH, la concentration, et la température. Le CBF offrant la plus grande stabilité, soit celui dérivé de l’histidine, a été conjugué à un peptide, le H[indice inférieur 2]N-PEG-[D-Tyr[indice supérieur 6],βAla[indice supérieur 11],Thi[indice supérieur 13],Nle[indice supérieur 14]]bombesin(6-14) (BBN), se liant fortement aux récepteurs de la relâche de la gastrine surexprimés dans les cancers du sein et de la prostate. La stabilité et l’activité spécifique du CBF-histidine et du radiotraceur marqués au [indice supérieur 64]Cu s’est avérée faible in vitro. Il est connu que l’activité antibactérienne de ligands hydroxamates est associée à leur capacité à complexer le fer. En perspective, comme nos chélateurs complexent très fortement le Fe(III), une alternative pour ces composés serait d’évaluer leur capacité à inhiber la croissance et la prolifération des bactéries. || Abstract : Thanks to its particular physical characteristics, [superscript 64]Cu (T[subscript ½= 12.7 h; β[superscript +], 0.65MeV [17.8 %]; β[superscript −], 0.58MeV [38.4 %]) is an ideal candidate for PET imaging and targeted cancer radiotherapy. Currently, its use is limited by the availability of bi-functional chelators (BFCs) which give high resistance to in vivo transmetallation reactions. Recently, we developed two new cyclic BFCs, DOTHA[subscript 2] and NOTHA[subscript 2], bearing hydroxamate pendant arms for the complexation with [superscript 64]Cu. Those BFCs have fast labeling kinetics under very mild conditions, a high in vivo stability and a biodistribution profile which is favorable with a fast clearance. Now, we propose to expand our approach to the preparation of acyclic BFCs, which are more flexible and compact, in order to better modulate biological properties and the pharmacokinetics of the peptidic tracers. The goal of my Master’s degree project is to develop a series of acyclic chelators derived from histidine and glutamic acid and functionalized with hydroxamate pendant arms to identify a BFC that shows highly stable in vivo complexes with [superscript 64]Cu(II). BFCs have been prepared in solution to facilitate the optimization of each reactive step. Hydroxamate chelating groups have been selected for their ability to form stable complexes with different metals and they have been conjugated in N-terminal position and on the lateral chain of amino acids via nucleophilic substitution reactions. Para-methoxy-benzyl groups have been judiciously selected for the protection of the hydroxamate groups to facilitate, if needed, a selective deprotection under mild conditions. The labeling optimization has been performed with a stable copper isotope, and then with [superscript 64]Cu varying the metallic counter-ion, pH, concentration and temperature. The BFC having the highest stability, the one derived from histidine, was conjugated to a peptide, H[subscript 2]N-PEG-[D-Tyr[superscript 6],βAla[superscript 11],Thi[superscript 13],Nle[superscript 14]]bombesin(6-14) (BBN), strongly bounding the gastrin releasing peptide receptor, which is overexpressed in breast and prostate cancers. Both the stability and specific activity of BFC-histidine of the radiotracer labeled with [superscript 64]Cu were low in vitro. It is known that the antibacterial activity of hydroxamate ligands is associated with their ability to complex iron. In perspective, because our hydroxamate ligands strongly complex Fe(III), an alternative for these compounds would be to assess their ability to inhibit the growth and proliferation of bacteria.

Chélateur bi-fonctionnel

[indice supérieur 64]Cu

Ligand hydroxamate

Histidine

Acide glutamique

Bifunctional chelator

[superscript 64]Cu

Hydroxamate pendant arm

Glutamic acid

Nanoparticules multifonctionnelles de PBLG destinées au ciblage et à la délivrance d’anticancéreux aux tissus osseux / Multifunctional PBLG nanoparticles for bone targeting and anticancer drug delivery into bone tissues

Miguel Martínez de Aragón, Laura de

01 October 2013

Des nanoparticules multifonctionnelles polymères, préparées par auto-assemblage de plusieurs dérivés du poly (L-glutamate de gamma-benzyle) (PBLG), ont été conçues afin d’assurer le ciblage des tissus osseux et la libération contrôlée de molécules actives. Des propriétés d'attachement aux tissus osseux leur ont été conférées par la présentation en surface de différents ligands ostéotropes, l'alendronate et l' acide poly(glutamique), seuls ou en combinaison. Leur affinité pour les tissus osseux a été évaluée in vivo ainsi que leur distribution fine dans ces tissus. Par ailleurs, des propriétés anticancéreux ont été conférées aux nanoparticules grâce à un mécanisme originale d’association du cisplatin par complexation. Le procédé mis en œuvre permet d’obtenir des cinétiques de libération très progressives de dérivés actifs du platine et déclenchée par la présence des ions chlorure. Enfin, leur cytotoxicité a été mesurée. Cette stratégie constitue donc une approche prometteuse en vue d’améliorer le traitement des métastases osseuses. / Multifunctional bone targeted polymeric nanoparticles prepared by self-assembly of several poly(gamma-benzyl-L-glutamate) (PBLG) derivates have been developed. Their bone binding properties were provided by two different osteotropic moieties, alendronate or/and poly(glutamic acid) exposed on the nanoparticle surface. Their affinity for bone tissues has been evaluated in vitro, ex vivo and in vivo, including their detailed distribution in bone tissues structures. Further, in view of bone cancer therapeutics, nanoparticles were provided with anticancer properties thanks to the complexation of cisplatin, which leaded to very well controlled release properties. Finally, cytotoxicity were studied. Therefore, this strategy constitute a promising approach for the improvement of bone cancer therapeutics.

Nanoparticules

Ciblage de l'os

Délivrance du principe actif

Poly(glutamate de benzyle)

Alendronate

Poly(acide glutamique)

Cisplatine

Nanoparticles

Bone targeting

Drug delivery

Poly(benzylglutamate)

Alendronate

Poly(glutamic acid)

Cisplatin

Hydroxyapatite

Potencialização de inibidores da recaptura de serotonina com N-acetilcisteína no tratamento do transtorno obsessivo-compulsivo resistente: estudo duplo-cego e controlado / Serotonin reuptake inhibitor augmentation with N-acetylcysteine in treatment-resistant obsessive-compulsive disorder: a double blind and controlled trial

Costa, Daniel Lucas da Conceição

28 September 2016

INTRODUÇÃO: O transtorno obsessivo-compulsivo (TOC) apresenta prevalência ao longo da vida ao redor de 2%. O tratamento farmacológico de primeira linha para o TOC é feito com inibidores da recaptura de serotonina (IRS). Aproximadamente metade dos pacientes tratados adequadamente com um IRS não apresenta resposta satisfatória. Resultados de estudos de neuroimagem, genéticos e de análise do líquido cefalorraquidiano de portadores de TOC sugerem o envolvimento da disfunção da atividade glutamatérgica na fisiopatologia do TOC. Medicamentos com efeito modulador da atividade glutamatérgica vem sendo testados em pacientes com TOC e alguns deles mostraram-se eficazes. A N-Acetilcisteína (NAC) é um agente modulador da atividade glutamatérgica e antioxidante. Este estudo tem como objetivo principal testar a eficácia da potencialização de IRS com NAC, em comparação com placebo, em pacientes com TOC resistente ao tratamento. MÉTODOS: Estudo duplo cego, randomizado e controlado com placebo, com duração de 16 semanas, conduzido num ambulatório especializado de um hospital terciário (maio/2012 - outubro/2014). Critérios de inclusão: 18-65 anos; diagnóstico principal de TOC, de acordo com os critérios do DSM-IV; falha terapêutica a pelo menos um tratamento farmacológico adequado para o TOC; escore inicial da escala Yale-Brown de Sintomas Obsessivo-Compulsivos (Y-BOCS) >= 16 ou >= 10, se apenas compulsões; e gravidade inicial do TOC pelo menos moderada, de acordo com a escala de gravidade da Impressão Clínica Global. Os medicamentos em uso no momento da randomização foram mantidos nas mesmas doses. A intervenção consistiu na associação de NAC (até 3000 mg/dia) ou placebo. Avaliações cegas foram realizadas antes e ao final da intervenção. Utilizamos como desfecho primário os escores da Y-BOCS. Utilizamos análise de variância não-paramétrica para medidas repetidas. Como desfechos secundários, consideramos a redução dos escores iniciais dos Inventários de Depressão e Ansiedade de Beck, da Y-BOCS Dimensional e da Escala Brown de Avaliação de Crenças. Registro do estudo: clinicaltrials.gov identifier: NCT01555970. RESULTADOS: Foram realizadas 145 consultas de triagem, 129 indivíduos preencheram os critérios de inclusão, 40 foram randomizados (NAC até 3000 mg/dia, n= 18; placebo, n= 22), 39 iniciaram a intervenção e 35 terminaram o estudo. Não houve diferença significativa entre os grupos quanto à taxa de perda (NAC: 1 em 17 [5,9%]; placebo: 3 em 22 [13,6%]; ?2 = 0,63; P= 0,43). Todos os indivíduos melhoraram significativamente ao longo do tempo, de acordo com a redução do escore da Y-BOCS, mas não houve diferenças significativas entre os grupos (NAC: 25,6 [DP= 4,4] para 21,3 [DP= 8,1]; placebo: 24,8 [DP= 3,8] para 21,8 [DP= 6,0]; F= 0,33; P= 0,92). A associação com NAC foi superior ao placebo em relação à melhora da gravidade dos sintomas ansiosos, indicada pela redução do escore do Inventário de Ansiedade de Beck (média [DP]: NAC= 7,8 [11,7]; placebo: -0,55 [7,9]; U= 89; P= 0,02). Não houve diferenças significativas entre os grupos quanto à melhora dos sintomas depressivos, das diferentes dimensões de sintomas de TOC e do nível de insight. CONCLUSÕES: A potencialização de IRS com NAC foi superior ao placebo em relação à melhora da gravidade dos sintomas ansiosos. Entretanto, não houve diferença entre os grupos na melhora da gravidade dos sintomas do TOC / INTRODUCTION: Obsessive-compulsive disorder (OCD) is a debilitating psychiatric disorder with a lifetime prevalence of 2-3%. Treatment guidelines recommend serotonin reuptake inhibitors (SRIs) as the first-line pharmacological treatment for OCD. However, approximately half of patients treated with an adequate trial of SRIs fail to fully respond to treatment. OCD is associated with hyperactivity in cortical-striatum-thalamus-cortical (CSTC) circuits. Cortico-striatal and thalamo-striatal afferents use the excitatory neurotransmitter glutamate, and there is evidence suggesting abnormal glutamate levels and/or homeostasis in OCD patients. Researchers have been testing glutamate-modulating medications in OCD, with some evidence for efficacy. N-Acetylcysteine (NAC), a glutamate-modulating agent, is being considered as an add-on strategy for treatment-resistant OCD. The main objective of this study was to determine if NAC is effective in treatment-resistant OCD patients after 16 weeks of SRI augmentation. METHODS: We conducted a randomized, double blind, placebo-controlled, 16-week trial in an OCD-specialized outpatient clinic at a tertiary hospital (May 2012-October 2014). Inclusion criteria: age between 18-65 years; DSM-IV primary diagnosis of OCD; failure to respond to at least one previous adequate pharmacological treatment for OCD; baseline Yale-Brown Obsessive-Compulsive Scale (Y-BOCS) global score >= 16 or >= 10 if only compulsions are present; OCD symptoms of at least moderate severity on the Clinical Global Impression-Severity subscale. Medications in use at randomization were maintained at the same dose. Assessments were conducted at baseline and end of the study. The primary outcome measure was the Y-BOCS scores. To evaluate the variables group, time, and interaction effects for Y-BOCS scores at all time points, we used nonparametric analysis of variance (ANOVA) with repeated measures. The secondary outcomes were the mean reduction of the baseline Beck Anxiety and Depression Inventories, Dimensional Yale-Brown Obsessive-Compulsive Scale and Brown Assessment of Beliefs Scale scores. Trial registration: clinicaltrials.gov identifier NCT01555970. RESULTS: We assessed 145 patients for eligibility, 129 were eligible, 40 were randomized (NAC up to 3000 mg/day, n= 18; placebo, n= 22), 39 initiated the intervention and 35 completed the trial. Dropout did not significantly differ by treatment group (NAC: 1 of 17 [5.9%]; placebo: 3 of 22 [13.6%]; ?2 = .63; P= .43). Both groups significantly improved over the 16 weeks, as indicated by the reduction of baseline Y-BOCS scores, but there were no significant differences between groups (NAC: 25.6 [SD= 4.4] to 21.3 [DP= 8.1]; placebo: 24.8 [SD= 3.8] to 21.8 [SD= 6.0]; F= .33; P = .92). Adding NAC to SRI was superior to placebo in improving anxiety symptoms, as measured by the reduction of baseline Beck Anxiety Inventory score (mean [SD]: NAC= 7.8 [11.7]; placebo: -.55 [7.9]; U= 89; P= .02). There were no significant differences between groups in regards to the improvement of depressive symptoms, different dimensions of OCD symptoms and insight level. CONCLUSIONS: NAC augmentation of SRI was more effective than placebo in reducing the severity of anxiety symptoms in this sample of treatment-resistant OCD individuals. However, it was not better than placebo in reducing OCD severity

Acetilcisteína

Acetylcysteine

Ácido glutâmico

Clinical trial

Ensaio clínico

Excitatory amino acid agents

Glutamic acid

Obsessive-compulsive disorder

Terapêutica

Therapeutics

Transtorno obsessivo-compulsivo

Directed Self-Assembly of Gold Nanorods Using Surface Modification

Walker, David A

10 July 2008

Metallic nanoparticles are unique materials for optical, electronic, catalytic, and sensing applications. Due to the vast flexibility in controlling the surface chemistry of these particles through functionalization there is a great deal of interest in using metallic nanoparticles as building blocks in the development of more complex nanostructures through the use of a 'bottom-up' approach. Using self assembly techniques, one can exploit spontaneous chemical interactions to build complex constructs on the nanometer scale. Towards this end, gold nanorods have been synthesized and modified with various polymers, inorganic oxides and organic ligands to establish principles for self-assembly of these unique nanomaterials. Gold nanorods are of great interest due to their strong optical absorption in the visible and near infrared regions, which can be tuned through material preparation and modification of the surrounding environment. This thesis focuses on investigating approaches for both irreversible and reversible self-assembly of gold nanorods. Techniques such as dynamic light scattering (DLS), ultraviolet-visible (UV) spectroscopy, transmission electron microscopy (TEM), and polarization modulation infrared reflection absorbance spectroscopy (PM-IRRAS) were used to characterize the colloidal particles and gold surfaces. A novel contribution of this work is the successful demonstration of end-to-end linking of gold nanorods in a rapid and reversible manner using a pH responsive polypeptide.

poly(L-glutamic acid)

resorcinarene

monolayers

composite particles

linear assembly

end-to-end assembly

reversible assembly

nanotechnology

sensors

metallic nanoparticles

American Studies

Arts and Humanities