Alterações morfológicas na área pré-óptica medial, núcleo periventricular anteroventral e amígdala medial póstero-dorsal induzidas pela manipulação neonatal

A manipulação neonatal imprime alterações no desenvolvimento neuroendócrino, morfológico e comportamental de ratos. A área pré-óptica medial (MPOA) contém neurônios produtores do hormônio liberador do hormônio luteinizante (LHRH) que estão intimamente relacionados com a reprodução. Os núcleos periventricular anteroventral (AVPV) e a amígdala medial póstero-dorsal (MePD) são áreas do sistema nervoso central (SNC) que apresentam receptores de estrógeno, portanto poderiam estar atuando no feedback das gonadotrofinas. O objetivo deste trabalho foi verificar os efeitos da manipulação neonatal sobre o volume do núcleo, a densidade de células, o diâmetro do corpo celular de neurônios e o número total estimado de neurônios da MePD e AVPV dos lados direito e esquerdo, em ratas aos 11 e 90 dias de idade. Na MPOA, foram avaliadas a densidade de células e o diâmetro do corpo celular de neurônios. A MPOA apresentou uma redução da densidade numérica de 50% em ratas manipuladas de 11 dias e 50% em ratas manipuladas aos 90 dias de idade. A manipulação neonatal provocou alterações nos parâmetros analisados nas três áreas estudadas, quando comparadas aos grupos não manipulados. Na MePD a redução foi 63% e de 47% respectivamente aos 11 e aos 90 dias de idade. No AVPV a redução foi de 44% e de 54% aos 11 e 90 dias de idade. As dimensões lineares do soma dos neurônios da MePD e MPOA apresentaram uma redução de tal forma que o diâmetro dos neurônios no grupo manipulado foi significativamente menor do que o grupo não manipulado. Mas as dimensões lineares dos neurônios do AVPV não apresentaram alterações significativas. A manipulação neonatal por uma causa ainda desconhecida induz a alterações estáveis na MPOA, MePD e AVPV. A diminuição do número de neurônios nessas estruturas pode explicar a redução da atividade do eixo hipotálamo-hipófise-gonadal (HPG) em ratas adultas, manipuladas no período neonatal.

Efeitos da manipulação neonatal sobre a concentração plasmática de hormônios da reprodução e a densidade de receptores de angiotensina II no sistema nervoso central de ratas adultas

A manipulação neonatal é um modelo experimental utilizado para avaliar o modo pelo qual interferências precoces na vida do animal podem alterar funções neuroendócrinas e comportamentos na vida adulta. O procedimento de manipulação neonatal, além de alterar a atividade do eixo hipotálamo-hipófise-adrenal (eixo HPA) em ratos machos e fêmeas, pode causar profundas mudanças na função reprodutiva de ratas adultas. De fato, há evidências de que a manipulação neonatal diminui a atividade do eixo HPA através da redução da síntese e secreção de hormônios que são liberados quando os animais são expostos ao estresse na vida adulta e, além disso, induz à presença de ciclos anovulatórios e diminui a receptividade sexual de ratas. Considerando essas alterações induzidas pela manipulação neonatal que são relacionadas à função reprodutiva de ratas, essa tese teve por objetivo estudar as possíveis causas da alteração no comportamento sexual e ovulação induzidas pela manipulação neonatal. Para isto, além de estudar o perfil hormonal desses animais, o que incluiu os esteróides gonadais, as gonadotrofinas e a prolactina (PRL) em diferentes fases e horários do ciclo estral, o conteúdo do hormônio liberador de gonadotrofinas (LHRH) em algumas regiões do sistema nervoso central (SNC) e na eminência mediana (EM); foi avaliada a possível participação do sistema angiotensinérgico central, através da análise da densidade dos receptores de angiotensina II (Ang II) pela técnica de auto-radiografia, na mediação dos efeitos da manipulação neonatal sobre a função do eixo hipotálamo-hipófise-gônada (eixo HPG) e do eixo HPA. O presente estudo confirmou dados obtidos em nosso laboratório sobre a redução do comportamento sexual e da ovulação em ratas manipuladas no período neonatal. Na tarde do proestro, período no qual ocorrem os eventos necessários para a ovulação na próxima fase do ciclo estral, os resultados mostram que os animais do grupo manipulado têm redução significativa da concentração plasmática de estradiol, de gonadotrofinas e de PRL, assim como um aumento no conteúdo de LHRH na área pré-óptica medial (APOM). A manipulação neonatal também reduziu a concentração plasmática de progesterona analisada após o coito que pode ser decorrente da reduzida estimulação vaginocervical recebida por essas ratas, já que houve uma redução significativa da freqüência de intromissão realizada pelo macho sobre as ratas do grupo manipulado. A densidade de receptores de Ang II na APOM e no núcleo paraventricular do hipotálamo (PVN) também foi alterada pela manipulação neonatal, pois houve redução significativa na densidade desses receptores nessas duas regiões. Em conclusão, a manipulação neonatal reduz profundamente a atividade do eixo HPG e essa alteração é causada por modificações nas concentrações de estradiol no plasma que, por sua vez, pode alterar a secreção de LHRH, de gonadotrofinas e de PRL, comprometendo dessa maneira a ovulação e a receptividade sexual. Contribuindo para os efeitos deletérios da manipulação neonatal sobre a função reprodutiva em ratas, este procedimento pode alterar a implantação do blastocisto devido à redução da secreção de progesterona observada após o coito no grupo manipulado. Alguns dos efeitos da manipulação neonatal parecem ser mediados pelo sistema angiotensinérgico central, como o aumento do conteúdo de LHRH na APOM e a diminuída resposta do eixo HPA observada em animais manipulados submetidos a situações estressantes na vida adulta.

Comparative study of the ultrastructure and secretory dynamic of hypopharyngeal glands in queens, workers and males of Sceptotrigona postica latreille (Hymenoptera, Apinae, Meliponini)

The secretory cycle of hypopharyngeal glands (HPGs) in Scaptotrigona postica resembles that of Apis mellifera: in newly emerged workers the HPGs are in prefunctional state, their maximum development happens in the nurse workers and in forager workers they show signs of reabsorption. In S. postica these glands are also present in queens and males where they are more developed in newly emerged individuals. The ultrastructural features of the HPG secretory cycle in workers of S. postica and A. mellifera are alike: granular endoplasmic reticulum well developed, large secretion masses around the intracellular canaliculus in nurse workers and extensive degenerative structures in forager workers. Then it is suggested that the HPG secrete similar substances in both species. A second secretory cycle seems to occur in early foragers, may be with production of enzymes. The role of the HPGs in queens and males remains unknown but one possibility is enzyme production.

LH Response (in vivo and in vitro) to an LHRH Agonist Administered to Domestic Male Cats

We investigated plasma luteinizing hormone (LH) concentration in domestic male cats challenged with Luteinizing Hormone Releasing Hormone Analog (LHRH-A) [des Gly10, (DTrp6)-LHRH ethylamide] that mediates the function of the hypothalamic-piruitary-gonadal axis (HPG). Plasma LH concentrations in cats treated daily with LHRH (10 μg/ 100 μl/kg/day, subcutaneously - sc) for 19 days (LHRH group) and in controls treated with saline (NaCl - 0.9%, same volume - SAL group) were chronically studied. LHRH administration (sc) for 15 days induced a significant fall (P < 0.05) in plasma LH concentrations during the chronic study. After the 15th day of treatment the groups were divided once more into animals treated with LHRH (10 μg/100 μl/kg) or saline (iv), and a time course study (300 min) was performed (acute study). Next, four groups of cats were compared in an acute study involving the sc/iv administration of SAL/SAL, SAL/LHRH, LHRH/SAL, and LHRH/LHRH. The responses of the SAL animals challenged by acute iv administration of LHRH (group SAL/LHRH) were significantly higher (P < 0.01) than those of animals treated with LHRH (sc) (group LHRH/LHRH). LH release was also significantly increased in the latter group (P < 0.05), although the effect was short lasting, being recorded only at the first observation (45 min). An in vitro study with the pituitaries was also performed on day 20. Mean (±SEM) LH concentrations in the culture medium containing pituitaries with LHRH (10-7 M) or saline were determined. In vitro analysis of these pituitaries demonstrated a significantly reduced response (P < 0.05) by animals treated sc with LHRH for 19 days. This study represents a source of data for the domestic cat going beyond its own physiology. Serving as a model, this animal provide important information for the study of reproductive physiology in other members of its family (Felidae), almost all of them threatened with extinction.

Resistência de união á dentina do canal radicular de cimentos endodônticos, em função da medicação intracanal com hidróxido de cálcio

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)

Photoperiod modulation of aggressive behavior is independent of androgens in a tropical cichlid fish

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)

Maternal separation on the ethanol-preferring adult rat liver structure

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

Comportamento materno e câncer de bexiga urinária: implicações da modulação de eixos hormonais e receptores de esteroides na fisiopatologia de lesões neoplásicas

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)

Facile double-functionalization of designed ankyrin repeat proteins using click and thiol chemistries

Click chemistry is a powerful technology for the functionalization of therapeutic proteins with effector moieties, because of its potential for bio-orthogonal, regio-selective, and high-yielding conjugation under mild conditions. Designed Ankyrin Repeat Proteins (DARPins), a novel class of highly stable binding proteins, are particularly well suited for the introduction of clickable methionine surrogates such as azidohomoalanine (Aha) or homopropargylglycine (Hpg), since the DARPin scaffold can be made methionine-free by an M34L mutation in the N-cap which fully maintains the biophysical properties of the protein. A single N-terminal azidohomoalanine, replacing the initiator Met, is incorporated in high yield, and allows preparation of "clickable" DARPins at about 30 mg per liter E. coli culture, fully retaining stability, specificity, and affinity. For a second modification, we introduced a cysteine at the C-terminus. Such DARPins could be conveniently site-specifically linked to two moieties, polyethylene glycol (PEG) to the N-terminus and the fluorophore Alexa488 to the C-terminus. We present a DARPin selected against the epithelial cell adhesion molecule (EpCAM) with excellent properties for tumor targeting as an example. We used these doubly modified molecules to measure binding kinetics on tumor cells and found that PEGylation has no effect on dissociation rate, but slightly decreases the association rate and the maximal number of cell-bound DARPins, fully consistent with our previous model of PEG action obtained in vitro. Our data demonstrate the benefit of click chemistry for site-specific modification of binding proteins like DARPins to conveniently add several functional moieties simultaneously for various biomedical applications.

Ar-40/Ar-39 Evidence for Middle Proterozoic (1300-1500 Ma) Slow Cooling of the Southern Black Hills, South Dakota, Midcontinent, North America: Implications for Early Proterozoic P-T Evolution and Posttectonic Magmatism

Ar-40/Ar-39 total gas and plateau dates from muscovite and biotite in the southern Black Hills, South Dakota, provide evidence for a period of Middle Proterozoic slow cooling. Early Proterozoic (1600-1650 Ma) mica dates were obtained from metasedimentary rocks located in a synformal structure between the Harney Peak and Bear Mountain domes and also south of Bear Mountain. Metamorphic rocks from the dome areas and undeformed samples of the similar to 1710 Ma Harney Peak Granite (HPG) yield Middle Proterozoic mica dates (similar to 1270-1500 Ma). Two samples collected between the synform and Bear Mountain dome yield intermediate total gas mica dates of similar to 1550 Ma. We suggest two end-member interpretations to explain the map pattern of cooling ages: (1) subhorizontal slow cooling of an area which exhibits variation in mica Ar retention intervals or (2) mild folding of a Middle Proterozoic (similar to 1500 Ma) similar to 300 degrees C isotherm. According to the second interpretation, the preservation of older dates between the domes may reflect reactivation of a preexisting synformal structure (and downwarping of relatively cold rocks) during a period of approximately east-west contraction and slow uplift during the Middle Proterozoic. The mica data, together with hornblende data from the Black Hills published elsewhere, indicate that the ambient country-rock temperature at the 3-4 kbar depth of emplacement of the HPG was between 350 degrees C and 500 degrees C, suggesting that the average upper crustal geothermal gradient was 25 degrees-40 degrees C/km prior to intrusion. The thermochronologic data suggest HPG emplacement was followed by a similar to 200 m.y. period of stability and tectonic quiescence with little uplift. We propose that crust thickened during the Early Proterozoic was uplifted and erosionally(?) thinned prior to similar to 1710 Ma and that the HPG magma was emplaced into isostatically stable crust of relatively normal thickness. We speculate that uplift and crustal thinning prior to HPG intrusion was the result of differential thinning of the subcrustal lithosphere beneath the Black Hills. If so, this process would have also caused an increase in mantle heat flux across the Moho and triggered vapor-absent melting of biotite to produce the HPG magma. This scenario for posttectonic granite generation is supported, in part, by the fact that in the whole of the Black Hills, the HPG is spatially associated with the deepest exposed Early Proterozoic country rock.

Molecular cloning and sequence analysis of the complestatin biosynthetic gene cluster

Streptomyces lavendulae produces complestatin, a cyclic peptide natural product that antagonizes pharmacologically relevant protein–protein interactions including formation of the C4b,2b complex in the complement cascade and gp120-CD4 binding in the HIV life cycle. Complestatin, a member of the vancomycin group of natural products, consists of an α-ketoacyl hexapeptide backbone modified by oxidative phenolic couplings and halogenations. The entire complestatin biosynthetic and regulatory gene cluster spanning ca. 50 kb was cloned and sequenced. It consisted of 16 ORFs, encoding proteins homologous to nonribosomal peptide synthetases, cytochrome P450-related oxidases, ferredoxins, nonheme halogenases, four enzymes involved in 4-hydroxyphenylglycine (Hpg) biosynthesis, transcriptional regulators, and ABC transporters. The nonribosomal peptide synthetase consisted of a priming module, six extending modules, and a terminal thioesterase; their arrangement and domain content was entirely consistent with functions required for the biosynthesis of a heptapeptide or α-ketoacyl hexapeptide backbone. Two oxidase genes were proposed to be responsible for the construction of the unique aryl-ether-aryl-aryl linkage on the linear heptapeptide intermediate. Hpg, 3,5-dichloro-Hpg, and 3,5-dichloro-hydroxybenzoylformate are unusual building blocks that repesent five of the seven requisite monomers in the complestatin peptide. Heterologous expression and biochemical analysis of 4-hydroxyphenylglycine transaminon confirmed its role as an aminotransferase responsible for formation of all three precursors. The close similarity but functional divergence between complestatin and chloroeremomycin biosynthetic genes also presents a unique opportunity for the construction of hybrid vancomycin-type antibiotics.

The whole-cell immobilization of D-hydantoinase-engineered Escherichia coli for D-CpHPG biosynthesis

Background: D-Hydroxyphenylglycine is considered to be an important chiral molecular building-block of antibiotic reagents such as pesticides, and β-lactam antibiotics. The process of its production is catalyzed by D-hydantoinase and D-carbamoylase in a two-step enzyme reaction. How to enhance the catalytic potential of the two enzymes is valuable for industrial application. In this investigation, an Escherichia coli strain genetically engineered with D-hydantoinase was immobilized by calcium alginate with certain adjuncts to evaluate the optimal condition for the biosynthesis of D-carbamoyl-p-hydroxyphenylglycine (D-CpHPG), the compound further be converted to D-hydroxyphenylglycine (D-HPG) by carbamoylase. Result: The optimal medium to produce D-CpHPG by whole-cell immobilization was a modified Luria-Bertani (LB) added with 3.0% (W/V) alginate, 1.5% (W/V) diatomite, 0.05% (W/V) CaCl2 and 1.00 mM MnCl2. The optimized diameter of immobilized beads for the whole-cell biosynthesis here was 2.60 mm. The maximized production rates of D-CpHPG were up to 76%, and the immobilized beads could be reused for 12 batches. Conclusions: This investigation not only provides an effective procedure for biological production of D-CpHPG, but gives an insight into the whole-cell immobilization technology. © 2016 Pontificia Universidad Católica de Valparaíso. Production and hosting by Elsevier B.V. All rights reserved.