Global ETD Search

1	Coupling of the HPA and HPG Axes Dismukes, Andrew 20 December 2013 (has links) The Hypothalamic-Pituitary-Adrenal (HPA) and –Gonadal (HPG) axes have been considered mutually inhibitory; however, emerging evidence supports the proposition that this might not necessarily be the case. This idea is termed “coupling,” in which the HPA-HPG axis are mutually activated or deactivated. Coupling is examined across three data sets with different time-courses of stress exposure, and results demonstrate HPA-HPG co-activation occurs. Furthermore, stress exposure influences this relationship. The discussion shows how it is physiologically possible to have positive coupling or co-activation between these axes according to complex regulatory feedback systems and overlapping neural structures. Findings are interpreted developmentally, because adolescence may be a critical time for this co-activation to occur. Finally, the discussion emphasizes an individual difference perspective because each individual differs in the duration and type of stress they experience, and these exerted individualized effects on HPA-HPG coupling. Stress HPA HPG Coupling Cortisol Testosterone Biological Psychology
2	Atuação das proteínas do relógio na senescência reprodutiva de ratas Wistar / Clock protein action in the senescence reproductive of female Wistar rats Nicola, Angela Cristina de [UNESP] 12 December 2017 (has links) Submitted by ANGELA CRISTINA DE NICOLA null (angela_bio2006@yahoo.com.br) on 2018-02-07T18:16:28Z No. of bitstreams: 1 Tese Angela.pdf: 2735259 bytes, checksum: bcfc7217ff01dee64fa4ca1839e45c76 (MD5) / Approved for entry into archive by Ana Paula Rimoli de Oliveira null (anapaula@foa.unesp.br) on 2018-02-09T17:42:31Z (GMT) No. of bitstreams: 1 nicola_ml_dr_araca_int.pdf: 2735259 bytes, checksum: bcfc7217ff01dee64fa4ca1839e45c76 (MD5) / Made available in DSpace on 2018-02-09T17:42:31Z (GMT). No. of bitstreams: 1 nicola_ml_dr_araca_int.pdf: 2735259 bytes, checksum: bcfc7217ff01dee64fa4ca1839e45c76 (MD5) Previous issue date: 2017-12-12 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) / O envelhecimento é considerado processo multidimensional no qual fatores ambientais podem proteger ou, inversamente, agravar seus sinais, de maneira não linear, nos processos fisiológicos e neurocomportamentais. Durante este processo, os ritmos circadianos são interrompidos ou fragmentados com dissociação consequente dos ritmos circadianos do indivíduo e disfunções relacionadas ao relógio circadiano contribuem para o envelhecimento e para patologias a ele relacionadas. O objetivo deste estudo foi averiguar possível alteração temporal do sistema CLOCK no eixo HPG e a relação com às alterações hormonais que caracterizam a periestropausa. Foram utilizadas fêmeas adultas com ciclo estral regular (CD) na fase do diestro e fêmeas senis com ciclo estral irregular e persistência da fase do diestro (IDP). Para análises de expressão gênica dos clock genes Per2, Rev-erbα e Bmal1 no eixo HPG, foram utilizados punchs das regiões do NSQ, onde também foi analisado RNAm de AVP, APO e HMB destes animais, além da adenohipófise e ovários dos quais se extraiu o RNA para confecção do cDNA e realização de qPCR. A determinação da atividade neuronal vasopressinérgica no NSQ foi realizada por imunoistoquíca com dupla marcação para cFos e AVP em tecido previamente fixado com paraformaldeído. A concentração plasmática de gonadotrofinas foi determinada por radioimunoensaio. De modo geral, os animais IDP revelaram alterações no perfil de expressão gênica durante o fotoperíodo, com redução de amplitude, deslocamento/desalinhamento de fase e ausência de antifase. O NSQ de animais IDP apresentou menor expressão de Rev-erbα e maior expressão de RNAm para AVP em relação ao grupo CD. A quantificação relativa de Bmal1 foi semelhante em ambos os grupos e não houve diferenças entre grupos na expressão de Per2. Na APO, animais IDP apresentaram maior expressão de Per2 e menor quantidade de RNAm para Rev-erbα. No HMB observou-se menor expressão para Per2 e Rev-erbα e maior expressão de Bmal1 nas fêmeas IDP. Per2 e Bmal1 na adenohipófise tiveram menor expressão que o gene Rev-erbα no grupo senil e o ovário destes animais revelou maior expressão para Per2 e Rev-erbα, em comparação com os animais CD. As concentrações plasmáticas de FSH foram maiores nas fêmeas com ciclo irregular (2,05 ± 0,44 ng/mL), principalmente durante a fase clara, assim como o LH (0,24 ± 0,07 ng/mL), cujos maiores valores foram encontrados durante a fase escura e com perfil semelhante ao RNAm de AVP. As imunomarcações revelaram alta atividade vasopressinérgica na porção dorsomedial do NSQ das fêmeas IDP. Juntos estes dados permitem concluir que há desarranjo na expressão temporal dos genes Per2, Rev-erbα, Bmal1 que compõem a maquinaria molecular do relógio circadiano, bem como de RNAm para AVP no NSQ, de fêmeas Wistar na periestropausa. Além disso, a maior atividade neuronal vasopressinérgica e a ausência de oscilação de Rev-erbα e Bmal1 no NSQ destes animais, comprometem a correta comunicação do relógio central do NSQ com o eixo HPG, inviabilizando a manutenção da fertilidade feminina e contribuindo para a senescência reprodutiva. / Aging is considered a multidimensional process in which environmental factors can protect or, conversely, aggravate its signals, non-linearly, in physiological and neurobehavioral processes. During this process, circadian rhythms are disrupted or fragmented with consequent dissociation of the individual's circadian rhythms and circadian clock-related dysfunctions contribute to aging and related pathologies. The objective of this study was to investigate possible temporal alteration of the CLOCK system in the HPG axis and the relation with the hormonal changes that characterize periestropause. Adult females with regular estrus cycle in the diestrous phase (RD) and old females with irregular estrous cycle and persistent diestrous phase (IPD). For analyzes of the gene expression of the genes Per2, Rev-erbα and Bmal1 in the HPG axis, punchs from the NSQ regions were used, where AVP, POA and MBH RNAm from these animals were also analyzed, as well as the adenohypophysis and ovaries from which they were extracted the RNA for cDNA production and qPCR performance. The determination of the vasopressinergic neuronal activity in the NSQ was performed by immunohistochemical with double labeling for cFos/AVP in tissue previously fixed with paraformaldehyde. The plasma concentration of gonadotrophins was determined by radioimmunoassay. In general, the IPD animals show alterations in the gene expression profile during the period analyzed, with amplitude reduction, phase shift / misalignment and absence of antiphase. The NSQ of IPD animals presented lower expression of Rev-erbα and higher RNAm expression for AVP than RD group. The relative quantification of Bmal1 was similar in both groups and there were no differences between groups in the expression of Per2. In PAO, IPD animals showed higher expression of Per2 and less amount of RNAm for Rev-erbα. MBH showed lower expression for Per2 and Rev-erbα and higher Bmal1 expression in IPD females. Per2 and Bmal1 in the adenohypophysis had lower expression than the Rev-erbα gene in the old group and the ovary of these animals showed higher expression for Per2 and Rev-erbα, in related to to the RD animals. Plasma concentrations of FSH were higher in females with irregular cycle (2.05 ± 0.44 ng / mL), mainly during the light phase, as well as LH (0.24 ± 0.07 ng / mL) whose values were found during the dark phase and with a profile similar to AVP RNAm. Immunolabeling demonstrated high vasopressinergic activity in the dorsomedial portion of the NSQ of the IPD females. Together these data allow us to conclude that there is a breakdown in the temporal expression of the Per2, Rev-erbα, Bmal1 genes that make up the molecular machinery of the circadian clock, as well as RNAm for AVP in NSQ of Wistar females in peri-masterpause. In addition, the increased vasopressinergic neuronal activity and the absence of Rev-erbα and Bmal1 oscillation in the NSQ of these animals compromise the correct communication of the central clock of the NSQ with the HPG axis, making it impossible to maintain female fertility and contributing to reproductive senescence. Envelhecimento reprodutivo Clock genes Vasopressina Ritmo circadiano Eixo HPG Reproductive aging Clock genes Vasopressin Circadian rhythm HPG axis
3	Role of the orphan nuclear receptor steroidogenic factor 1 in mouse reproductive function Eilers Smith, Olivia 04 1900 (has links) Le récepteur nucléaire orphelin facteur stéroïdogénique 1 (SF-1 ou NR5A1) est un modulateur indispensable du développement surrénal et gonadique et qui joue un rôle dans la détermination du sexe, le développent hypothalamique, la fonction hypophysaire et la stéroïdogénèse. Toutefois, les études sur SF-1 dans le milieu de la biologie de la reproduction portent majoritairement sur des modèles embryonnaires ou de mammifères immatures. L’objectif principal de cette thèse était de déterminer le rôle de SF-1 dans les évènements clés de la fonction reproductrice chez les mâles et femelles matures. Ce facteur de transcription est exprimé dans différents organes, principalement ceux de l’axe hypothalamo-hypophyso-gonadique, et dans divers types cellulaires des gonades. Nous avons donc généré 4 modèles de souris knockout conditionnels (cKO) en utilisant les allèles Cre-recombinase et flox de SF-1 (SF-1f/f) afin d’identifier son rôle dans les différentes populations cellulaires des testicules et ovaires de souris matures. Dans la première étude, nous avons présenté une analyse des souris femelles du modèle cKO du récepteur de la progestérone (PRCre/+;Nr5a1f/f), où la suppression de SF-1 est spécifique aux cellules gonadotropes de l’hypophyse et aux cellules ovariennes de type granulosa suite au déclenchement du signal ovulatoire ainsi que les cellules lutéales du corps jaune. Cette étude a révélé de nouveaux rôles in vivo de SF-1 durant l’ovulation et la lutéinisation, tout en suggérant que SF-1 est un médiateur de la synthèse et sécrétion des gonadotrophines. Les femelles PRCre/+;Nr5a1f/f cKO étaient infertiles principalement en raison de l’importante réduction de FSH et LH sécrété dans la circulation, causé par le phénotype hypophysaire. Afin de contourner cette dysfonction hypophysaire, des traitements de gonadotrophines exogènes ainsi que des transplantations d’ovaires nous ont permis de démontrer que SF-1 régule la transcription de gènes impliqués dans l’expansion du cumulus ainsi que la rupture de follicules pour induire l’ovulation. De plus, nous avons montré que l’absence de SF-1 dans les ovaires de souris matures peut mener à l’infertilité, indépendamment du phénotype hypophysaire. D’autre part, nos trouvailles indiquent que, malgré la basse expression de SF-1 dans le corpus luteum chez la souris, sa déplétion dans les cellules lutéales conditionnée par recombinase Cre inhibe la production de progestérone. Aucun phénotype reproductif a été observé chez les souris PRCre/+;Nr5a1f/f cKO mâles. La deuxième étude a démontré le rôle essentiel de SF-1 dans la fonction du testicule mature. La souris mâle P450 17α-hydroxylase (Cyp17Cre/+;Nr5a1f/f) cKO, où la suppression de SF-1 est spécifique aux cellules de Leydig, était fertile malgré la taille réduite de ses testicules, la malformation de ses tubes séminifères, la perturbation de la spermiogénèse, ainsi que la réduction d’expression de gènes de la stéroïdogénèse. Bien que les mâles aromatase (Cyp19Cre/+;Nr5a1f/f) cKO, supprimant SF-1 dans les cellules de Sertoli, étaient fertiles et démontraient des capacités reproductives similaires aux mâles contrôle, les souris Cyp17Cre/++Cyp19Cre/+; Nr5a1f/f cKO (dKO) étaient soit infertiles ou montrait une fertilité affaiblie. La dysgénésie sévère du cordon testiculaire ainsi que la spermatogénèse perturbée chez la souris dKO étaient causées par la déplétion simultanée de SF-1 chez les cellules de Leydig et Sertoli, suggérant que les cellules de Sertoli peuvent compenser pour l’absence de SF-1 dans les cellules de Leydig et vice versa. Ces données démontrent que SF-1 est requis pour une stéroïdogénèse testiculaire et une spermatogénèse ainsi qu’une fertilité normale, bien que savoir si la régulation de ces fonctions par SF-1 est directe ou indirecte reste à élucider. De façon intéressante, les femelles des trois lignées cKO étudié dans ce deuxième article étaient fertiles et la sous expression de SF-1 dans les cellules ovariennes de type granulosa ou de la thèque a produit des effets mineurs sur leur fonction reproductive. En somme, la recherche présentée dans cette thèse contribue à l’avancement des connaissances sur SF-1 et son rôle dans la régulation d’événements reproductifs cruciaux dans l’hypophyse, l’ovaire et le testicule de souris matures. Les lignes de souris produites dans ce projet vont servir d’outil indispensable pour élucider les mécanismes de régulation de SF-1 sur la fonction gonadique and présenter de nouvelles avenues de recherches pour ce récepteur orphelin. / The orphan nuclear receptor steroidogenic factor-1 (SF-1 or NR5A1) is an indispensable modulator of adrenal and gonadal development, playing key roles in sex determination, hypothalamic development, pituitary function and steroidogenesis. Yet, studies to date of SF-1 in reproductive biology mostly focus on embryonic and immature mammalian models. The overall objective of this thesis was to determine the role of SF-1 in key events of mature male and female mouse reproductive function. This transcription factor is expressed in a variety of organs, mainly those of the hypothalamic-pituitary-gonadal axis, as well as in multiple cell types of the gonads. Therefore, we generated four conditional KO (cKO) mouse models employing Cre-recombinase and floxed alleles of SF-1 (SF-1f/f) to identify its role in different cell types of the testes and ovaries of mature mice. Our first study presents an analysis of female mice from the progesterone receptor (PRCre/+;Nr5a1f/f) cKO model, where SF-1 depletion is specific to gonadotropes in the pituitary gland as well as granulosa cells of the peri-ovulatory follicle and luteal cells of the corpus luteum. This research highlighted new in vivo roles for SF-1 in ovulation and luteinization, and provided further evidence that SF-1 is a mediator of gonadotropin synthesis and secretion. PRCre/+;Nr5a1f/f cKO females were infertile, due in large part to the reduced secretion of FSH and LH, caused by the pituitary phenotype. Exogenous gonadotropin treatments and ovarian transplantation experiments allowed us to circumvent the pituitary dysfunction to demonstrate that SF-1 in granulosa cells regulates the transcription of cumulus expansion and follicle rupture genes to induce ovulation. In addition, we showed that the absence of SF-1 in ovaries of mature mice can lead to female infertility, independent of the pituitary phenotype. Moreover, the data showed that, though SF-1 expression is reduced in mouse corpus luteum, its Cre-mediated depletion in luteal cells abrogates progesterone production. No reproductive phenotype was observed in PRCre/+;Nr5a1f/f cKO males. Results from our second study demonstrated that SF-1 plays an essential role in mature testicular function. The P450 17α-hydroxylase (Cyp17Cre/+;Nr5a1f/f) cKO male mouse, where the SF-1 depletion is specific to Leydig cells, were fertile, though showed reduced testis size with disrupted seminiferous tubules and impaired spermiogenesis, in addition to reduced expression of steroidogenic genes. While the aromatase (Cyp19Cre/+;Nr5a1f/f) cKO males were fertile and showed reproductive capacities comparable to control males, the Cyp17Cre/++Cyp19Cre/+; Nr5a1f/f cKO (dKO) model were either infertile or showed significantly impaired fertility. The dKO males displayed severe testis cord dysgenesis and impaired spermatogenesis caused by the depletion of SF-1 in both Leydig and Sertoli cells, suggesting that Sertoli cells can compensate for the absence of SF-1 in Leydig cells and vice versa. These data provide strong evidence that SF-1 is required for normal testicular steroidogenesis, spermatogenesis and male fertility, though whether the regulation of these functions is direct or indirect remains to be elucidated. Interestingly, the females of the three cKO mouse lines studied in this second article were fertile and the depletion of SF-1 in granulosa cells of antral follicles or in theca cells produced minor effects on their steroidogenic capacities. Collectively, the research presented in this thesis contributes to advance our understanding of the role of SF-1 in the regulation of essential reproductive events in the pituitary, ovary and testis of mature mouse gonads. The mouse lines generated for this project will serve as valuable tools to elucidate the mechanisms underlying SF-1 regulation of gonad function and present novel directions for the investigation of this nuclear receptor. SF-1 Axe HPG ovulation lutéinisation stéroïdogénèse spermatogenèse fertilité HPG axis luteinization steroidogenesis spermatogenesis fertility
4	Konstruktion av metod och verktyg för kontroll av snabbkopplingen Stäubli RBE03.1150/IA/HPG/JE Winberg, Erik January 2017 (has links) Detta examensarbete redogör för hur en metod samt ettverktyg utvecklats med ändamålet att kontrollera skicket på en kopplingshona(Stäubli RBE03.1150/IA/HPG/JE), vilken behandlar kvävgas. Arbetet hargenomförts på uppdrag av Saab AB. Det primära syftet var att ta fram enprovmetod för kontroll av kopplingen, det sekundära syftet att ta fram ettverktyg till denna metod. Det primära målet var att leverera instruktioner förprovmetod medan det sekundära målet var att leverera konstruktionsritningar förverktyget. Saab AB beställer dessa kopplingshonor av Stäubli International AG,för att sedan erbjuda kunden denna produkt i kombination med teknisk supportoch erhållet ansvar för att honan är funktionsduglig. Det har uppkommitproblematik med några kopplingspar där en del är RBE03.1150/IA/HPG/JE.Kopplingen separerar då den är under tryck vilket genererar en knall, detta ärej önskvärt och ett problem som ska utvärderas och åtgärdas. Arbetet hargenomförts i en agil projektform där en leveransplan följts samtidigt som detnärmsta arbetet har planerats systematiskt. Under förstudien har de trasigahonorna undersökts och tester genomförts, vilket har gett kunskap om vid vilkakrafter kopplingshonorna separerar. I förstudien kartlades även möjliga sättatt mäta när kopplingarna är slitna. Med den kunskapen har koncept samtprototyper skapats genom diverse produktutvecklingsmetoder, dessa harutvärderats och genererat det slutgiltiga resultatet, vilket varkonstruktionsritningar för ett verktyg och instruktioner för provmetod.Slutsatsen av detta är att målet med arbetet har uppfyllts. / <p>År och termin: 2017 VT</p><p>Datum för betyg: 2017-09-13</p> Stäubli koppling kopplingshona RBE03.1150/IA/HPG/JE Other Mechanical Engineering Annan maskinteknik
5	Premenstrual Dysphoric Disorder : A Review of Neural and Cognitive Changes in Women with PMDD Wiklund, Liselotte January 2017 (has links) Around 3-8% of all women in reproductive age suffer from premenstrual dysphoric disorder (PMDD) which disenables them to live an ordinary life during the luteal phase (premenstrual phase) of the menstrual cycle. Throughout the premenstrual phase these women experience emotional, cognitive and physiological changes. Hitherto, the etiology of this disorder is unknown. Some consider the source of this state as non-biological, claiming that PMDD is a social construction imbedded in gender roles, that suggests that women should not show aggressive behavior or depressive mood unless it is during the premenstrual stage. Contradictory, research made in cognitive neuroscience claim that the origin is biological. It is assumed that the increased symptoms in women with PMDD is a result from dysfunctional sensitivity for the progesterone metabolite allopregnanolone that has a receptor in the GABAA system, hence, producing an anxious effect from high levels of allopregnanolone instead of the expected sedative, soothing effects. Research suggest that structural and functional changes occur in brain areas such as the hippocampus, parahippocampus, amygdala, cerebellum as well as in brainderived neurotrophic factor which is important for brain plasticity, growth and survival of neurons. Cognitive behaviors such as anticipation for negative stimuli, working memory and lack of cognitive control also seem to be affected by PMDD. Nonetheless, the evidence is inconsistent, the area of research face multiple issues in regards to study designs, hence making generalization at this point difficult. In sum, this essay reviews recent studies conducted in neuroscience of cognitive changes in women with PMDD, with focus on functional, structural and behavioral changes between the phases of the cycle. PMDD menstrual cycle allopregnanolone estrogen progesterone HPG-axis cognition Neurosciences Neurovetenskaper
6	Influ?ncia de microg?is de hidroxipropilguar nas propriedades reol?gicas e de filtra??o de fluidos de perfura??o aquosos Silva, Rafael Ara?jo da 29 January 2015 (has links) Submitted by Automa??o e Estat?stica (sst@bczm.ufrn.br) on 2017-03-14T21:09:10Z No. of bitstreams: 1 RafaelAraujoDaSilva_DISSERT.pdf: 1302282 bytes, checksum: cb4d89880b246386e0981baae0eea668 (MD5) / Approved for entry into archive by Arlan Eloi Leite Silva (eloihistoriador@yahoo.com.br) on 2017-03-15T21:55:04Z (GMT) No. of bitstreams: 1 RafaelAraujoDaSilva_DISSERT.pdf: 1302282 bytes, checksum: cb4d89880b246386e0981baae0eea668 (MD5) / Made available in DSpace on 2017-03-15T21:55:04Z (GMT). No. of bitstreams: 1 RafaelAraujoDaSilva_DISSERT.pdf: 1302282 bytes, checksum: cb4d89880b246386e0981baae0eea668 (MD5) Previous issue date: 2015-01-29 / Os fluidos de perfura??o aquosos s?o os sistemas mais utilizados no mundo para a perfura??o de po?os petrol?feros, tendo sido, nas ?ltimas d?cadas, desenvolvidas excelentes formula??es para perfura??o de se??es iniciais com baixa temperatura e baixa press?o. No entanto, as reservas de petr?leo nessas condi??es est?o cada vez mais escassas, surgindo a necessidade operacional de atua??o em condi??es mais severas, ou seja, vem sendo relatada na literatura a necessidade de sistemas aquosos para atua??o em altas temperaturas e altas press?es (ATAP). As altas temperaturas dos po?os de petr?leo favorecem a degrada??o qu?mica dos pol?meros (aditivo comumente presente nas formula??es relatadas, atualmente, na literatura e aplicados em situa??es operacionais), podendo promover a redu??o da massa molar e perdas de viscosidade do sistema. Os microg?is podem ser aplicados em v?rios seguimentos da ind?stria, com destaque na ?rea do petr?leo, situa??o que s?o aplicados na estimula??o de po?os e na recupera??o avan?ada de petr?leo (EOR). Neste trabalho, a aplicabilidade de microg?is de hidroxipropilguar (HPG), obtidos por reticula??o do HPG com ?ons borato, foi avaliada quanto ? resist?ncia t?rmica em fluidos de perfura??o aquosos. A aplica??o de microg?is de HPG no fluido de perfura??o base ?gua aumentou a viscosidade aparente e reduziu o volume de filtrado na temperatura ? 25?C. Entretanto, com o aumento da temperatura para 50 ?C ocorreu redu??o da viscosidade aparente de 85 mPa.s para 25,45 mPa.s. Esses resultados indicam que o emprego de microg?is em fluidos de perfura??o aquosos pode ser uma alternativa promissora, desde que o agente reticulante seja adequadamente selecionado, ou seja, n?o sofra desativa??o com o aumento da temperatura e n?o seja influenciado pela salinidade do meio. / Aqueous drilling fluids are a widely used systemin the world to drill oil wells. This drilling system has been being developed excellent formulations for drilling initial sections with low temperature and low pressure in recent decades. However, the oil reserves in these conditions are increasingly scarce, ending up in the need for drilling fluids with better operational performance in the toughest conditions. Therefore, it has been reported in the literature the need for aqueous systems to operate at high temperatures and high pressures (HTHP). High temperatures of oil wells favor the chemical degradation of polymers (commonly reported in additive formulations currently in the literature and applied in operational situations), that can generate molecular weight reduction and viscosity losses. Microgels can be applied in vast industrie`s segments, highlighted in the oil field, as they are used in the estimulation of wells and in the Advanced Oil Recovery (EOR). In this work, the applicability of hydroxypropyl guar`s microgels (HPG), obtained by crosslinking the HPG with borate ions, was measured as the thermal stability in water based drilling fluids.The application HPG microgels in water-based drilling fluid has increased viscosity and the apparent volume of the filtrate reduced around 25 ? C. However, with the increase of temperature to 50 ?C, the viscosity of drilling fluids based on HPG microgels decreased from 85 mPa.s to 25,45 mPa.s. These results indicate that the use of microgels in aqueous drilling fluids is a promising alternative since the crosslinking agent has been properly selected, i.e., does not undergo deactivation with increasing temperature and is not affected by the salinity of the system. Fluido de perfura??o aquoso Hidroxipropilguar Microgel de HPG Controle de filtrado Propriedades reol?gicas
7	The Response of Marine Synechococcus to a Landscape of Environmental Stressors: A Proteomic Exploration Michels, Dana E 01 March 2021 (has links) (PDF) In the field of marine microbial ecology, many questions remain unanswered with regards to the physiological trade-offs made by phytoplankton to maximize growth (e.g., nutrient acquisition) and minimize loss (e.g., predation defenses). These tradeoffs, which occur at the cellular level, have wide reaching impacts on food web dynamics and global biogeochemical cycles. In the first chapter, we explored the use of a non-canonical amino acid (NCAA) technique, bioorthogonal non-canonical amino-acid tagging (BONCAT), in phytoplankton model systems. This technique has potential to work well in natural systems by enabling isolation of only newly synthesized proteins during an incubation period with the NCAA, reducing the complexity of natural proteomics and easing the elucidation of patterns. However, in testing BONCAT across several groups of cultured phytoplankton, we discovered that the NCAA molecule induced a stress response in the globally ubiquitous marine picocyanobacteria, Synechococcus sp. Therefore, in addition to confirming the uptake of modified amino acids by phytoplankton, chapter one investigated the implications of this stress response and limitations when using this technique to study marine microbial communities. In chapter two, we addressed our initial question by exploring tradeoffs at the protein level in a simplified culture system. This approach revealed insights into metabolic tradeoffs in response to predation pressure and nutrient stress. These insights into how phytoplankton negotiate these physiological tradeoffs at the protein level could ultimately allow for targeted proteomic studies in natural systems. Synechococcus Marine Proteomics BONCAT HPG Oxyrrhis marina Grazers Nutrient Limitation Marine Biology Microbial Physiology
8	The Production and Localization of Luteinizing Hormone in the Brain Courtney, Ya'el Carmel 29 May 2019 (has links) No description available. Neurobiology Neurosciences Biology Cellular Biology Bioinformatics luteinizing hormone hormone hormones HPG axis cognitive decline alzheimers AD neuroendocrinology endocrinology in-situ in situ hybridization single cell LH LHB
9	Fabrication and Characterisation of iontronic micropipette Hamrefors, Henrik January 2022 (has links) The biological translation between biological and electrical signals have inspired scientists over the last decade and has opened new way of therapeutics. The group of Bioelectronics at the Laboratory of organic electronics (LOE) develops systems that utilizes this translation to reduce the gap between electronics and biology. A known example of devices that does this are called iontronic delivery devices. These devices allow very specific transport and delivery of charged compounds. The most basic iontronic delivery device is the organic electronic ion pump (OEIP). The OEIP have been developed and fabricated into many variations, for example the iontronic micropipette which is a device that has been developed at LOE. In this project, the fabrication and characterization of the iontronic micropipette have been developed to find fabrication parameters that generates stable, high performing and reproduceable devices together with good and reproduceable characterization protocols. The iontronic micropipette is fabricated in a cleanroom and characterized in two steps, optically in a microscope and then electrically by transporting ions through the membrane. Two different membrane materials were tested, 2- acrylamido-2-methylpropane sulfonic acid (AMPSA) and Hyperbranched polyglycerols (HPG). The results that were obtained from the fabrication of the AMPSA showed a reproducibility between many devices, but many AMPSA device broke during the fabrication so the protocol for the AMPSA still need improvement. Regarding the A-HPG fabrication, the results were much more positive and the yield from the fabrication were sufficient. The results that were obtained in the characterization of the AMPSA device showed that these devices had a very equal resistance between the device from the same batch. For the A-HPG, it was a much larger spread in the resistance between the device but the resistance were still much lower than for the AMPSA which is more preferable for most applications on living cells. / <p>Examensarbetet är utfört vid Institutionen för teknik och naturvetenskap (ITN) vid Tekniska fakulteten, Linköpings universitet</p> Iontronic drug delivery Iontronic micropipette Ion exchange membrane AMPSA A-HPG Fabrication Characterisation Teknisk biologi Teknisk biologi Övrig annan teknik
10	Identification et caractérisation de nouveaux outils pharmacologiques sélectifs pour les différents récepteurs à peptides RF-amides / Identification and characterization of new selective pharmacological tools for the different RF-amides receptors Quillet, Raphaëlle 05 April 2018 (has links) Les RF-amides (RFRPs, NPFF, QRFP, PrRPs, Kisspeptines) sont une famille de peptides caractérisée par une signature Arg-Phe-NH2 à l’extrémité C-terminale très conservée au cours de l’évolution. Ils exercent leurs effets via 5 récepteurs couplés aux protéines G (NPFF1R, NPFF2R, QRFPR, PrRPR, Kiss1R), et plusieurs études soutiennent leur implication dans la modulation de nombreuses fonctions physiologiques telles que la douleur et la nociception, la reproduction, ou encore le métabolisme. Néanmoins, l’étude de ces systèmes est entravée par l’absence d’outils pharmacologiques tels que des antagonistes sélectifs. C’est pourquoi mon travail de thèse a consisté au développement d’outils pharmacologiques permettant de répondre à ces attentes, particulièrement sur les récepteurs NPFF1R, NPFF2R et Kiss1R. Des études de relation structure-activité nous ont amenés à considérer l’importance de la signature Arg-Phe-NH2 dans l’activité des peptides RF-amides sur leurs récepteurs. L’introduction de modifications au niveau N-terminal ou C-terminal du dipeptide Arg-Phe-NH2 nous a conduits à l’identification d’un antagoniste hautement affin et sélectif pour le récepteur NPFF1R in vitro et in vivo. Ce dernier nous a permis d’identifier le rôle du récepteur NPFF1R dans les effets secondaires liés à l’administration d’opiacés, tels que l’hyperalgésie et la tolérance morphinique. La responsabilité du récepteur NPFF1R dans ces phénomènes a été par la suite confirmée chez des souris KO NPFF1R. De plus, des données plus récentes suggèrent l’importance de ce dernier au niveau de l’axe hypothalamo-hypophyso-gonadotropique (HHG) des animaux saisonniers, et en particulier du hamster. Notre antagoniste nous a permis de déterminer le rôle du récepteur NPFF1R dans la libération de LH induite par le RFRP-3. Pour la première fois, nous avons également mis en évidence des molécules hautement affines et sélectives pour le récepteur NPFF2R, pour lequel nous avons révélé une activité agoniste partielle in vitro. Mon travail a également mené à la caractérisation in vitro d’un antagoniste sélectif du récepteur Kiss1R, qui vient compléter l’ensemble des outils disponibles pour l’étude des fonctions physiologiques modulées par ce récepteur et son ligand, la kisspeptine. Dans l’ensemble, mon travail de thèse a permis de caractériser plusieurs ligands affins et sélectifs des récepteurs à peptides RF-amides, et de mettre en lumière le rôle du système RFRP-3/NPFF1R dans les effets à long-terme liés aux opiacés. / RF-amides (RFRPs, NPFF, QRFP, PrRPs, Kisspeptins) belong to a family of peptide characterized by a Arg-Phe-NH2 C-terminus highly conserved throughout the evolution. They target 5 G-protein coupled receptors (NPFF1R, NPFF2R, QRFPR, PrRPR, Kiss1R) and most studies highlight their roles in the modulation of various functions as pain and nociception, reproduction or metabolism. Nonetheless, the study of these systems is severely limited by the absence of pharmacological tools as selective antagonists. Thus, my PhD project consisted in the development of selective ligands to answer these questions, notably on NPFF1R, NPFF2R and Kiss1R receptors. Structure-Activity relationship studies highlighted the importance of Arg-Phe-NH2 signature for the activity of RF-amide peptides on their receptors. Introduction of modifications at N or C-terminus of Arg-Phe-NH2 dipeptide led us to the identification of a compound displaying high affinity, selectivity and antagonist activity for NPFF1R both in vitro and in vivo. This compound allowed us to identify the critical role played by NPFF1R in the secondary effects related to opiates administration, as hyperalgesia and analgesic tolerance. The involvement of NPFF1R was then confirmed in KO NPFF1R mice. Moreover, recent data suggest the importance of NPFF1R on hypothalamo-pituitary gonadotropic (HPG) axis of seasonal animals, and particularly of hamsters. Our antagonist allowed us to decipher the role of NPFF1R in RFRP-3-induced-LH release. For the first time, we also have characterized high affinity and selective compounds for NPFF2R that display partial agonist activity in vitro. Moreover, our work led to the in vitro characterization of a selective antagonist for Kiss1R, that complete the available tools to study the physiological functions modulated by this receptor and its ligand, the kisspeptine. Overall, my PhD thesis led to the characterization of several selective ligands for RF-amide receptors, and highlight the role of RFRP-3/NPFF1R system in the long-term effects associated to opiates. Peptides RF-amides RFRP-3, NPFF, NPFF1R, NPFF2R, Kiss1R Nociception Hyperalgésie Antagoniste Axe HHG RF-amide peptides RFRP-3, NPFF, NPFF1R, NPFF2R, Kiss1R Nociception Hyperalgesia Antagonist HPG axis 615.7 616.8

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