Mapeamento genético e caracterização fenotípica do mutante anêmico induzido por Ethyl-nitroso-urea. / Genetic mapping and phenotypic characterization of an anemic mutant by ethylnitrosourea.

Carolina Cavalcante da Cruz

24 September 2009

A mutagênese química utilizando o agente mutagênico N-ethyl-N-nitrosourea (ENU) seguida da observação do fenótipo deu origem a um mutante Anêmico. O tipo de herança é autossômica dominante, com morte intra útero dos mutantes homozigotos. O mapeamento genético foi feito utilizando-se marcadores microssatélites, sendo selecionados marcadores polimórficos entre as linhagens BALB/c e C57BL/6 envolvidas no mapeamento. Estabeleceu-se um painel de microssatélites distribuídos por todo o genoma do camundongo, que permitisse a localização do cromossomo portador da mutação. O gene mutante foi localizado no cromossomo 7 entre os marcadores D7Mit301 e D7Mit131 delimitando um intervalo entre 46,5cM e 51cM de 4,5cM. Através das análises fenotípicas do mutante Anêmico e estudo dos genes candidatos neste intervalo, foi selecionado o gene Hbb responsável pela síntese das globinas b-major e b-minor , sendo o gene que mais se identifica com as características do mutante, localizado a 50cM. A deficiência deste gene leva a uma das mais severas anemias humana, a b-Talassemia major. / Chemical mutagenesis, using the mutagenic agent N-ethyl-N-nitrosourea (ENU), and followed by observation of the phenotype, originated in an Anaemic mutant. The inheritance-type is dominant auto-somic, with intra-uterus death of the homozygotic mutants. Genetic mapping was undertaken by means of micro-satellite markers, polymorphic markers being selected from among the BALB/c and C57BL/6 lineages involved in the mapping itself. A panel was established of the micro-satellites distributed throughout the whole mouse genome, thereby permitting localization of the mutation bearing chromosome. The mutant gene was located in chromosome 7 between markers D7Mit301 and D7Mit131, these delimiting an interval between 46,5cM and 51cM of 4,5cM. Selection of the Hbb gene responsible for synthesis of the b-major and b-minor globins came about through phenotypic analysis of the Anaemic mutant and a study of candidate genes within this interval, the selected gene being that which was most identified with the mutants characteristics and located at 50cM. A deficiency in this gene leads to one of the most severe forms of human anaemia, b-Talhassemia major.

Anemia hemolítica

Biotecnologia

Camundongos BALB/c

Fenótipos (características)

Mapeamento genético

Mutação genética induzida

Mutagênese

BALB/c mouse

Biotechnology

Genetic mapping

Hemolytic anemia

Induced gene mutation

Mutagenesis

Phenotype (characteristics)

Der Einfluss von Relaxin auf das Wachstum von Mammakarzinomen

Habla, Christiane

27 April 2010

Brustkrebs ist die häufigste Krebstodesursache bei Frauen in den Industrienationen mit einer jährlich ansteigenden Neuerkrankungsrate (Senn und Niederberger 2002). Durch vorangegangene Untersuchungen wurde bereits deutlich, dass das Peptidhormon Relaxin unter in vitro Bedingungen maßgeblich zur Tumorprogression von Mammakarzinomen beiträgt (Binder et al. 2002). Die vorliegende Arbeit hat untersucht, ob Relaxin diese Wirkung auch in vivo auf Mammakarzinome ausübt. Relaxin ist ein multifunktionales Hormon. Es ist ein Aktivator verschiedenerWachstumsund Transkriptionsfaktoren (Samuel et al. 2007a) und nimmt eine Schlüsselfunktion im Bindegewebsstoffwechsel ein, indem es durch eine Steigerung der MMP-Expression zur bindegewebigen Erweichung führt (Unemori et al. 1996). Im Krebsgeschehen schafft das Peptidhormon damit die Voraussetzungen für Tumorwachstum und Metastasierung (Bingle et al. 2002). Für die Fragestellung der vorliegenden Arbeit wurde das Brustkrebsmodell der BalbneuT- Maus eingesetzt, die aufgrund der transgenen HER2-Überexpression spontan Mammakarzinome entwickelt. Es wurden 45 weibliche Tiere mit beginnendem Wachstum von Mammatumoren auf eine Relaxin- (n=22) und eine Kontrollgruppe (n=23) aufgeteilt. Den Tieren wurde über eine unter das Nackenfell implantierte osmotische Minipumpe (Fa. Alzet, Modell 2004; Kupertura, Kanada) im Falle der Relaxin-Gruppe Relaxin und im Falle der Kontrollgruppe isotone Natriumchloridlösung verabreicht. Danach wurden die Tiere 10-49 Tage beobachtet und daraufhin eingeschläfert. Es wurden die Tumoren, Biopsien von Leber, Lunge und Nieren sowie Blutproben entnommen. Um beurteilen zu können, ob die Tumoren der Relaxin-behandelten Tiere ein schnelleres Wachstum zeigten, wurden Tumorvolumina und -gewichte zu den unterschiedlichen Tötungszeitpunkten erfasst. Weiterhin wurden im Tumorgewebe immunhistochemisch der Proliferationsmarker Ki67, der Makrophagenmarker MAC 387, der Relaxinrezeptor RXFP1 sowie die Steroidhormonrezeptoren für 17!-Östradiol (ER) und Progesteron (PR) bestimmt. Zusätzlich wurde die RXFP1-spezifische mRNA molekularbiologisch im Tumorgewebe dargestellt. Außerdem wurden die peripheren Hormonkonzentrationen von Relaxin, 17!-Östradiol (E2) und Progesteron (P4) ermittelt. Die Ergebnisse der vorliegenden Arbeit konnten den Beweis erbringen, dass Relaxin auch in vivo dasWachstum von Mammakarzinomen unterstützt. Relaxin bewirkte im vorliegenden Experiment eine Rekrutierung von Tumor-assoziierten Makrophagen (TAMs) ins tumorumgebenden Bindegewebe. Dadurch erfolgte dort die Synthese verschiedener Faktoren und Enzyme, welche zur bindegewebigen Erweichung, Apoptosehemmung und zu einer gesteigerten Zellproliferation führten (Bingle et al. 2002; Devetzi et al. 2008). Weiterhin induzierte die exogene Relaxingabe eine vermehrte E2-Synthese, was sich ebenfalls wachstumsfördernd und apoptosehemmend auswirkte und somit die Tumorproliferation unterstützt hat (Catalano et al. 2009; Lewis-Wambi und Jordan 2009). Die Expression des RXFP1 im Tumorgewebe wurde durch Relaxin über eine gesteigerte E2- Synthese (Wilson et al. 2008) gefördert, ebenso wie die Expression des ER. Weiterhin führte Relaxin zu einer gesteigerten P4-Synthese und zur gesteigerten Expression des PR im Tumorgewebe über einen derzeit noch unbekannten Mechanismus. Aufgrund der maßgeblichen Bedeutung des Peptidhormons für das Progressionsverhalten von Mammakarzinomen kann die Bestimmung der Relaxinblutspiegel bei Brustkrebspatientinnen deshalb in Zukunft ein wichtiges Hilfsmittel bei der Wahl der richtigen Therapie und bei der Prognosebeurteilung werden.

info:eu-repo/classification/ddc/610

ddc:610

Xenodiagnóza infekcí Leishmania major u symptomatických a asymptomatických hlodavců. / Xenodiagnosis of Leishmania major infections in symptomatic and asymptomatic rodents.

Vojtková, Barbora

January 2016

Leishmaniasis is a disease circulating in endemic areas between sand flies (Diptera: Phlebotominae) and reservoir hosts, which - in the case of Leishmania major - are principally rodents (Rodentia). Unlike in human patients, leishmaniasis is often asymptomatic in animal hosts. For transmission and maintenance of the parasite in nature, infectiousness of hosts for sand flies is essential; and the only method to directly test the infectiousness is xenodiagnosis. The main objective of this thesis is to establish a laboratory model for studying xenodiagnosis with L. major on inbred BALB/c mice and then to apply this model to potential reservoir ro- dents from the genus Mastomys. BALB/c mice were infected by intradermal inoculation of infective stages of L. major (iso- lated from sand fly guts) together with salivary gland homogenates from Phlebotomus duboscqi; infected mice were then exposed to P. duboscqi females for a period of ten weeks. Two inbred lines of BALB/c mice differed significantly in both the manifestation of the disease and infectiousness for sandflies. In BALB/c OlaHsdmice, great lesions were formed (up to 10 mm), mice were able to infect sand flies from the 2nd week after infection and their infec- tiousness reached up to 20.1% during the experiment. In BALB/c AnNCrl mice, only small...

Susceptibility and resistance to nematode infection : role of recruited vs. resident macrophages

Campbell, Sharon Mary

January 2017

Macrophages are phagocytic cells of the innate immune system, which have a central role in immune surveillance, tissue homeostasis and the immune response to bacterial, viral, protozoan and helminth parasites. It is now appreciated that many tissue resident macrophage (resMΦ) populations, including those in the peritoneal and pleural cavity, are derived prenatally prior to the establishment of definitive haematopoiesis in the bone marrow. Once seeded, these resMΦ populations are long-lived and capable of self-renewal via in situ proliferation driven by CSF-1. An inflammatory insult, such as bacterial infection, results in the recruitment of bone marrow derived macrophages (BMDMΦ) and the disappearance of the resMΦ population. BMDMΦ recruited to the site of infection become classically activated upon engagement of pathogen recognition receptors and subsequent STAT1 induction. Classically activated macrophages (CAMΦ) are highly bactericidal through the production of inflammatory cytokines, which direct the TH1 immune response, and upregulation of iNOS to generate high concentrations of intracellular nitric oxide. During resolution of acute inflammation resMΦ undergo a CSF-1 driven proliferative burst to repopulate the tissue. In contrast to bacterial infection, helminth parasites drive a TH2 immune response characterised by CD4+ T cell production of IL-4, which induces proliferation and alternative activation of the resMΦ population, thereby overcoming the need for an inflammatory influx of BMDMΦ. Alternatively activated macrophages (AAMΦ) are generated through signalling from the IL-4Rα subunit and subsequent expression of the molecules RELMα, YM1 and arginase-1. While both BMDMΦ and resMΦ upregulate RELMα, YM1 and Arg-1 in response to IL-4Rα stimulation, microarray analysis revealed an otherwise diverse transcriptional and cell surface phenotype between these populations. It was hypothesised that the diverse modes of macrophage accumulation enlisted by bacterial and helminth parasites, combined with the distinct alternative activation phenotypes employed by BMDMΦ and resMΦ populations would translate into important functional differences as regards anti-parasitic immunity. Chapter 1 and 2 of this thesis addresses the importance of macrophage origin during infection with the filarial nematode Litomosoides sigmodontis, taking advantage of the naturally occurring resistant C57BL/6 and susceptible BALB/c strains. A large disparity in MΦ accumulation was observed throughout the infection time course, with significantly larger numbers present within the pleural cavity of resistant C57BL/6 mice. This difference in MΦ number was a reflection of enhanced F4/80hi resMΦ accumulation. Through Ki67hi staining and the use of CCR2-/- and partial bone marrow chimeric mice, the expanded F4/80hi population in resistant C57BL/6 mice was shown to be a result of proliferation of the local F4/80hiGATA6+CD102+ resMΦ population. A high degree of BMDMΦ incorporation into the resMΦ pool through assumption of an F4/80hiGATA6+CD102+ phenotype was observed in both naïve and infected bone marrow chimeric animals, supporting a recent publication showing gradual incorporation of these cells into the resMΦ niche with age. Importantly, the degree of BMDMΦ incorporation into the F4/80hi population was equivalent between naïve and infected animals, despite a 27-fold difference in cell number, illustrating that expansion is a result of proliferation of local resMΦ, independent of origin. Susceptibility was marked by reduced resMΦ proliferation and enhanced recruitment of bone marrow derived F4/80lo MΦ and monocytes. These recruited BMDMΦ displaced the resMΦ population, failed to integrate the resMΦ niche and were highly positive for PD-L2, a marker specific to BMD AAMΦ. Prevention of monocyte influx and subsequent resMΦ displacement resulted in increased worm killing and a stronger TH2 immune response in susceptible BALB/c mice, thereby confirming a detrimental role for BMD AAMΦ in worm killing. Conversely, in order to confirm a protective role for the expanded resMΦ in resistant C57BL/6 mice we attempted to deplete the resMΦ population through intrapleural delivery of clodronate-loaded liposomes. Due to technical issues we were unable generate statistically significant results when depleting the resMΦ population, however a trend toward decreased worm killing in the absence of resMΦ is evident. Previously generated microarrays in the lab identified the complement cascade as being highly upregulated by AAMΦ induced in response to Brugia malayi infection compared to BMDMΦ (thioglycollate elicited). To investigate the role of complement in resistance to L. sigmodontis, Chapter 3 briefly phenotypes the macrophage compartment of C3-/- C57BL/6 mice during infection. No differences in worm burden or macrophage phenotype could be detected in C3-/- mice compared to WT controls, however this may be explained through differences in strain or MΦ origin. This chapter provides an important foundation for future studies on complement and its role in worm killing during L. sigmodontis infection. The final chapter of the thesis focuses on examining the bactericidal capabilities of BMD and resMΦ populations. An in vitro system was utilised to assess the interaction of bone marrow derived macrophages (thioglycollate elicited) and ResMΦ (from naïve mice) with Salmonella enterica serovar Typhimurium SL3261. I found that in vitro BMDMΦ are infected by/ingest SL3261 to a much greater degree than resMΦ. The resMΦ population is less efficient at both controlling the spread and killing intracellular SL3261 overtime, compared to the BMDMΦ population. In vivo however, there appears to be no difference in the ability of the monocyte derived F4/80lo MΦ and the F4/80hi resident MΦ to be infected by/ ingest SL3261, nor was a difference in bactericidal ability detected. Ultimately my work highlights that the anti-parasitic functions of MΦ populations are not dictated by origin but rather the activation phenotype upon infection and ability to respond to local stimuli.

The impact of social stress on acute Theiler's murine encephalitis virus infection.

Johnson, Robin Ranee

30 September 2004

Stress is known to alter immune function, both in positive and negative ways. The disparate effects of stress on immune function remains an active area of investigation. This thesis investigates how the application of social disruption stress either prior to or concurrent with infection alters the neuropathogenesis of Theiler's murine encephalitis virus. Experiment 1 verified that social disruption prior to infection exacerbated the course of infection. Experiment 2 examined application of social disruption concurrent with infection, and found that this may produce a delay in symptom onset, and possibly a protective effect. Experiment 3 directly compared the two schedules to each other. The previous findings were replicated and expanded with additional measures (both behavioral and physiological) that further verified the earlier findings. Social disruption applied prior to infection resulted in greater behavioral and physiological exacerbation of the disease. Concurrently applied stress remained protective or inhibitory in the disease progression. Timing of stress is one of several quantitative aspects of stress that has been found to impact the stress-immune interaction and should be further investigated.

Stress

social stress

mice

infection

CNS

inflammation

BALB/cJ

neuropathogenisis

encephalitis

virus

behavioral

Theiler's virus

The impact of social stress on acute Theiler's murine encephalitis virus infection.

Johnson, Robin Ranee

30 September 2004

Stress is known to alter immune function, both in positive and negative ways. The disparate effects of stress on immune function remains an active area of investigation. This thesis investigates how the application of social disruption stress either prior to or concurrent with infection alters the neuropathogenesis of Theiler's murine encephalitis virus. Experiment 1 verified that social disruption prior to infection exacerbated the course of infection. Experiment 2 examined application of social disruption concurrent with infection, and found that this may produce a delay in symptom onset, and possibly a protective effect. Experiment 3 directly compared the two schedules to each other. The previous findings were replicated and expanded with additional measures (both behavioral and physiological) that further verified the earlier findings. Social disruption applied prior to infection resulted in greater behavioral and physiological exacerbation of the disease. Concurrently applied stress remained protective or inhibitory in the disease progression. Timing of stress is one of several quantitative aspects of stress that has been found to impact the stress-immune interaction and should be further investigated.

Stress

social stress

mice

infection

CNS

inflammation

BALB/cJ

neuropathogenisis

encephalitis

virus

behavioral

Theiler's virus

Untersuchungen zur Bedeutung des Lipopolysaccharid-bindenden Proteins (LBP) für Mikroorganismen des Magen-Darm-Traktes von BALB/c-LBP+/+ - und BALB/c-LBP-/- (Knock-out)-Mäusen

Werth, Nadine

19 April 2006

Durch Forschungsarbeiten der neueren Zeit ist die Bedeutung der Akut-Phase-Proteine als wichtiger Bestandteil der unspezifischen Abwehr im Organismus sichtbar geworden. Die möglichen Wechselwirkungen zwischen der physiologischen Magen-Darm-Flora und diesen Proteinen sind jedoch weitesgehend unbekannt. In dieser Arbeit wurde die Magen-Darm-Flora von einem LBP-/--Knock-out-Maus-Stamm und dem Wildstamm (jeweils 20 Tiere) untersucht. Dabei wurde die aerobe Gesamtkeimzahl, die aerobe und anaerobe Gram-negative Gesamtkeimzahl und die Gesamtkeimzahl der auf MRS-Agar gewachsenen Keime in Darminhaltsproben der Darmabschnitte Jejunum, Zäkum und Kolon von oben genannten Mäusen erfasst. Zusätzlich wurden sieben serologische Untersuchungen bei 40 Tieren durchgeführt, um mögliche parallele immunologische Reaktionen des Körpers auf Bestandteile der physiologischen Magen-Darm-Flora zu erfassen und vergleichend zu betrachten. Bei den Untersuchungen konnten hochsignifikante Unterschiede bezüglich der Höhe und Zusammensetzung der aeroben Gesamtkeimzahl, der aeroben Gram-negativen Gesamtkeimzahl, der anaeroben Gram-negativen Gesamtkeimzahl und der Laktobazillen-Gesamtkeimzahl festgestellt werden. Dabei waren bei der LBP-/--Gruppe, den gendeletierten Mäusen, die aerobe Gesamtkeimzahl signifikant erhöht, die anderen Keimzahlen, insbesondere die Keimzahlen der aeroben und anaeroben Gram-negativen Bakterien und der Laktobazillen signifikant erniedrigt. Zusätzlich konnten Abweichungen verschiedener Koloniemerkmale wie Hämolyseverhalten, Koloniemorphologie und Genausprägung zwischen der LBP-/-- und der LBP+/+-Gruppe festgestellt werden. Bei den serologischen Untersuchungen konnten die Ergebnisse der mikrobiologischen Untersuchungen bestätigt werden. Es wurden signifikante Erhöhungen der relativen Antikörperspiegel gegenüber ausgewählten bakteriellen Strukturen, von Mikroorganismen, welche auch signifikant häufiger von den jeweiligen Gruppen isoliert werden konnten, festgestellt. Diese Ergebnisse lassen auf einen möglichen Zusammenhang zwischen der Gendeletion, also der Nichtexpression von LBP, und der Zusammensetzung der Magen-Darm-Flora schließen. Inwiefern dies auf direkten oder indirekten Einfluss des LBP auf die Magen-Darm-Flora zurückzuführen ist, müssen weitere Untersuchungen zeigen. Dabei sollten noch andere Einflussfaktoren, wie z. B. die Varianz des LBP in seiner genotypischen Ausprägung, berücksichtigt werden.

LBP

Gendeletion

BALB/c-Mäuse

Magen-Darm-Flora

Immunantwort

ddc:620

Estudo cinético ex vivo dos linfócitos T e B em camundongos BALB/c durante a infecção por Leishmania (Leishmania) amazonensis

Silveira Júnior, Lenilton Silva da

January 2011

Submitted by Alessandra Portugal (alessandradf@ioc.fiocruz.br) on 2013-09-17T16:37:38Z No. of bitstreams: 1 Dissertacao completa - Lenilton Silveira.pdf: 2646876 bytes, checksum: fbad76d9c78a2517359d01fc6fc96b45 (MD5) / Made available in DSpace on 2013-09-17T16:37:38Z (GMT). No. of bitstreams: 1 Dissertacao completa - Lenilton Silveira.pdf: 2646876 bytes, checksum: fbad76d9c78a2517359d01fc6fc96b45 (MD5) Previous issue date: 2011 / Fundação Oswaldo Cruz. Instituto Oswaldo Cruz. Rio de Janeiro, RJ, Brasil / Neste estudo nós realizamos um monitoramento cinético, ex vivo, da resposta imune do hospedeiro, induzida durante infecção murina por L. (L.) amazonensis. Fêmeas de camundongos BALB/c foram inoculadas subcutaneamente no coxim plantar esquerdo com 106 promastigotas de fase estacionária e o progresso da infecção foi monitorado por medição da área de lesão. Os linfócitos dos linfonodos poplíteos drenantes da lesão (LNs) foram analisados por citometria de fluxo (FACS - fluorescence-activated cell sorting) e por ressonância plasmônica de superfície (SPR - surface plasmon resonance). Os resultados de FACS indicaram que o perfil de linfócitos é definido na primeira semana de infecção e caracterizado por elevados níveis de linfócitos B e por uma diminuição de linfócitos T. O percentual de linfócitos B foi três vezes maior quando comparado com o dos camundongos não infectados e os linfócitos T eram 1,5 vezes mais baixo. Estes valores permaneceram constantes ao longo da infecção até o ultimo ponto analisado. Foi observado um discreto aumento (0.3 a 0.5) na relação CD8+/CD4+ nos animais infectados, enquanto nos não infectados esta relação permaneceu em torno de 0.35, até o último dia do estudo. Adicionalmente, nós realizamos ensaios de detecção de linfócitos T CD8+ dos LNs, em tempo real, por SPR, utilizando moléculas H-2 Ld:Ig ligadas à peptídeos da região COOH-terminal de cisteína-proteinase B de L. (L.) amazonensis (P6.3= EFCLGGGL, P6.4= CLGGGLCL, P6.5= EFCLGGGLC, P1.7= VMVEQVICF, P1.9= MVEQVICFD, P1.10= VEQVICFD). Os peptídeos testados indicaram valores de constante de associação (0.16x107 – 22.0x107) e dissociação (0.047-0.123) favoráveis a formar complexos com os dímeros H-2 Ld em pH neutro, com valores de energia livre de Gibbs < 0. De forma geral, a ligação das células ao complexo H-2 Ld:Ig/peptídeo, mostrou uma resposta (RU - Response unit) de dissociação maior em células de animais infectados (113 RU – 465 RU) que nas dos animais não infectados (71 RU – 304 RU). A resposta aos complexos H-2 Ld:Ig/peptídeo revelou diferenças de reconhecimento nas semanas avaliadas, como alta resposta ao P1.10 (227 RU) na 3ª semana e ausência de resposta ao P1.7 na 16ª semana. Em uma mesma semana de análise, vimos que o nível de reconhecimento dos peptídeos difere entre eles, uns apresentando alto valor de RU e outros um valor mais baixo: 3ª (P1.10>P6.3>P1.9>P1.7>P6.4>P6.5), 4ª (P6.3.>P6.5>P1.9>P6.4>P1.7), 6ª (P6.4>P1.10>P1.9>P1.7>P6.5), 12ª (P1.9.>P6.3>P1.10>P6.5), 18ª semana (P6.4=P1.9>P6.3>P1.10>P1.7). Embora, apenas, dois peptídeos tenham sido testados na 1ª semana, a maior resposta foi relacionada ao P1.7 (161 RU), seguido do P1.9 (115 RU). Os dados gerados indicaram uma flutuação na população dos linfócitos T e B, assim como o envolvimento de linfócitos T CD8+ direcionados a peptídeos da região COOH-terminal da CPB, ao longo da infecção / In this study, we performed a kinetic ex vivo monitoring of host immune responses during murine infection with Leishmania (Leishmania) amazonensis. Female BALB/c mice were injected subcutaneously in the left hind footpad with 106 promastigotes in stationary growth phase and the progression of infection was monitored by measuring lesion area expansion. Lymphocytes from lesion draining popliteal lymph nodes (LNs) were analyzed by fluorescence-activated cell sorting (FACS) and surface plasmon resonance (SPR). FACS results indicated that the lymphocytes profile is defined in the first week post infection and was characterized by high levels of B cells and by a decrease in T cell numbers. The percentage of B lymphocytes was three times higher when compared to the non-infected mice and T lymphocytes were up to 1.5 times lower. These values remained constant throughout infection until the last point analyzed. It was observed a slight increase (0.3 to 0.5) in the CD8+/CD4+ ratio in the infected mice, whereas in the not infected group this ratio remained around 0.35, until the last assessed infection day. Additionally, we have performed an assay to detect CD8+ T lymphocytes from LNs in real time, by SPR, utilizing H-2 Ld:Ig molecules bound to peptides derived from the COOH-terminal region of cysteine-proteinase B from L. (L.) amazonensis (P6.3= EFCLGGGL, P6.4= CLGGGLCL, P6.5= EFCLGGGLC, P1.7= VMVEQVICF, P1.9= MVEQVICFD, P1.10= VEQVICFD). The peptides tested presented values of association (0.16x107 – 22.0x107) and dissociation constant (0.047-0.123) favorable to form complexes with H-2 Ld at neutral pH, with values of Gibbs free energy < 0. In general, the binding of cells to the H-2 Ld:Ig/peptide complexes showed a response unit (RU) of dissociation higher in cell preparations from infected mice (113 RU - 465 RU) than the cells from uninfected mice (71 RU – 304 RU). The recognition response to the complex H-2 Ld:Ig/peptide were assessed at different weeks as high response to P1.10 (227 RU) at 3th week and absence of response to P1.7 at 16th week. In the same week of analysis, we found that the level of recognition of peptides differs among them, some presenting a high value of RU and others a lower value: 3th (P1.10 >P6.3>P1.9>P1.7>P6.4>P6.5), 4th (P6.3.>P6.5>P1.9>P6.4>P1.7), 6th (P6.4> P1.10>P1.9>P1.7>P6.5), 12th (P1.9.>P6.3>P1.10>P6.5), 18th week (P6.4=P1.9>P6.3>P1.10>P1.7). Although only two peptides were tested at 1th week, the highest response was related to P1.7 (165 RU), followed by P1.9 (115 RU). Generated data indicated a fluctuation in the population of T and B lymphocytes, as well as the involvement of CD8+ T cells directed to peptides of the COOH-terminal region of the CPB, throughout the infection

Camundongos BALB/c

Leishmania (Leishmania) amazonensis

Peptídeos

Linfócitos

Citometria de fluxo

Ressonância plasmônica de superfície

Estudo das alterações do estado de mal epiléptico induzido por pilocarpina no cérebro de camundongos imunodeficientes BALB/c nude / Study of the pilocarpine-induced status epilepticus changes in brain of immunodeficient BALB/c nude mice

Vignoli, Thiago [UNIFESP]

29 September 2010

Made available in DSpace on 2015-07-22T20:50:07Z (GMT). No. of bitstreams: 0 Previous issue date: 2010-09-29 / A epilepsia acomete cerca de 1 a 2% da população mundial e carece de propostas terapêuticas mais eficazes. Aproximadamente 30% das epilepsias são sintomáticas e a epilepsia do lobo temporal (ELT) se destaca pela alta incidência e gravidade. Cerca de 30% de pacientes com ELT possuem crises refratárias ao tratamento medicamentoso, sendo necessário, muitas vezes, intervenção cirúrgica para o controle das mesmas. A investigação dos mecanismos fisiopatológicos empregando tecido humano extraído cirurgicamente, embora muito importante, tem a limitação de refletir apenas o processo crônico em que as alterações moleculares, bioquímicas e de neuroplasticidade resultantes do quadro epiléptico já se encontram estabelecidos. Nesse sentido, os modelos experimentais são fundamentais por permitir uma melhor abordagem dos mecanismos envolvidos com a epileptogênese, ou seja, aqueles ativados durante a indução até o estabelecimento do quadro epiléptico. O modelo lesional de epilepsia induzida por pilocarpina em pequenos roedores tem sido amplamente utilizado por reproduzir as principais características da ELT. Nesse modelo as crises epilépticas são acompanhadas por uma ação combinada entre o sistema imune, nervoso e endócrino, envolvendo a ativação de mediadores como citocinas, quimiocinas, neurotransmissores e seus receptores celulares. Estes processos têm sido associados com a etiologia da condição epiléptica. No presente projeto, camundongos imunodeficientes BALB/c nude foram submetidos ao modelo de epilepsia induzida por pilocarpina, para caracterização das alterações comportamentais, eletrográficas, neuroquímicas e histológicas comparadas ao seu controle BALB/c. Os resultados indicaram que a integridade do sistema imunológico é necessário para proteger o sistema nervoso central do insulto causado pelo status epilepticus (SE) induzido pela pilocarpina. Após a aplicação da pilocarpina, os animais BALB/c nude apresentaram um maior número de crises tônicoclônicas até atingirem o SE, apresentando um alto índice de mortalidade quando comparados ao BALB/c. Os camundongos BALB/c nude também apresentaram uma maior ativação de c-Fos em áreas relacionadas com a circuitaria das crises e uma menor expressão de parvalbumina, uma proteína ligadora de cálcio intracelular em relação ao BALB/c estudado na mesma condição experimental. Diferenças nas concentrações de neurotransmissores excitatórios e inibitórios também foram observados no córtex e hipocampo do BALB/c nude em relação ao BALB/c. Os camundongos BALB/c nude tiveram aumento na concentração de aminoácidos excitatórios sem a alteração compensatória dos aminoácidos inibitórios durante as crises, conforme ocorreu nos camundongos BALB/c. A morte neuronal avaliada pelas técnicas histológicas de Fluoro Jade-B e Nissl, também se mostrou aumentada em algumas áreas do sistema nervoso central dos camundongos BALB/c nude que apresentaram SE em relação ao BALB/c Os dados sugerem uma correlação positiva entre ativação de c-Fos, concentração de aminoácidos excitatórios e morte neuronal nos camundongos BALB/c nude, sugerindo que a deficiência imunológica possa ter contribuído para a hiperexcitabilidade e vulnerabilidade do sistema nervoso central aos danos causados pelas crises. / Epilepsy affects about 1-2% of world population and lack of effective therapeutic interventions more effective. Approximately 30% are symptomatic of epilepsy and temporal lobe epilepsy (TLE) is distinguished by the high incidence and severity. About 30% of patients with TLE seizures are refractory to treatment, if necessary, often, surgical intervention for control of them. The investigation of pathophysiology mechanism using human tissue extracted surgically, although very important, is limited by reflects only the chronic process in which the molecular, biochemical, and neuronal plasticity alterations resulting from epileptic effects already established. Thus, experimental models are essential for better approach of the mechanisms involved in epileptogenesis. The epilepsy induced by pilocarpine in small rodents has been widely used for reproducing the main features of TLE. In this model, the seizures are accompanied by a combined action between immune system, nervous and endocrine systems, involving the mediators activation such as cytokines, chemokines, neurotransmitters and their cell receptors. These processes have been associated with the etiology of the epileptic condition. In this project, immunodeficient BALB/c nude mice submitted to epilepsy model induced by pilocarpine to characterize behavior, electrographic, histological and neurochemical changes compared to their control BALB/c. The results indicated that integrity of the immune system is necessary to protect the central nervous system insult caused by status epilepticus. After administration of pilocarpine, the BALB/c nude mice showed a larger number of tonic-clonic seizures, with a high mortality rate when compared to BALB/c. The BALB/c nude also showed a greater activation of c-Fos in areas related to the circuitry of the crisis and a lower expression of parvalbumin, an intracellular calcium-binding protein compared to BALB/c studied in the same experimental condition. Differences concentrations of excitatory and inhibitory neurotransmitters were also observed in cortex and hippocampus of the BALB/c nude compared to BALB/c. The BALB/c nude showed increased of the excitatory amino acids concentrations without compensatory alteration in the inhibitory amino acids during seizure, as occurred in BALB/c. Neuronal death measured by Fluoro Jade- B and Nissl histological techniques, was also increased in some areas of the central nervous system of BALB/c nude SE presented relative to BALB/c. The data suggest a positive correlation between c-Fos activation, excitatory amino acids concentration and neuronal death in BALB/c nude mice, suggesting that immune deficiency may have contributed to the hyperexcitability and vulnerability of the central nervous system injury caused by seizure. / TEDE / BV UNIFESP: Teses e dissertações

Morte Neuronal

BALB/c nude

Pilocarpina

Sistema imunológico

Epilepsia

Pilocarpine

Epilepsy

Immune System

Papel de antígenos secretados de uma linhagem atenuada de Corynebacterium pseudotuberculosis na indução de resposta imune em camundongos

Rodrigues, Gabriele Costa

January 2009

Submitted by Hiolanda Rêgo (hiolandarego@gmail.com) on 2015-10-20T16:10:30Z No. of bitstreams: 1 Dissertação_ICS_ Gabriele Costa Rodrigues.pdf: 669924 bytes, checksum: 39da9a8e9734a6d7491ddbfaf0f55cd4 (MD5) / Made available in DSpace on 2015-10-20T16:10:30Z (GMT). No. of bitstreams: 1 Dissertação_ICS_ Gabriele Costa Rodrigues.pdf: 669924 bytes, checksum: 39da9a8e9734a6d7491ddbfaf0f55cd4 (MD5) / A linfadenite caseosa é uma doença infecciosa crônica que afeta ovinos e caprinos, causada por uma bactéria intracelular facultativa, Corynebacterium pseudotuberculosis. Pouco se conhece sobre a imunorreatividade induzida por diferentes linhagens deste microrganismo, bem como sobre o efeito no hospedeiro de seus antígenos secretados. O objetivo deste trabalho foi avaliar o reconhecimento antigênico e a ativação de células esplênicas de camundongos Balb/c infectados com duas linhagens de C. pseudotuberculosis, utilizando para tanto dois preparados antigênicos obtidos a partir da linhagem atenuada T1, denominados SeT1 e Q5, ao longo dos primeiros 35 dias após a inoculação. Os camundongos foram infectados com 102 CFU da linhagem VD57 ou da linhagem T1 e sacrificados nos dias 0, 15 e 35. A resposta humoral e celular foram avaliadas pela identificação de IgG total e subclasses, específicas contra estes antígenos secretados, bem como pela quantificação de citocinas produzidas “in vitro”, contra estas mencionadas biomoléculas. O grupo infectado com a linhagem selvagem VD57 apresentou diversas lesões granulomatosas, ao contrário dos camundongos infectados com a linhagem atenuada T1 que não desenvolveram lesões. A linhagem VD57 induziu expressiva produção de TNF-alfa, IFN-gama e IL-10, enquanto que a produção de IL-4 foi semelhante nos dois grupos, apesar de ter apresentado valores significativos com a estimulação pela fração Q5. Através do “Western Blotting” foi possível identificar quatro bandas na fração antigênica Q5, reativas com soros de camundongos infectados com a linhagem T1. Utilizando-se o ensaio imunoenzimático ELISA observou-se uma baixa resposta pelo grupo infectado com a linhagem T1 e uma resposta expressiva dos animais infectados com a linhagem VD57 apenas no dia 35. Neste último grupo, notou-se resposta predominante de IgG1 e IgG2a quando se utilizou como antígeno, respectivamente os preparados Q5 e SeT1. Os dados mostram que os dois preparados antigênicos foram capazes de estimular a imunidade humoral e celular, entretanto, ativando diferentemente os padrões de resposta Th1 e Th2.

Ciências da Saúde

resposta imune

Corynebacterium pseudotuberculosis

antígeno secretado

fração protéica

camundongos Balb/c