Imunofenotipagem e avaliação quantitativa de linfócitos circulantes de bovinos da raça curraleiro / Immunophenotyping and quantitative assessment of circulating lyphocytes of the breed of Curraleiro Cattle

MORAES, Júlia de Miranda

03 March 2008

Made available in DSpace on 2014-07-29T15:07:56Z (GMT). No. of bitstreams: 1 Dissertacao Julia de Miranda Moraes.pdf: 1781008 bytes, checksum: 240b1d82cc44d5f20591020197abd396 (MD5) Previous issue date: 2008-03-03 / The Curraleiro cattle are extremely docile and resistant to infectious diseases and parasites. They may be used in exploration of low-quality pastures, without great investments, when other breeds could show a low productivity or even survival difficulties. This genetic potential runs risk to extinction due to its replace by more productive breeds. The Curraleiro cattle resistence to illness is popularly known and many works has been published about it, although its immunologic system physiology is completely unknown. Such features are plausible reasons for the preservation of this potentially genetic resource. So, the mean aim of this study was to establish an immunological profile by marking and quantification of T and B lymphocytes in Curraleiro breed with immunocytochemistry. Thus, it was used 116 bovines, male and female, with different ages from two farms situated at Goiás State, Brazil. The animals were allotted in groups according to age, sex and origin. Blood samples were collected and processed in accordance with immunocytochemistry standard technique using lymphoid markers species-specific, anti-CD3 (MM1A BoCD3) and anti-LB (LCTB16A clone B-B14), for T and B lymphocytes counting, respectively. All procedures were accomplished at Veterinary School, Federal University of Goiás, Brazil. The data were submitted to descriptive statistics and then to Kruskall Wallis and Mann-Whitney tests. The results showed decreased levels of leukocytes, lymphocytes, T lymphocytes and B lymphocytes along the age advance. Absolute values of leukocytes, lymphocytes and T lymphocytes were higher in males than females. None of the evaluated parameters were affected by differences of the management carried out at two farms. / O gado Curraleiro é extremamente dócil, resistente às doenças e parasitas, que pode ser utilizado, sem grandes investimentos na exploração de pastagens naturais de baixa qualidade onde outras raças teriam baixa produtividade ou até mesmo dificuldades de sobrevivência. Todo esse potencial genético encontra-se em sério risco de extinção, uma vez que esses animais vêm sendo substituídos por outros com maior produtividade. A resistência do Curraleiro às enfermidades é popularmente conhecida e divulgada, porém desconhece-se por completo a fisiologia do sistema imunológico desses animais. Estas características são notáveis justificativas para conservar este recurso genético potencialmente importante. Assim, este estudo teve por objetivo traçar um perfil imunológico, através de marcação imunocitoquímica e quantificação de linfócitos T e B em bovinos da raça Curraleiro. Para tal, foram utilizados 116 animais entre machos e fêmeas, de diferentes faixas etárias, provenientes de duas propriedades de criação de gado Curraleiro do Estado de Goiás, sendo alocados em grupos conforme a faixa etária, sexo e origem. As amostras de sangue foram colhidas e processadas de acordo com o padrão da técnica de imunocitoquímica e posteriormente utilizados os marcadores linfóides espécieespecíficos, anti-CD3 (MM1A BoCD3) e anti-LB (LCTB16A clone B-B14), para a quantificação de linfócitos T e linfócitos B, respectivamente. Todo procedimento foi realizado na Escola de Veterinária da UFG. Inicialmente os dados foram submetidos à estatística descritiva e posteriormente ao teste de Kruskall Wallis e Mann-Whitney. Com o avançar da idade, diminuíram-se os níveis de leucócitos, linfócitos, linfócitos T e linfócitos B. Os valores absolutos de leucócitos, linfócitos e linfócitos T foram maiores nos machos em relação às fêmeas. Nenhum dos parâmetros avaliados sofreu influência em relação à diferença de qualidade de manejo nas duas propriedades.

Cytogenetic and molecular characterization of CD3-CD4+ T cells from patients with the lymphocytic variant of hypereosinophilic syndrome / Caractérisation cytogénétique et moléculaire des cellules T CD3-CD4+ de patients atteints de la variante lymphocytaire du syndrome d'hyperéosinophilie

Ravoet, Marie

16 April 2010

La variante lymphocytaire du syndrome hyperéosinophilique (L-SHE) est une pathologie extrêmement rare caractérisée par une prolifération monoclonale de lymphocytes T surproduisant l’interleukine IL-5, responsable d’une hyperéosinophilie persistante. En outre, un immunophénotype aberrant CD3−CD4+ est fréquemment observé à la surface des cellules T clonales. Cette pathologie se distingue par une lymphoprolifération chronique indolente habituellement révélée par une hyperéosinophilie sanguine et une infiltration éosinophilique des tissus cutanés. Toutefois, l’évolution vers un lymphome T observée chez certains patients suggère la présence d’un potentiel malin des cellules T. Ce modèle représente donc une rare opportunité d’identifier les changements moléculaires liés aux différentes étapes du processus transformant lymphoïde T.<p>Dans le cadre de ce travail, nous avons cherché à établir les caractéristiques cytogénétiques et moléculaires des cellules T CD3−CD4+ d’une cohorte de patients L-SHE. L’analyse cytogénétique de cellules T CD3−CD4+ isolées au moment du diagnostic chez deux patientes (P1 et P2) a révélé la présence d’une délétion similaire 6q13-q22.1. En étudiant les stades cliniques successifs de P1 et P2, nous avons montré la persistance des cellules porteuses de la délétion 6q au cours de la progression chronique et leur prédominance lors du développement d’un lymphome T chez P1. Ces résultats suggèrent l’implication précoce et potentiellement critique de la délétion 6q dans cette pathologie lymphoproliférative T. L’analyse des dérégulations transcriptionnelles résultant de ce remaniement a montré une réduction de l’expression des gènes pro-apototiques BACH2 et PA26 dans les cellules T CD3−CD4+ de P1 et P2. En particulier, BACH2, dont l’expression diminue continuellement au cours de l’évolution de P1, jouerait un rôle oncosuppresseur dans la lymphogenèse T.<p>Afin d’identifier les modifications moléculaires des cellules T clonales, nous avons analysé l’expression de 95% des gènes humains dans les cellules T CD3−CD4+ de trois patients en phase chronique (P1, P2 et P3). La grande homologie des changements transcriptionnels chez les trois patients indique une altération des mêmes mécanismes moléculaires. Ainsi, un profil immunophénotypique exhaustif, validé chez trois patients supplémentaires, a pu être établi. En outre, les dérégulations des voies apoptotiques, TGFβ ou<p>9<p>encore de signalisation intracellulaire altèrent l’homéostasie des cellules T CD3−CD4+ pouvant favoriser la perte de la capacité apoptotique et/ou la croissance cellulaire. Cette signature moléculaire a été étendue par l’identification de 20 microARNs dont l’expression est dérégulée dans les cellules T CD3−CD4+ d’une cohorte de 6 patients. Par ailleurs, la modification de l’expression des récepteurs impliqués dans la migration leucocytaire au cours de l’évolution de P1 pourrait expliquer l’infiltration ganglionnaire des cellules T clonales et la progression du lymphome.<p>La caractérisation des désordres cytogénétiques et moléculaires des cellules T CD3−CD4+ chez les patients L-SHE permettrait à terme d’identifier de nouveaux marqueurs diagnostiques et contribuer ainsi au développement de nouvelles cibles thérapeutiques dans une grande diversité de pathologies lymphoprolifératives de type Th2. / Doctorat en Sciences biomédicales et pharmaceutiques / info:eu-repo/semantics/nonPublished

Disciplines biomédicales diverses

Eosinophilia

Lymphoproliferative disorders

T cells

Cell proliferation

Eosinophilie

Syndromes lymphoprolifératifs

Lymphocytes T

Cellules -- Prolifération

profil d'expression

TGFb

TGFb / Syndrome d'hyperéosinophilie

6q

lymphome T

cellule T CD3-CD4+

CD3-CD4+ T-cell lymphoma

Hypereosinophilic syndrome

Immunhistokemisk (IHC) analys av låggradigt inflammerade biopsier med apikal parodontit -en pilotstudie / Immunohistochemical (IHC) analysis of biopsies with apical periodontitis with assessed low-grade inflammation – a pilot study

Pesonen, Izabell, Ismail, Midia

January 2021

Syfte: Att ta reda på hur relationen ser ut för B- respektive T-lymfocyter i biopsier av rotfyllda tänder med apikal parodontit med bedömd låggradig inflammation. Denna studie kommer även att analysera hur den inflammatoriska bilden ser ut i förhållande till beskrivna symtom i dessa biopsier. Material &amp; metod: En pilotstudie utfördes på 10 biopsier från rotfyllda tänder med apikal parodontit med bedömd låggradig inflammation enligt Danesh et al 2019 klassificeringssystem. Biopsierna hämtades från Malmö universitets biobank. Immunhistokemisk infärgning av antigenerna CD20+ och CD3+ utfördes samt analyserades med hjälp av digitalmikroskop. Jämförelsen av symtomen från remisserna skedde efter att de histologiska resultaten sammanställts. Resultat: Det fanns fler T-lymfocyter än B-lymfocyter i 6 stycken av biopsierna. I de resterande 4 biopsierna var de lika många. I remisserna hade symtombilden inte angetts föralla biopsier. Slutsats: Enligt vår pilotstudie ser vi tendenser till att T-lymfocyter är fler än B-lymfocyter eller att de är lika många. Inga slutsatser kunde dras gällande symtombilden. Ett större material från olika remittenter krävs för definitiva slutsatser. En vidare infärgning av CD4+ samt CD8+ skulle vara intressant. / Aim: To investigate the relation between B- and T- lymphocytes in biopsies of root-filled teeth with apical periodontitis with assessed low-grade inflammation. This study will also analyse what the inflammation looks like in relation to the symptoms described in these biopsies.  Study design: A pilot study was performed on 10 biopsies of root-filled teeth with apical periodontitis with assessed low-grade inflammation according to the classification system of Danesh et al 2019. The biopsies were collected from Malmö University's biobank. An immunohistochemical staining of antigens CD20+ and CD3+ were performed and analysed by a digital microscope. A comparison of the symptoms from the referrals were performed once the histological results were compiled. Results: There were more T-lymphocytes than B-lymphocytes in 6 of the biopsies. In the remaining 4 biopsies there were an equal amount of B- and T-lymphocytes. The symptoms were not stated for all biopsies in the referrals.  Conclusion: According to our pilot study, we see tendencies that T lymphocytes are more than B lymphocytes or that they are equal. No conclusions could be drawn regarding the symptom picture. Larger material from different referrers is required for definitive conclusions. A further staining of CD4 + and CD8 + would be interesting.

Apical periodontitis

B-lymphocytes

biopsy

CD3

CD20

Immunohistochemistry

low-graded inflammation

T-lymphocytes

persistent periapical pathology

Apikal parodontit

B-lymfocyter

T-lymfocyter

CD3

CD20

biopsi

låggradig inflammation

rotfyllning

immunhistokemi

Dentistry

Odontologi

The importance of the intracytoplasmic domain of CD3 epsilon in thymocyte development /

Li, Samantha.

January 2009

The development of T cells in the thymus is a tightly regulated process. Any defect in thymic differentiation could result in autoimmune disorders, inability to ward off infections or neoplasm. Early thymocyte development requires signals mediated through the preTCR complex by the associated CD3 chains (gamma, delta, epsilon, and zeta). Research conducted towards this project has revealed that signaling modules within the intracytoplasmic domain of CD3epsilon is absolutely required for this process. Interestingly, our results emphasized the importance of the proline-rich sequence motif in preTCR mediated signaling events, such as the proliferation of double negative thymocytes and the regulation of TCR surface expression on double positive thymocytes in a stage-specific manner. The outcomes of this project may provide a better understanding of the mechanism of preTCR-mediated thymocyte differentiation and the role of CD3 chains in these processes.

Thymus Gland -- immunology.

Thymus Gland -- cytology.

Antigens, CD3 -- immunology.

Cytoplasm -- immunology.

Cell Differentiation -- immunology.

Mice, Knockout.

Mice.

EFFECTS ON SEMEN QUALITY AND ON ESTABLISHMENT OF PERSISTENT EQUINE ARTERITIS VIRUS (EAV) INFECTION IN STALLIONS FOLLOWING EXPERIMENTAL CHALLENGE WITH THE KENTUCKY 84 (KY84) STRAIN

Campos, Juliana Roberta

01 January 2012

Equine arteritis virus (EAV) is the causal agent of equine viral arteritis (EVA), a disease of equids. Following EAV infection, up to 70% of stallions may become carriers and continuously shed the virus in their semen for varying time periods. The long-term carrier stallion has an important role in the transmission and maintenance of EAV in horse populations. Recently, it has been demonstrated a correlation between in vitro susceptibility of CD3+ T lymphocytes to EAV infection and establishment of long-term persistent infection among stallions following natural infections. In this study, we investigated whether stallions with in vitro EAV susceptible CD3+ T lymphocytes are at higher risk of becoming long-term carriers compared to those with the resistant phenotype following experimental infection with the KY84 strain of EAV. Furthermore, we investigated whether there is a significant effect of EAV infection on semen quality during acute phase of the infection. The data suggested that the establishment of the long-term carrier state seems to be associated with the in vitro CD3+ T lymphocyte susceptible phenotypes and that reduced semen quality resulted from the combined effect of fever and scrotal edema observed following EAV infection rather than the direct effect of the virus.

Equine arteritis virus

equine viral arteritis

persistent viral infection

carrier stallions

Immunology and Infectious Disease

Study of cysteines in the stalk region of CD3 proteins : evolutionarily conserved residues critical for T cell development and function /

Wang, Yibing,

January 2008

Thesis (Ph.D. in Immunology) -- University of Colorado Denver, 2008. / Typescript. Includes bibliographical references (leaves 138-153). Free to UCD Anschutz Medical Campus. Online version available via ProQuest Digital Dissertations;

The importance of the intracytoplasmic domain of CD3 epsilon in thymocyte development /

Li, Samantha.

January 2009

No description available.

Mice, Knockout.

Cell Differentiation -- immunology.

Thymus Gland -- cytology.

Cytoplasm -- immunology.

Antigens, CD3 -- immunology.

Mice.

Thymus Gland -- immunology.

Increased number of T cells and exacerbated inflammatory pathophysiology in a human IgG4 knock-in MRL/lpr mouse model / ヒトIgG4ノックインMRL/lprモデルマウスにおけるT細胞数の増加と炎症病態の増悪

Gon, Takaho (Yoshie)

23 March 2023

京都大学 / 新制・課程博士 / 博士(医学) / 甲第24528号 / 医博第4970号 / 新制||医||1065(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 伊藤 能永, 教授 羽賀 博典, 教授 河本 宏 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

IgG4

MRL/lpr mice

CD3+B220+CD138+ T cells

allergy

myasthenia gravis

pemphigus

IgG4-related diseases

490

Alterations in lymphocyte signalling produced by exposure to mercury

Yole, Margaret Jane

03 July 2007

The effects of 1 min 4 hr exposures to mercuric chloride (HgCl2), methyl mercuric chloride (CH3HgCl), p-chloromercuribenzoate (p-CMB) and ethylmercurithiosalicylate (TMS) on cell viability and kinetics of cell death, microtubules, F-actin, CD3 receptor expression, protein tyrosine phosphorylation (PTyr-P), intracellular calcium [Ca2+]i and responses to polarized signals in YAC-1 lymphoma cells were investigated. We hypothesized that immunotoxic effects of HgCl2 (Hg2+) are initiated by global receptor triggering, accompanied by increased protein tyrosine phosphorylation (PTyr-P) and down-regulation of the T-cell receptor (TCR). As a polychloride anion with poor lipid solubility, inorganic Hg2+ may produce effects at the outer cell membrane before significant intracellular accumulation, loss of microtubule integrity (a sensitive target) and activation of cell death through apoptotic pathways. The organomercurial compound p-CMB is likewise thought to penetrate membranes slowly as a result of ionization. In contrast, the highly lipid-soluble organomercurial compounds CH3HgCl and TMS were expected to reduce responses to polarized stimuli only in conjunction with and not prior to loss of microtubule integrity and the onset of necrotic cell death. <p>Two general patterns of effects were observed. In HgCl2-treated YAC-1 cells, inhibition of responses to polarized stimuli preceded loss of microtubules and onset of cell death. Effects on polarized stimuli were preceded by a transient Ca2+ signal; however, this Ca2+ signal appeared abortive, accompanied by a paradoxic decrease in PTyr-P and partial down-regulation of CD3 receptors. Responses to polarised stimuli were inhibited prior to extensive loss of microtubule staining, indicating effects preceded cytosolic Hg2+ accumulation. HgCl2 exposure was followed rapidly by necrotic cell death. <p>Similarly, p-CMB-treated YAC-1 cells failed to respond to polarized stimuli before effects on microtubules or loss of viability, and proceeded rapidly to late apoptosis; however, a transient Ca2+ signal and progressive loss of F-actin preceded effects in all other assays and may account for loss of polarized responses. <p>In CH3HgCl- and TMS-treated YAC-1 cells, CD3 receptor expression, [Ca2+] and PTyr-P were increased immediately, along with loss of microtubules. These reductions preceded inhibition of polarized signaling responses and seemed to indicate a general loss of cellular homeostasis not seen in HgCl2- and p-CMB-treated cells; loss of homeostasis did not necessarily produce simultaneous loss of viability, as TMS-treated cells remained viable for 30 min while CH3HgCl-treated cells became apoptotic within 1 min. Nonetheless, the YAC-1 cells proceeded to cell death more slowly, remaining early apoptotic after 4 hr, when almost all HgCl2- and p-CMB-treated cells were necrotic. These findings indicate the two groups of mercury compounds may alter responses to polarized stimuli and induce cell death by distinct pathways, one involving an apparently abortive signal and the other mediated by much more profound disruption of cellular homeostasis. Within the larger patterns there are further differences between the effects produced by each Hg compound, likely reflecting the combined influence of pharmacokinetic and dynamic factors governing access to and interactions with different cellular targets leading to cell death. These distinct targets may in turn be reflected in the different immune effects produced by these compounds <i>in vivo</i>.

methyl mercuric chloride

mercuric chloride

phosphotyrosine

CD3 receptor

intracellular calcium

microtubles

actin

immunological synapse

organic mercury

inorganic mercury

p-chloromercuribenzoate

thimerosal

YAC-1 lymphoma

cytotoxicity

apoptosis

viability

Alterations in lymphocyte signalling produced by exposure to mercury

Yole, Margaret Jane

03 July 2007

The effects of 1 min 4 hr exposures to mercuric chloride (HgCl2), methyl mercuric chloride (CH3HgCl), p-chloromercuribenzoate (p-CMB) and ethylmercurithiosalicylate (TMS) on cell viability and kinetics of cell death, microtubules, F-actin, CD3 receptor expression, protein tyrosine phosphorylation (PTyr-P), intracellular calcium [Ca2+]i and responses to polarized signals in YAC-1 lymphoma cells were investigated. We hypothesized that immunotoxic effects of HgCl2 (Hg2+) are initiated by global receptor triggering, accompanied by increased protein tyrosine phosphorylation (PTyr-P) and down-regulation of the T-cell receptor (TCR). As a polychloride anion with poor lipid solubility, inorganic Hg2+ may produce effects at the outer cell membrane before significant intracellular accumulation, loss of microtubule integrity (a sensitive target) and activation of cell death through apoptotic pathways. The organomercurial compound p-CMB is likewise thought to penetrate membranes slowly as a result of ionization. In contrast, the highly lipid-soluble organomercurial compounds CH3HgCl and TMS were expected to reduce responses to polarized stimuli only in conjunction with and not prior to loss of microtubule integrity and the onset of necrotic cell death. <p>Two general patterns of effects were observed. In HgCl2-treated YAC-1 cells, inhibition of responses to polarized stimuli preceded loss of microtubules and onset of cell death. Effects on polarized stimuli were preceded by a transient Ca2+ signal; however, this Ca2+ signal appeared abortive, accompanied by a paradoxic decrease in PTyr-P and partial down-regulation of CD3 receptors. Responses to polarised stimuli were inhibited prior to extensive loss of microtubule staining, indicating effects preceded cytosolic Hg2+ accumulation. HgCl2 exposure was followed rapidly by necrotic cell death. <p>Similarly, p-CMB-treated YAC-1 cells failed to respond to polarized stimuli before effects on microtubules or loss of viability, and proceeded rapidly to late apoptosis; however, a transient Ca2+ signal and progressive loss of F-actin preceded effects in all other assays and may account for loss of polarized responses. <p>In CH3HgCl- and TMS-treated YAC-1 cells, CD3 receptor expression, [Ca2+] and PTyr-P were increased immediately, along with loss of microtubules. These reductions preceded inhibition of polarized signaling responses and seemed to indicate a general loss of cellular homeostasis not seen in HgCl2- and p-CMB-treated cells; loss of homeostasis did not necessarily produce simultaneous loss of viability, as TMS-treated cells remained viable for 30 min while CH3HgCl-treated cells became apoptotic within 1 min. Nonetheless, the YAC-1 cells proceeded to cell death more slowly, remaining early apoptotic after 4 hr, when almost all HgCl2- and p-CMB-treated cells were necrotic. These findings indicate the two groups of mercury compounds may alter responses to polarized stimuli and induce cell death by distinct pathways, one involving an apparently abortive signal and the other mediated by much more profound disruption of cellular homeostasis. Within the larger patterns there are further differences between the effects produced by each Hg compound, likely reflecting the combined influence of pharmacokinetic and dynamic factors governing access to and interactions with different cellular targets leading to cell death. These distinct targets may in turn be reflected in the different immune effects produced by these compounds <i>in vivo</i>.

methyl mercuric chloride

mercuric chloride

phosphotyrosine

CD3 receptor

intracellular calcium

microtubles

actin

immunological synapse

organic mercury

inorganic mercury

p-chloromercuribenzoate

thimerosal

YAC-1 lymphoma

cytotoxicity

apoptosis

viability