AIRE-exprimující buňky v imunitní toleranci ve zdraví a nemoci / AIRE-expressing cells in immune tolerance in health and disease

Vobořil, Matouš

January 2020

The process of self-nonself discrimination by the immune system is a fundamental attribute of healthy organisms. Since T-cell receptors (TCRs) are generated by the random process of somatic recombination without regard to its targets, the newly developed T-cell clones could recognize either self or nonself antigens. The mechanisms of central tolerance robustly limit the self-reactive repertoire within the T-cell population via deletion of clones that express self-reactive TCRs or their deviation into the regulatory T-cells (Tregs). These processes occur mainly in the thymic medulla where the TCR reactivity to self-antigens is tested by various types of antigen-presenting cells, mainly medullary thymic epithelial cells (mTECs), dendritic cells (DCs), and B-cells. The cooperation between these cell-types has been shown to be essential for the establishment of thymic tolerance. A key molecule regulating the production of self-antigens is the autoimmune regulator (AIRE), which is thought to be expressed primarily by mTECs and its mutations are associated with the development of severe autoimmune disorders. In this context, the presented thesis describes the novel regulatory pathways important for the development of a functional and "harmless" repertoire of T-cells and for enforcement of tolerance....

Spinal Muscular Atrophy: Evidence of a Multi-System Disease

Deguise, Marc-Olivier

10 January 2020

Spinal muscular atrophy (SMA) is a devastating recessive neurological disorder thought to be affecting primarily the motor neurons. As such, paralysis, motor weakness and death ensue. While SMA is most commonly seen in infants and children, it can span all ages. Its genetic etiology revolves around the homozygous deletion or mutation of the SMN1 gene, whose product (SMN protein) has critical and ubiquitous roles in mRNA splicing, amongst various other functions in mRNA metabolism. As such, SMN depletion in other non-neuronal cells type is likely to have physiological repercussions, and perhaps modulate the SMA phenotype. Herein, we identify the molecular pathways of atrophy in skeletal and cardiac muscle of two mouse models of SMA and their therapeutic modulation via the histone deacetylase inhibitor trichostatin A. We also identify dramatic changes in immune organs in mouse models of SMA, which could impact susceptibility to infections. Furthermore, we establish the presence of important defects in fatty acid homeostasis in the liver and plasma seen in both mouse models and SMA patients. Finally, we provide the first mild mouse model of SMA that reliably reproduces canonical features of SMA, permitting aging studies. This model presents with a prominent myopathic phenotype prior to motor neuron death, without extra-neuronal involvement during the course of its lifespan. Overall, our work shows multiple potentially clinically relevant defects in extra-neuronal organs, provides ways to abrogate them and provides a framework to study them over the course of aging.

Muscle

Immune system

Metabolism

Aging

SMA

Non-neuronal defects

HDAC inhibitors

NAFLD

Non-alcoholic fatty liver disease

Dyslipidemia

Atrophy

spleen

Thymus

Liver

Diet

全身イメージング質量分析法を用いたデキサメタゾン投与によるマウス胸腺を主軸とする免疫代謝変動の解明 / ゼンシン イメージング シツリョウ ブンセキホウ オ モチイタ デキサメタゾン トウヨ ニヨル マウス キョウセン オ シュジク トスル メンエキ タイシャ ヘンドウ ノ カイメイ

辻 雄大, Yudai Tsuji

22 March 2022

博士(理学) / Doctor of Philosophy in Science / 同志社大学 / Doshisha University

胸腺

デキサメタゾン

質量分析イメージング

メタボロミクス

免疫

thymus

dexamethasone

mass spectrometry imaging

UMAP

metabolomics

immunity

Tolérance au soi : rôle des éléments transposables dans les tissus somatiques et le thymus

Larouche, Jean-David

08 1900

Les éléments transposables (TE) sont des séquences répétitives représentant environ 45% des génomes humain et murin. Il est généralement assumé que leur expression est réprimée dans les cellules somatiques pour protéger l’intégrité du génome, et cette régulation épigénétique est fréquemment perdue dans les cancers, menant à la surexpression des TEs dans les tumeurs. Puisque l’expression aberrante des TEs est associée à l’infiltration de la tumeur par les cellules immunitaires, les TEs sont considérés comme des cibles prometteuses d’immunothérapies du cancer. Une meilleure description de l’expression des TEs dans les tissus somatiques ainsi que dans le thymus, l’organe responsable du développement de la tolérance au soi des lymphocytes T, est toutefois nécessaire pour évaluer la capacité des TEs d’induire des réponses immunitaires et déterminer si l’expression des TEs est belle et bien spécifique aux tumeurs. L’objectif de cette thèse est donc de brosser un portrait exhaustif de l’expression des TEs dans les tissus somatiques humains ainsi que dans le thymus. Pour ce faire, des données transcriptomiques et immunopeptidomiques ont été analysées pour mieux comprendre les interactions entre les TEs et les lymphocytes T à l’état basal. Nos résultats ont montré que l’expression des TEs est répandue dans les tissus somatiques humains, bien que leur niveau d’expression varie d’un tissu à l’autre et que plusieurs TEs sont exprimés de façon tissu-spécifique. De plus, les TEs peuvent être traduits et présentés par le CMH-I à la surface de cellules non-cancéreuses. Nous avons aussi déterminé que les TEs ont trois fonctions potentielles dans le thymus : ils pourraient fournir des sites de liaison à un grand nombre de facteurs de transcription dans toutes les populations cellulaires du thymus, ils stimuleraient la sécrétion d’IFN ɑ/β par les pDCs thymiques, et ils contribuent aux sélections positive et négative des thymocytes. Nos travaux illustrent la complexité des interactions entre les TEs et le système immunitaire adaptatif. Finalement, étant donnée l’expression répandue des TEs dans les tissus somatiques, nos travaux soulignent l’importance d’établir la tolérance des lymphocytes T à l’égard des TEs pour éviter des réactions auto-immunes. / Transposable elements are repetitive sequences representing around 45% of the human and murine genomes. It is generally assumed that their expression is repressed in somatic cells to preserve genomic integrity, but this epigenetic regulation is frequently lost in cancer cells, leading to the aberrant expression of TEs in tumors. As aberrant TE expression is associated with tumor infiltration by immune cells, TEs are considered as promising cancer immunotherapy targets. However, a better description of TE expression in somatic tissues and in the thymus, the organ responsible of T cell self-tolerance induction, is required to evaluate the potential of TEs to induce immune responses as well as the tumor specificity of TE expression. Thus, this thesis’ objective is to draw an exhaustive profile of TE expression in human somatic tissues and in the thymus. To do so, we analyzed transcriptomic and immunopeptidomic data to better understand interactions between TEs and T cells at steady state. Our work shows that TE expression is widespread in human somatic tissues, even though their expression level varies between tissues and many TEs are expressed in a tissue-specific manner. Additionally, TEs are translated and presented by the MHC-I on the surface of non-malignant cells. We also determined that TEs have three potential functions in the thymus: they could provide transcription factor binding sites in all cell populations of the thymus, they might induce the constitutive IFN ɑ/β secretion of thymic pDCs, and they contribute to both positive and negative selections of thymocytes. Altogether, our work illustrates the complexity of the interactions between TEs and the vertebrate adaptive immune system. Given the widespread expression of TEs in somatic tissues, this thesis highlights the importance of establishing T cell tolerance towards TE sequences to avoid autoimmune reactions in peripheral tissues.

Éléments transposables

Peptides associés au CMH-I

Thymus

Immunologie

Transcriptomique

Transposable elements

MHC I-associated peptides

Immunology

Transcriptomics

Imunorregulação central e periférica em pacientes com Síndrome de Down e autoimunidade / Central and peripheral immunoregulation in patients with Down syndrome and autoimmunity

Ribeiro, Luciana Maria de Andrade

24 November 2011

Introdução: A Síndrome de Down (SD) é uma doença genética de alta prevalência, com várias alterações imunológicas decorrentes da disfunção tímica associada à doença. Neste estudo, avaliou-se a associação entre presença de autoimunidade e disfunção do timo em pacientes com SD. Métodos: Foram avaliados 22 pacientes com SD (11 com autoimunidade e 11 sem), que preenchiam os critérios de inclusão: diagnóstico clinico e genético, idade > a 10 anos e sem uso de drogas imunossupressoras. Estes pacientes foram comparados a um grupo controle formado por adolescentes saudáveis (n=11) e outro de pacientes com doenças autoimunes, caracterizados por manifestações clínicas e presença de autoanticorpos (n=11). Todos os grupos foram pareados por idade e sexo. Os parâmetros laboratoriais avaliados foram: número de leucócitos, linfócitos CD3+, CD4+, CD8+, CD19+, CD21+, CD4+CD28null , células T reguladoras (CD4+CD25+Foxp3+), linfócitos T naive (CD4+CD45RA+CD62L+) e linfócitos T de memória (CD4+CD45RO+CD62L- ) e célula NK (CD3-CD16+, CD56+) por citometria de fluxo, Foi também avaliada a concentração de sjTREC (T receptor excision circles) em sangue total por qRT-PCR .Resultados: Nos pacientes com SD, observou-se redução das concentrações séricas de sjTREC, do número de linfócitos B e aumento do número de células CD4+CD28null. Na análise concomitante entre os grupos formados (SD com e sem autoimunidade, controle e autoimunidade sem SD), após correção de Bonferroni, observou-se que o grupo SD com autoimunidade apresentou redução de linfócitos T CD4, linfócitos naive e linfócitos B. Quando comparados os grupos SD com e sem autoimunidade observou-se redução significativa das concentrações de TREC no primeiro grupo. Não houve alterações das Células NK. Em valores percentuais, os pacientes com SD e autoimunidade apresentaram elevação da subpopulação de células T reguladoras. Conclusões: Este estudo mostra que pacientes com SD apresentam disfunção tímica quando avaliados pela quantificação de concentrações de TREC, sendo esta última mais expressiva nos pacientes com SD e autoimunidade. A redução dos linfócitos T naive associada a número normal de linfócitos T de memória sugere disfunção tímica primária, não compatível com processo de senescência. A observação do aumento do número de linfócitos CD4+CD28null poderia ser consequência de múltiplos estímulos celulares provavelmente em consequência da linfopenia observada. A elevação de células Treg em pacientes com SD e autoimunidade poderia ser decorrente de alterações funcionais destas células bem como de alterações nos processos de homeostase / Introduction: Down syndrome (DS) is a genetic disease of high prevalence, with many immunological alterations as a consequence of thymic disfunction associated to this disease. In this study, it was evaluated the association between the presence of thymic disfunction and autoimmunity in patients with DS. Methods: It was evaluated 22 patients with DS (11 with and 11 without autoimmunity) who fulfilled the inclusion criteria: clinical and genetic diagnosis, and age >10 years and no use of immunosuppressive drugs. These patients were compared to a control group composed by health adolescents (n=11) and patients with autoimmune diseases, characterized by clinical manifestations and autoantibodies (n=11). All groups were matched for age and sex. The laboratory parameters evaluated were: number of leukocytes, CD3+, CD4+, CD8+, CD19+, CD4+CD28null lymphocytes, regulatory T cells (CD4+CD25+Foxp3+), naive T lymphocytes (CD4+CD45RA+CD62L+), memory T lymphocytes (CD4+CD45RO+CD62L-) and NK cells (CD3-CD16+CD56+). The subpopulations of lymphocytes were determined by flow cytometry. It was also evaluated whole blood sjTREC (T receptor excision circles) concentrations by PCR. Results: In DS patients, there was reduction of sjTREC concentration, B lymphocytes number and increase of CD4+CD28null cells number. When compared all the groups formed (SD with and without autoimmunity, autoimmunity without SD and control group), after Bonferroni correction, the SD group with autoimmunity showed a reduction of T CD4+lymphocytes, naïve cells and B lymphocytes. When SD with and without autoimmunity groups were compared it was observed significant reduction in the TREC concentrations in the first group. There were no changes in NK cells. Patients with DS and autoimmune diseases had huge percentages of T reg cells comparing different groups. Conclusions: This study showed that DS patients presented thymic disfunction by reduced levels of whole blood sjTREC, and this condition is more expressive to patients with DS and autoimmune disease associated. The reduction of TCD4+ naïve cells with normal TCD4+ memory cells is suggestive of primary thymic disfunction against a senescent process. The elevated number of CD4+CD28null in DS patients probably was a consequence of reduced T cell numbers. The elevation of Treg cells remains unclear, and coud be a result of ineffective cells or deregulation of Thymus dependent immunity

Autoimmunity

Autoimunidade

Down Syndrome

Síndrome de Down

Sub-populações de linfócitos T

T-lymphocyte subsets

Thymus gland/abnormalities

Thymus gland/immunology

Timo/anormalidades

Timo/imunologia

Imunorregulação central e periférica em pacientes com Síndrome de Down e autoimunidade / Central and peripheral immunoregulation in patients with Down syndrome and autoimmunity

Luciana Maria de Andrade Ribeiro

24 November 2011

Introdução: A Síndrome de Down (SD) é uma doença genética de alta prevalência, com várias alterações imunológicas decorrentes da disfunção tímica associada à doença. Neste estudo, avaliou-se a associação entre presença de autoimunidade e disfunção do timo em pacientes com SD. Métodos: Foram avaliados 22 pacientes com SD (11 com autoimunidade e 11 sem), que preenchiam os critérios de inclusão: diagnóstico clinico e genético, idade > a 10 anos e sem uso de drogas imunossupressoras. Estes pacientes foram comparados a um grupo controle formado por adolescentes saudáveis (n=11) e outro de pacientes com doenças autoimunes, caracterizados por manifestações clínicas e presença de autoanticorpos (n=11). Todos os grupos foram pareados por idade e sexo. Os parâmetros laboratoriais avaliados foram: número de leucócitos, linfócitos CD3+, CD4+, CD8+, CD19+, CD21+, CD4+CD28null , células T reguladoras (CD4+CD25+Foxp3+), linfócitos T naive (CD4+CD45RA+CD62L+) e linfócitos T de memória (CD4+CD45RO+CD62L- ) e célula NK (CD3-CD16+, CD56+) por citometria de fluxo, Foi também avaliada a concentração de sjTREC (T receptor excision circles) em sangue total por qRT-PCR .Resultados: Nos pacientes com SD, observou-se redução das concentrações séricas de sjTREC, do número de linfócitos B e aumento do número de células CD4+CD28null. Na análise concomitante entre os grupos formados (SD com e sem autoimunidade, controle e autoimunidade sem SD), após correção de Bonferroni, observou-se que o grupo SD com autoimunidade apresentou redução de linfócitos T CD4, linfócitos naive e linfócitos B. Quando comparados os grupos SD com e sem autoimunidade observou-se redução significativa das concentrações de TREC no primeiro grupo. Não houve alterações das Células NK. Em valores percentuais, os pacientes com SD e autoimunidade apresentaram elevação da subpopulação de células T reguladoras. Conclusões: Este estudo mostra que pacientes com SD apresentam disfunção tímica quando avaliados pela quantificação de concentrações de TREC, sendo esta última mais expressiva nos pacientes com SD e autoimunidade. A redução dos linfócitos T naive associada a número normal de linfócitos T de memória sugere disfunção tímica primária, não compatível com processo de senescência. A observação do aumento do número de linfócitos CD4+CD28null poderia ser consequência de múltiplos estímulos celulares provavelmente em consequência da linfopenia observada. A elevação de células Treg em pacientes com SD e autoimunidade poderia ser decorrente de alterações funcionais destas células bem como de alterações nos processos de homeostase / Introduction: Down syndrome (DS) is a genetic disease of high prevalence, with many immunological alterations as a consequence of thymic disfunction associated to this disease. In this study, it was evaluated the association between the presence of thymic disfunction and autoimmunity in patients with DS. Methods: It was evaluated 22 patients with DS (11 with and 11 without autoimmunity) who fulfilled the inclusion criteria: clinical and genetic diagnosis, and age >10 years and no use of immunosuppressive drugs. These patients were compared to a control group composed by health adolescents (n=11) and patients with autoimmune diseases, characterized by clinical manifestations and autoantibodies (n=11). All groups were matched for age and sex. The laboratory parameters evaluated were: number of leukocytes, CD3+, CD4+, CD8+, CD19+, CD4+CD28null lymphocytes, regulatory T cells (CD4+CD25+Foxp3+), naive T lymphocytes (CD4+CD45RA+CD62L+), memory T lymphocytes (CD4+CD45RO+CD62L-) and NK cells (CD3-CD16+CD56+). The subpopulations of lymphocytes were determined by flow cytometry. It was also evaluated whole blood sjTREC (T receptor excision circles) concentrations by PCR. Results: In DS patients, there was reduction of sjTREC concentration, B lymphocytes number and increase of CD4+CD28null cells number. When compared all the groups formed (SD with and without autoimmunity, autoimmunity without SD and control group), after Bonferroni correction, the SD group with autoimmunity showed a reduction of T CD4+lymphocytes, naïve cells and B lymphocytes. When SD with and without autoimmunity groups were compared it was observed significant reduction in the TREC concentrations in the first group. There were no changes in NK cells. Patients with DS and autoimmune diseases had huge percentages of T reg cells comparing different groups. Conclusions: This study showed that DS patients presented thymic disfunction by reduced levels of whole blood sjTREC, and this condition is more expressive to patients with DS and autoimmune disease associated. The reduction of TCD4+ naïve cells with normal TCD4+ memory cells is suggestive of primary thymic disfunction against a senescent process. The elevated number of CD4+CD28null in DS patients probably was a consequence of reduced T cell numbers. The elevation of Treg cells remains unclear, and coud be a result of ineffective cells or deregulation of Thymus dependent immunity

Autoimunidade

Síndrome de Down

Sub-populações de linfócitos T

Timo/anormalidades

Timo/imunologia

Autoimmunity

Down Syndrome

T-lymphocyte subsets

Thymus gland/abnormalities

Thymus gland/immunology

Febre reumática: quantificação de fragmentos circulares excisados pelo rearranjo do receptor da célula T em linfócitos T de sangue periférico / Quantification of T cell receptor excision circles in peripheral blood of rheumatic fever patients

Santos, Nathália Moreira

24 October 2013

Há um amplo espectro de doenças causadas por estreptococos do grupo A (GAS), e são consideradas um problema de saúde pública em vários países, principalmente os em desenvolvimento, com aproximadamente 600 milhões de casos/ano. As infecções causadas por GAS podem ocasionar doenças invasivas como faringite e pioderma com seqüelas auto-imunes graves como a febre reumática (FR) e glomerulonefrite. A FR acomete principalmente crianças e jovens adultos. A FR apresenta diversas manifestações, sendo a doença reumática cardíaca (DRC) a seqüela mais grave, caracterizada por lesões cardíacas valvares progressivas e permanentes. O tratamento, frequentemente envolve cirurgia cardíaca para a correção de lesões valvulares, o que acarreta alto custo para o Sistema Único de Saúde no Brasil e em vários países. Em trabalhos anteriores sobre os mecanismos desencadeadores das lesões reumáticas no coração, foi possível identificar o papel do linfócito T como mediador principal da autoimunidade, através da análise do receptor de células T infiltrantes de lesão cardíaca de indivíduos com DRC. Várias expansões oligoclonais com diferentes tamanhos da região que reconhece o antígeno, CDR3 foram encontradas. No presente trabalho, analisou-se a atividade tímica através da quantificação de fragmentos circulares excisados pelo rearranjo do gene do receptor do linfócito T (TREC) em linfócitos T de sangue periférico de indivíduos com FR e DRC. Também foi avaliada a presença de células T naïve e de memória através de citometria de fluxo. Os resultados do presente trabalho mostraram que a quantidade de TREC em amostras de sangue periférico do grupo de pacientes com FR/DRC foi significantemente menor quando comparada a observada em indivíduos saudáveis. Interessantemente, em ambos os grupos a quantidade de TREC apresentou correlação negativa com a idade dos indivíduos estudados. Os resultados indicaram diferenças na atividade tímica em pacientes com FR/DRC, provavelmente decorrente do processo autoimune que envolve linfócitos T / There is a wide spectrum of diseases caused by group A streptococci (GAS), that still being considered a public health problem in developing countries, with about 600 million cases per year. Infections by GAS can cause invasive diseases such as pharyngitis and pyoderma leading to serious autoimmune complications such as rheumatic fever (RF) and glomerulonephritis. RF mainly affects children and young adults, and presents different manifestations. Rheumatic heart disease (RHD) is considered the most serious complication leading to valvular lesions that are characterized by progressive and permanent heart damage, which entails high cost to the Public Health System in Brazil and worldwide. In previous works that focused on the mechanisms leading to rheumatic heart lesions, we identified the role of T lymphocytes as principal mediator of autoimmune reactions. Through the in deep analysis of infiltrating T-cell receptor repertoire of patients with RHD, we identified oligoclonal expansions with different sizes of CDR3 that is the region of antigen recognition. In the present study we analyzed the thymic activity through T cell receptor excision circles (TREC) quantification in T cells from peripheral blood of RF/RHD patients. We also evaluated naïve and memory T cells from peripheral blood by flow cytometry. Our results showed that the amount of TREC in the peripheral blood of patients was significantly lower when compared to the healthy individuals. In addition, both groups showed that the amount of TREC is negatively correlated with age. These results indicated that the thymic activity in RF/RHD patients is altered probably due to the autoimmune process that involves T lymphocytes

Autoimmunity

Autoimunidade

Cardiopatia reumática/imunologia

Febre reumática/imunologia

Genes T-cell receptor beta

Linfócitos T

Rheumatic fever/immunology

Rheumatic heart disease/immunology

Streptococcus pyogenes

Streptococcus pyogenes

Thymus gland/physiology

Thymus gland/immunology

Timo/fisiologia

Timo/imunologia

TLymphocytes

Febre reumática: quantificação de fragmentos circulares excisados pelo rearranjo do receptor da célula T em linfócitos T de sangue periférico / Quantification of T cell receptor excision circles in peripheral blood of rheumatic fever patients

Nathália Moreira Santos

24 October 2013

Há um amplo espectro de doenças causadas por estreptococos do grupo A (GAS), e são consideradas um problema de saúde pública em vários países, principalmente os em desenvolvimento, com aproximadamente 600 milhões de casos/ano. As infecções causadas por GAS podem ocasionar doenças invasivas como faringite e pioderma com seqüelas auto-imunes graves como a febre reumática (FR) e glomerulonefrite. A FR acomete principalmente crianças e jovens adultos. A FR apresenta diversas manifestações, sendo a doença reumática cardíaca (DRC) a seqüela mais grave, caracterizada por lesões cardíacas valvares progressivas e permanentes. O tratamento, frequentemente envolve cirurgia cardíaca para a correção de lesões valvulares, o que acarreta alto custo para o Sistema Único de Saúde no Brasil e em vários países. Em trabalhos anteriores sobre os mecanismos desencadeadores das lesões reumáticas no coração, foi possível identificar o papel do linfócito T como mediador principal da autoimunidade, através da análise do receptor de células T infiltrantes de lesão cardíaca de indivíduos com DRC. Várias expansões oligoclonais com diferentes tamanhos da região que reconhece o antígeno, CDR3 foram encontradas. No presente trabalho, analisou-se a atividade tímica através da quantificação de fragmentos circulares excisados pelo rearranjo do gene do receptor do linfócito T (TREC) em linfócitos T de sangue periférico de indivíduos com FR e DRC. Também foi avaliada a presença de células T naïve e de memória através de citometria de fluxo. Os resultados do presente trabalho mostraram que a quantidade de TREC em amostras de sangue periférico do grupo de pacientes com FR/DRC foi significantemente menor quando comparada a observada em indivíduos saudáveis. Interessantemente, em ambos os grupos a quantidade de TREC apresentou correlação negativa com a idade dos indivíduos estudados. Os resultados indicaram diferenças na atividade tímica em pacientes com FR/DRC, provavelmente decorrente do processo autoimune que envolve linfócitos T / There is a wide spectrum of diseases caused by group A streptococci (GAS), that still being considered a public health problem in developing countries, with about 600 million cases per year. Infections by GAS can cause invasive diseases such as pharyngitis and pyoderma leading to serious autoimmune complications such as rheumatic fever (RF) and glomerulonephritis. RF mainly affects children and young adults, and presents different manifestations. Rheumatic heart disease (RHD) is considered the most serious complication leading to valvular lesions that are characterized by progressive and permanent heart damage, which entails high cost to the Public Health System in Brazil and worldwide. In previous works that focused on the mechanisms leading to rheumatic heart lesions, we identified the role of T lymphocytes as principal mediator of autoimmune reactions. Through the in deep analysis of infiltrating T-cell receptor repertoire of patients with RHD, we identified oligoclonal expansions with different sizes of CDR3 that is the region of antigen recognition. In the present study we analyzed the thymic activity through T cell receptor excision circles (TREC) quantification in T cells from peripheral blood of RF/RHD patients. We also evaluated naïve and memory T cells from peripheral blood by flow cytometry. Our results showed that the amount of TREC in the peripheral blood of patients was significantly lower when compared to the healthy individuals. In addition, both groups showed that the amount of TREC is negatively correlated with age. These results indicated that the thymic activity in RF/RHD patients is altered probably due to the autoimmune process that involves T lymphocytes

Autoimunidade

Cardiopatia reumática/imunologia

Febre reumática/imunologia

Linfócitos T

Streptococcus pyogenes

Timo/fisiologia

Timo/imunologia

Autoimmunity

Genes T-cell receptor beta

Rheumatic fever/immunology

Rheumatic heart disease/immunology

Streptococcus pyogenes

Thymus gland/physiology

Thymus gland/immunology

TLymphocytes

Farmakološki efekti sirupa i tinkture timijana / Pharmacological effects of thyme syrup and tincture

Kvrgić Maja

21 September 2016

<p>Poslednjih godina je prisutan trend povratka prirodi i upotrebi biljnih lekova, kako u prevenciji tako i u lecenju razlicitih bolesti. Timijan (Thymus vulgaris L.) se u narodnoj medicini koristio u lecenju respiratornih oboljenja kao &scaron;to su ka&scaron;alj, bronhitis i astma. Rezultati novijih istraživanja pokazuju da timijan poseduje i druga potencijalno korisna farmakolo&scaron;ka svojstva (antimikrobna, antiinflamatorna, antioksidativna, spazmoliticka, antidijabetesna i anksioliticka). Ciljevi ovog istraživanja su bili da se ispitaju farmakodinamske osobine preparata timijana, njihove interakcije sa lekovima koji deluju na centralni nervni sistem, uticaj na funkciju jetre i parametrem oksidativnog stresa kod životinja izloženih ugljentetrahloridu, kao sadržaj karvakrola i timola u sirupu timijna, pri razlicitim uslovima cuvanja. U farmakodinamskim ispitivanjima kao eksperimentalne životinje kori&scaron;ceni su mi&scaron;evi soja NMRI, a u svim drugim ispitivanjima pacovi soja Wistar. Tinktura timijana je primenjena u dozi od 0,4mk/kg, a sirup u dozi od 12,08 ml/kg, na mi&scaron;evima. Primenjene doze na pacovima su bile 0,18 ml/kg za tinkturu i 5,6 ml/kg za sirup timijana. Za ispitivanje analgetickog dejstva kori&scaron;ceni su metod vrele ploce i test sircetne kiseline. Za procenu motorne koordinacije kori&scaron;cen je test rotirajuceg &scaron;tapa, a za procenu hipnotickog delovanja mereno je vreme spavanja. Prilikom ispitivanja uticaja preparata timijana na farmakokinetiku paracetamola, odre_ivana je koncentracija ovog leka HPLC metodom, a nakon toga su odreeni farmakokinetski parametri paracetamola. Antioksidantna aktivnost preparata timijana odre_ivana je pomocu in vitro i in vivo testova. Nakon žrtvovanja životinja ra_ena je histopatolo&scaron;ka analiza jetrenog tkiva, a u serumu su odre_ivani biohemijski parametri, kao i pokazatelji bubrežene i jetrene funkcije. Sadržaj timola i karvakrola i sirupu timijana odre_en je GC/MS metodom. Sirup i tinktura timijana su pokazali analgeticki efekat u testu vrele ploce, kao i smanjenje broja grceva izazvano primenom sircetne kiseline. Sedmodnevna primena preparata timijana smanjila je analgeticko dejstvo kodeina, a pojacala analgeticki efekat paracetamola. Sirup timijana je potencirao diazepamom izazvan poremecaj motorne koordinacije. Ispitivanjem uticaja preparata timijana na hipnoticko delovanje pentobarbitala, postignuti su razliciti rezultati u zavisnosti od dužine trajanja pretremana. Sedmodnevna primena timijana je produžila vreme trajanja spavanja, dok je jednokratna primena timijana skratila vreme trajanja spavanja. Nakon i intravenske i peroralne primene paracetamola, grupe životinja koje su bile pretretirane preparatima timijana imale su krace poluvreme eliminacije i vecu konstantu eliminacije. Upotreba samo preparata timijana nije imala uticaj na biohemijske i histolo&scaron;ke promene jetrene funkcije. S druge strane, upotreba tincture timijana u kombinaciji sa ugljen-tetrahloridom dovela je do porasta vrednosti AST i ALT enzima u serumu, dok je sirup timijana u kombinaciji sa ugljentetrahloridom smanjio aktivnost aminotransferaza. Najvece odstupanje u koncentracijama aktivnih komponenti timola i karavkrola, pokazali su sirupi cuvani na sobnoj temperaturi (20&deg;C), u sekundarnoj ambalaži i na svetlom mestu. Rezultati dobijeni u toku ovog istraživanja ukazuju da preparati timijana uticu na farmakodinamske osobine kodeina, paracetamola, diazepama i pentobarbitala, kao i na farmakokinetiku paracetamola. Upotreba preparata timijana ispoljila je analgeticki efekat i umanjila posledice izloženosti oksidativnom stresu. Uslovi cuvanja sirupa timijana uticali su na njegovu stabilnost.</p> / <p>In recent years is present trend of return to nature and the use of herbal medicines in prevention and treatment of different diseases. Thyme (Thymus vulgaris L.) was used in folk medicine in the treatment of respiratory diseases such as cough, bronchitis and asthma. The new research results have demonstrated that thyme has many others potentially useful pharmacological properties (antimicrobial, antiinflammatory, antioxidant, antispasmodic, antidiabetic and anxiolytic). The aims of this research were to determine the pharmacodynamic properties of thyme preparations and their interactions with central nervous system drugs, influence on liver function and oxidative stress parameters of animals exposed to carbon tetrachloride, as well as concentration of thymol and carvacrol in thyme syrup, at different storage conditions. In pharmacodynamics examination as experimental animals were used NMRI mice, while in all other test were used Wistar rats. Applied dose of thyme tincture was 0.4 ml/kg and of syrup 12.08 ml/kg, for mice. For rats, applied doses of tincture and syrup were 0.18 ml/kg and 5.6 ml/kg, respectively. The analgesic activity was examined by the hot plate test and acetic acid test. The Rotarod test was used to evaluate the motor coordination and to evaluate hypnotic activity sleeping time was mesaured. In order to examine the influence of thyme preparations on pharmacokinetics of paracetamol, the concentracion of this drug was measured by HPLC metods, and after that pharmocokinetic parameters of paracetamol were determined.The antioxidant acivity of thyme preparations was determined by using in vitro and in vivo tests. After animals sacrificing, histopathological analysis of liver tissue were peroformed, in serum were determined biochemical parameters and renal and hepatic function parameters. Quantification of thymol and carvacrol in syrup was carried out by GC/MS method. Thyme syrup and thyme tincture exhibited analgesic activity in hot plate test and reduced the number of writhes induced by acetic acid. Seven-day pretreatment with thyme preparations reduced analgesic activity of codeine and increased analgesic effect of paracetamol. Thyme syrup potentiated diazepam induced motor coordination impairment. Examining the impact of thyme preparations on hypnotic effect induced by pentobarbital, different results were achieved depending on the duration of pretreatment. Seven-day pretreatment with thyme had prolonged the sleeping time, while after single dose of thyme the sleeping time was decreased. After intravenous and after oral administration of paracetamol, groups pretreated with thyme preparations had decreased elimination half-life and increased elimination constant rate. Administration of thyme preparations alone did not change biochemical nor histological markers of hepatic function. On the other hand, co-administration of thyme tincture and carbon tetrachloride resulted in exacerbation of AST and ALT values in serum, while thyme syrup in coadministration with carbon tetrachloride managed to reduce activities of aminotransferases. The concentration of major active compounds, thymol and carvacrol, was mostly changed when syrups were stored at room temperature (20&deg;C), in secondary containers and in light place. Results obtained in this study demonstrated that thyme preparations do affect pharmacodynamic properties of codeine, paracetamol, diazepam and pentobarbital and pharmacokinetics of paracetamol. Administration of thyme preparations exhibited analgesic activity and reduced the effects of exposure to oxidative stress. Storage conditions of thyme syrup did affect its stability.</p>

Avaliação da função tímica em pacientes com diabetes mellitus tipo 1 submetidos ao transplante autólogo de células-tronco hematopoéticas / Evaluation of thymic function in type 1 diabetes mellitus patients following autologous hematopoietic stem cell transplantation.

Azevedo, Júlia Teixeira Cottas de

19 August 2013

O diabetes mellitus tipo 1 (DM-1) é uma doença autoimune órgão-específica caracterizada pela destruição seletiva das células pancreáticas produtoras de insulina. A imunossupressão em altas doses seguida do transplante autólogo de células-tronco hematopoéticas (TACTH) constitui uma alternativa terapêutica recente e promissora para o DM-1 recém-diagnosticado, impedindo a progressão da destruição das células pancreáticas produtoras de insulina e induzindo independência insulínica por um período prolongado na maioria dos pacientes. O princípio dessa terapia baseia-se na eliminação das células autorreativas pela imunossupressão intensa e na reconstituição de um sistema imunológico novo e tolerante após o transplante. Com o objetivo de avaliar a função do timo e sua contribuição na geração do repertório de células T nos pacientes com DM-1 após o TACTH, nesse trabalho foram avaliados os níveis de T cell receptor excision circles (TRECs) em células T do sangue periférico e a diversidade do repertório de células T dos pacientes com DM-1 (n=23) antes e em diversos períodos após o transplante. A quantificação absoluta dos níveis de TRECs (número de moléculas de TRECs/100g de DNA) foi realizada pela técnica de PCR em tempo real e a avaliação do repertório de células T foi realizada pela técnica de TCRBV CDR3 Spectratyping. Dentre os vinte e três pacientes, vinte alcançaram a independência insulínica por períodos variáveis de tempo e três não responderam ao tratamento. Não foi observada a restrição do repertório de células T nos pacientes com DM-1 no período pré-transplante, ou seja, quando recém-diagnosticados. Foram identificadas cinco famílias V (7, 18, 19, 20 e 22) em expansão clonal nos pacientes com DM-1. As famílias V 7, 18, 19, 20 apresentaram-se em expansão clonal antes do transplante e se mantiveram com frequência elevada após o transplante, enquanto a família V 22 apresentou aumento da frequência somente nos períodos mais tardios após o transplante. Nos primeiros meses após o transplante, houve redução do número de moléculas de TRECs e restrição do repertório de células T. Contudo, um ano após o transplante, o número de moléculas de TRECs atingiram valores normais e o repertório de células T apresentou-se com ampla diversidade. Nossos resultados mostraram que o TACTH foi capaz de induzir mudanças na composição do repertório de células T dos pacientes com DM-1 após a terapia de IAD/TACTH, evidenciadas por alterações qualitativas e quantitativas dos picos de CDR3 do TCR, sugerindo a reconstituição de um repertório de células T diverso até dois anos pós-transplante. Embora tenha ocorrido reativação da função tímica após o transplante, evidenciada pelo aumento dos níveis de TRECs de um ano e meio a cinco anos pós-transplante, a diversidade do repertório das células T diminuiu a partir de dois anos e meio pós-transplante, sugerindo uma reconstituição tímica de novo de células T naive que expressam preferencialmente algumas cadeias V. Estas evidências imunológicas poderiam explicar a melhora clínica (independência insulínica) temporária observada na maioria dos pacientes após a terapia de IAD/TACTH. / Type 1 diabetes mellitus (T1D) is an organ-specific autoimmune disease characterized by insulin-producing pancreatic cell destruction. High-dose immunosuppression followed by autologous hematopoietic stem cell transplantation (AHSCT) is a recent and promising therapeutic approach for treatment of T1D, preventing the progress of destruction of pancreatic cells and inducing insulin independence for a prolonged period in most patients. The rationale of the AHSCT is based on the elimination of autoreactive cells by the intense immunosuppression and on the reconstitution of a new and tolerant immune system after transplantation. Aiming at assessing the thymic role in the production of new T cell repertoire in T1D patients after AHSCT, in this study was evaluated the levels of T cell receptor excision circles (TRECs) in T cells of peripheral blood as well as the clonality and diversity of T cell repertoire in T1D patients (n=23) before and several periods after transplantation. The absolute quantification of TRECs levels (number of molecules of TRECs/100ng of DNA) was performed by real-time PCR and the analysis of T cell repertoire was performed by TCRBV CDR3 Spectratyping. Among the twenty-three patients, twenty achieved insulin independence for variable periods and three did not respond to the treatment. The T cell repertoire in T1D patients was not restricted in pre-transplantation, i.e., when newly diagnosed. It was identified five V families (7, 18, 19, 20 e 22) in the clonal expansion in T1D patients. The V families 7, 18, 19, 20 were in clonal expansion before transplantation and maintained with high frequency after transplantation, whereas the V 22 family increased its frequency only in the later periods after transplantation. It was observed that the numbers of molecules of TRECs decreased and the T cell repertoire was restricted in the early months after transplantation. However, the levels of TRECs were normalized and the T cell repertoire showed diversity one year after transplantation. Our results indicate that AHSCT was able to induce changes in the composition of the T cell repertoire of patients after AHSCT, evidenced by qualitative and quantitative changes in the composition of T-cell receptor -chain CDR3 peaks, suggesting the reconstitution of diverse T cell repertoire up to two years after transplantation. Although there was reactivation of thymic function after transplantation, as evidenced by increased levels of TRECs from one and a half year to five years after transplantation, the diversity of the T cells repertoire decreased from two and a half years after transplantation, suggesting a reconstruction of new naive T cells that preferentially express some V chains. These immunological evidences could explain the temporary clinical improvement (insulin independence) observed in most patients after IAD / AHSCT therapy.

CDR3

CDR3

Diabetes mellitus tipo 1

Immune reconstitution

Receptor de célula T

Reconstituição imunológica

T cell receptor

Thymus

Timo

TREC.

TREC.

Type 1 Diabetes mellitus