Analysen zur differentiellen Plasmazellhomöostase beim Menschen

Mei, Henrik Eckhard

05 January 2010

Das humorale Immungedächtnis wird von reifen Plasmazellen des Knochenmarks vermittelt, welche bei Immunreaktionen aus aktivierten B-Lymphozyten gebildet werden. Dabei sind im Blut Plasmablasten als unmittelbare Vorläufer der Plasmazellen nachweisbar, die von dort aus in das Knochenmark einwandern. Anhand der durchflusszytometrischen Detektion spezifischer Plasmablasten gelang es hier, das simultane Auftauchen von Wellen neu generierter, migratorischer Plasmablasten und reifer, nicht-migratorischer Plasmazellen im Blut eine Woche nach einer Tetanusimpfung nachzuweisen. Plasmablasten und Plasmazellen lagen stets im Gleichgewicht vor, wodurch auf die stöchiometrische Mobilisierung reifer Plasmazellen des Knochenmarks durch systemisch induzierte Plasmablasten geschlossen wurde. Ein solcher Verdrängungsmechanismus wird hier erstmalig als Anpassungsmechanismus des humoralen Immungedächtnisses dargestellt, der die Aufnahme neuer Spezifitäten in das Gedächtnis unter Wahrung der Stabilität präexistierender Spezifitäten erlaubt. Anders als systemisch induzierte Plasmablasten, weisen Plasmablasten, die im immunologischen Ruhephase zirkulieren, Kennzeichen mukosaler Immunreaktionen auf: sie exprimieren IgA sowie die mukosalen Zellmigrationsrezeptoren alpha4beta7-Integrin und CCR10. Wahrscheinlich wandern sie in mukosale Plasmazelldepots ein und interferieren nicht mit den Plasmazellen des Knochenmarks, sodass die Stabilität des humoralen Gedächtnisses in der Ruhephase gewahrt bleibt. Eine Anpassung des humoralen Gedächtnisses findet somit nur im Rahmen systemischer Immunreaktionen statt. Bei splenektomierten Patienten und unter der B-Zell-Depletionstherapie bei Rheumapatienten bleiben mukosale Plasmablasten im Blut nachweisbar. Dies belegt deren autonome Bildung aus mukosalen, therapie-refraktären B-Zellen. Insgesamt wird hier eine bisher unbeachtete Komplexität menschlicher peripherer Plasmablasten und Plasmazellen und ihren Beziehungen zum humoralen Immungedächtnis dargestellt. / Humoral memory, i.e. persistence of specific antibody titers, is provided by plasma cells in the bone marrow, which are generated from activated B cells during immune responses. At this, immediate plasma cell precursors, the plasmablasts, migrate via the blood to the bone marrow. Using cytometric detection of antigen-specific plasmablasts, synchronous circulation of waves of recently generated, migratory plasmablasts and non migratory plasma cells with a mature phenotype was demonstrated one week after tetanus vaccination. Circulating plasmablast and plasma cell numbers were always in homeostasis, so that the stoichiometric mobilization of old bone marrow plasma cells by recently generated plasmablasts was hypothesized. This plasma cell replacement mechanism is herein described for the first time as an adaption mechanism of the humoral memory that allows incorporation of new antibody specificities while maintaining pre-existing ones. In immunological steady state, very low numbers of plasmablasts are detectable in any donor. These express IgA and receptors for mucosal homing, alpha4beta7 integrin and CCR10, and therefore most likely migrate into mucosal plasma cell depots and do not interfere with plasma cells of the bone marrow, preserving the stability of humoral memory during steady state. Hence, adaption of humoral memory is only possible during systemic immune reactions. Circulating mucosal plasmablasts produced during steady state remain detectable in patients with rheumatoid arthritis during B cell depletion therapy as well as in asplenic patients. Hence, this type of plasmablasts is self-sufficiently generated from mucosal B cells that are refractory to B cell depletion therapy. This work demonstrates a hitherto disregarded complexity of peripheral plasmablast and plasma cell subsets in healthy humans, with implications for the regulation of induction and maintenance of humoral memory.

Antikörper

Zelladhäsion

IgG

Plasmazelle

humorales Immungedächtnis

Plasmablast

mukosale Immunreaktion

Tetanusimmunisierung

Rituximab

Splenektomie

IgA

Zellmigration

B-Zelle

antibody

cell adhesion

IgG

vaccination

B cell

plasma cell

humoral memory

plasmablast

immunity

mucosal

immunological memory

tetanus

B cell depletion

rituximab

splenectomy

IgA

cell migration

570 Biowissenschaften, Biologie

32 Biologie

WF 9860

ddc:570

Transferência de anticorpos reativos com intiminas α, β, γ de Escherichia coli pela placenta e aleitamento materno: determinação quantitativa em soros de recém-nascidos e soros e colostros de suas mães / Transference of antibodies reactive with intimins α, β and γ of Escherichia coli by placenta and breastfeeding: quantitative determination in the sera of newborns and the colostrum and sera of their mothers

Silvia Patricia Nuñes Vaca

14 April 2010

Intimina é uma adesina de natureza protéica das bactérias diarreiogênicas Escherichia coli enteropatogenica (EPEC) e enterohemorrágica (EHEC), capazes de induzir a lesão \'attaching e effacing\' em enterócitos. Os principais subtipos de intiminas de EPEC e EHEC prevalentes no Brasil são α, β e γ. Nosso objetivo foi investigar a transferência de anticorpos maternos anti-intiminas aos recém-nascidos de mães saudáveis de São Paulo, Brasil. Foram pesquisados anticorpos SIgA no colostro e IgG no soro de 50 mulheres saudáveis e no soro de cordão umbilical de seus recém-nascidos, por ELISA utilizando como antígeno proteínas recombinantes purificadas das regiões conservadas e variáveis de intiminas α, β e γ. As concentrações de anticorpos no colostro foram superiores quando comparadas com as concentrações do soro para todos os tipos de intiminas. Não se observaram diferenças estatísticas entre as concentrações de anticorpos reativos com as diferentes intiminas nas amostras de colostro. As concentrações de anticorpos reativos com a região conservada da intimina foram significativamente mais elevadas em comparação com as regiões variáveis no soro dos grupos de mães e de recém-nascidos. Houve alta correlação entre todos os anticorpos anti-intiminas nas amostras de colostro. Comparando-se as concentrações de anticorpos séricos, os coeficientes foram maiores entre anti-α e anti-β que entre os outros pares. Nossos resultados confirmam a transferência de anticorpos maternos para o recém-nascido pela placenta e pelo aleitamento materno e reforça o efeito protetor da amamentação contra infecção por EPEC. / Intimin is a proteic adhesin of enteropatogenic (EPEC) and enterohemorragic (EHEC) Escherichia coli, capable of inducing attachment and effacement lesion in enterocytes. The main subtypes of intimins of EPEC and EHEC prevalent in Brazil are α, β and γ. Our aim is to investigate the transference of maternal anti-intimin antibodies to the newborns of healthy mothers from Sao Paulo, Brazil. IgG and SIgA antibodies were determined in sera and colostrum from 50 healthy women and cord sera from their newborns, by ELISA using as antigens purified recombinant proteins, conserved and variable regions of α, β and γ intimins. The IgA antibody concentrations of colostrum are higher than IgG antibodies in serum for all intimins and there were no statistical differences between them in colostrum samples. The concentrations of antibodies reactive with the conserved region of intimin are significantly higher compared to the variable regions in the sera groups, mothers and newborns. There were high correlation coefficients between all the anti-intimins antibodies in colostrum samples. In the comparison of the seric antibody concentrations, the coefficients were higher between anti-α and anti-β than all the other pairs. Our results confirm the transference of maternal antibodies to the newborns by placenta and breastfeeding and reinforce the high protection effect of breastfeeding against EPEC infection.

Aleitamento materno

Anticorpos IgA (ou Imunoglobulina A)

Anticorpos IgG (ou Imunoglobulina G)

Colostro humano

Imunização passiva

Intimina

Transferência placentária

Breastfeeding

Human colostrum

IgA antibodies (or Immunoglobulin A)

IgG antibodies (or Immunoglobulin G)

Intimin

Passive immunization

Placental transfer

Infectious and bleeding complications in patients with hematological malignancies : Studies on diagnosis and prevention

Svensson, Tobias

January 2017

The overall aim of this thesis is to improve knowledge about the prevention of infectious and bleeding complications in patients with hematological malignancies, primarily in those with chronic lymphocytic leukemia (CLL) and myelodysplatic syndrome (MDS). Hypogammaglobulinemia, impaired production of immunoglobulins (Ig), is an established risk factor for infection, but the impact of IgG pure subclass deficiency (IgG subclass deficiency with adequate production of IgG, IgA, and IgM) has been debated. In a retrospective single institution study, we concluded that pure IgG subclass deficiency in CLL patients is rare and is not associated with an increased risk of infection. Hence, routine analysis of IgG subclasses in patients with CLL is not warranted. There is no consensus on recommending vaccination against Streptococcus pneumoniae to CLL patients mainly because comparative studies are lacking. In our randomized trial, the efficacy of a conjugated pneumococcal vaccine on immune response was superior or equal to a polysaccharide vaccine for all pneumococcal serotypes common for the two vaccines. A conjugate pneumococcal vaccine should therefore be included in vaccination programs for patients with CLL. Bronchoalveolar lavage (BAL) is a well-established invasive method to identify the cause of pulmonary infiltrates in immunocompromised patients. In a retrospective trial, we have studied the diagnostic yield of BAL in patients with hematological malignancies. We concluded that BAL is highly useful in either verifying or excluding some of the important respiratory tract infections affecting these patients, particularly invasive pulmonary aspergillosis (IPA) and Pneumocystis jirovecii pneumonia (PJP). However, standardized procedures for BAL sampling should be continually revised to avoid unnecessary microbiological tests. Thrombocytopenia, an adverse prognostic factor in patients with MDS, can be aggravated by azacitidine, first-line treatment for high-risk MDS. Eltrombopag, a thrombopoietin-receptor agonist (TPO-R), alleviates thrombocytopenia in patients with immune thrombocytopenic purpura (ITP). In a phase I clinical trial, we concluded that the combination of eltrombopag and azacitidine in high-risk MDS patients with thrombocytopenia is feasible and well tolerated in doses up to 200 mg eltrombopag daily.

Chronic lymphocytic leukemia

Immunodeficiency

Hypogammaglobulinemia

IgG subclass

Pneumococci

Pneumococcal vaccine

Polysaccharide vaccine

Protein-conjugate vaccine

Aspergillosis

Bronchoalveolar lavage

Invasive fungal disease

Pneumocystis jirovecii pneumonia

Myelodysplastic syndrome

Azacitidine

Eltrombopag

Thrombocytopenia

Thrombopoietin receptor

Medical and Health Sciences

Medicin och hälsovetenskap

Experimentální infekce Oryctolagus cuniculus motolicí Fascioloides magna / Experimental infection of Oryctolagus cuniculus with fluke Fascioloides magna

Melounová, Klára

January 2015

Fasioloides magna is a trematode parasitizing in the liver parenchyma of ruminants. Its life cycle is associated with the humid environment and includes intermediate freshwater snail hosts from family Lymnaeidae. According to the ability of host to form a certain type of a pseudocyst during fascioloidosis, they can be,divided in three groups, specific definitive hosts (red deers, fallow deers, roe deers), nonspecific definitive hosts (cattle, wild boars and elks) and atypical hosts (sheeps and goats). Beside the natural infections also the experimental infections of other potential host species has been realized (chamois, llama and bighorn sheep and traditional laboratory animals such as mice, guinea pigs, rats and rabbits). In the context of different diseases, many changes in infected organism can occur. These can be qualitatively and quantitatively evaluated. Similarly, during fascioloidosis the changes associated with the presence of the parasite in the host's body is possible to monitor, e.g. antibody production, increase in the number of eosinophils, release of eggs in faeces, internal bleeding, or the level liver damage. The liver damage is corresponding primarily to biochemical parameters of blood, not only the liver enzymes, but also other blood components, like blood proteins, lipids,...

ASPECTOS CLÍNICOS E SOROLÓGICOS DE INDIVÍDUOS COM SINAIS E SINTOMAS DE FEBRE CHIKUNGUNYA / Clinical and serological aspects of individuals with signs and symptoms of Chikungunya Fever

Koga, Rosemary de Carvalho Rocha

15 March 2017

Submitted by admin tede (tede@pucgoias.edu.br) on 2017-04-27T14:37:47Z No. of bitstreams: 1 ROSEMARY DE CARVALHO ROCHA KOGA.pdf: 1840064 bytes, checksum: 5be7272271d61789b6dc93e32af0b7a3 (MD5) / Made available in DSpace on 2017-04-27T14:37:47Z (GMT). No. of bitstreams: 1 ROSEMARY DE CARVALHO ROCHA KOGA.pdf: 1840064 bytes, checksum: 5be7272271d61789b6dc93e32af0b7a3 (MD5) Previous issue date: 2017-03-15 / Introduction: Chikungunya fever (FCHIK) is a disease of abrupt onset, transmitted by arthropod mosquitoes intermediate hosts of the Chikungunya virus (CHIKV). The illness has a significant impact on the quality of life of the affected person. Since a disease causes intense and prolonged symptoms of polyarthralgia and myalgia, it requires health care, during a recovery, more than other arboviruses. The objective of this study was to study clinicians and clinicians suggestive of FCHIK, residing in the States of Amapá and Goiás, aiming to correlate the results of laboratory tests with the presented symptomatology. Materials and methods: The study was carried out at the Center for Immunological Studies and Research of the Pontifical Catholic University of Goiás, Goiânia, and in Emergency Care Units in the cities of Macapá, Oiapoque and Santana-AP. The study population consisted of 80 individuals with suspected FCHIK and for investigators of inflammatory markers, the control group consisted of 20 blood samples from healthy donors from Goiana Central de Serologia e Imunohematologia. Viral RNA extraction was performed, followed by RNA detection by Real-Time Polymerase Chain Reaction. In addition to ELISA for detection of IgM and IgG against Chikungunya virus. Participants symptoms were correlated with serology and Creactive protein (CRP), which was evaluated in healthy subjects and in people with FCHIK. Results: No data presented for detection of viral RNA by RT-qPCR for CHIKV, but three samples were positive in this technique for zika virus and one for dengue subtype 1 (DENV1). In an enzyme-linked immunosorbent assay, 26 samples were positive for IgG and 3 for IgM. Regarding the stage of the disease, 10 were in the acute phase, 04 in the subacute phase and 12 in the chronic phase. Correlated the results of the serology with a symptomatology it was observed that the acute phase, all have fever, 90% headache, 70% arthralgia and 60% edema. (100%), myalgia and edema (75%). (100%), arthralgia (92%) and myalgia (75%). When comparing participants with negative serology, n = 54, the most prevalent symptoms were rash, headache, fever, and arthralgia. The CRP levels in individuals infected with more than four symptoms were higher when compared with healthy individuals. Conclusion: The study focused on people with a clinical picture characteristic of FCHIK. The most common symptom in the three phases presented for arthralgia, followed by edema and myalgia, a fever was frequent only in the acute phase. All participants were negative in the evaluation of viral RNA by RT-qPCR for CHIKV, for the virus has a short duration in the body, and this methodology is limited to the time of symptom onset and sample collection, DENV and ZIKV. IG G. Those with negative serology for CHIKV, despite taking into account the joints, symptoms common to other arboviruses. CRP levels have been shown to be high relative to healthy subjects. / Introdução: A Febre Chikungunya (FCHIK) é uma doença de início abrupto, transmitida por mosquitos artrópodes hospedeiros intermediários do vírus Chikungunya (CHIKV). A enfermidade representa um significativo impacto na qualidade de vida da pessoa afetada. Uma vez que a doença causa sintomas intensos e prolongados de poliartralgia e mialgia, requerendo atenção de saúde, durante a recuperação, mais do que outras arboviroses. Objetivou-se estudar aspectos clínicos e sorológicos de indivíduos apresentando quadro clínico sugestivo de FCHIK, residentes nos Estados de Amapá e Goiás, visando correlacionar os resultados de testes laboratoriais com a sintomatologia apresentada. Materiais e métodos: O estudo foi realizado no Núcleo de Estudos e Pesquisa Imunológica da Pontifícia Universidade Católica de Goiás, em Goiânia, e em Unidades de Pronto Atendimento de Saúde das cidades de Macapá, Oiapoque e Santana-AP. A população de estudo foi constituída de 80 indivíduos com suspeita de FCHIK e para comparar os marcadores inflamatórios, o grupo controle foi constituído de 20 amostras de sangue de doadores saudáveis da Central Goiana de Sorologia e Imunohematologia. Foi realizada a extração do RNA viral, seguido de detecção do RNA por meio de Reação em Cadeia de Polimerase em Tempo Real. Além de ELISA para detecção de IgM e IgG específicos para o CHIKV. Os sintomas dos participantes foram correlacionados com o resultado da sorologia e da proteína C reativa (PCR), que foi avaliada em indivíduos saudáveis e em pessoas com FCHIK. Resultados: Nenhuma amostra apresentou limiar de detecção do RNA viral por RT-qPCR para CHIKV, porém três amostras foram positivas nessa técnica para vírus zika (ZIKV) e uma para dengue subtipo 1 (DENV1). Em ensaio imunoenzimático, 26 amostras foram positivas para IgG e 3 dessas para IgM. Em relação ao estágio da doença, 10 encontravam-se em fase aguda, 04 em fase subaguda e 12 em fase crônica. Correlacionados os resultados da sorologia com a sintomatologia observou-se que os de fase aguda, todos tiveram febre, 90% cefaleia, 70% artralgia e 60% edema. Enquanto que, os de fase subaguda tiveram: artralgia e cefaleia (100%), mialgia e edema (75%). Os de fase crônica tiveram edema (100%), artralgia (92%) e mialgia (75%). Quando comparados os participantes com sorologia negativa, n=54, os sintomas mais apresentados foram exantema, cefaleia, febre e artralgia. Os níveis de PCR nos indivíduos infectados e que apresentavam mais de quatro sintomas foram maiores quando comparados com indivíduos saudáveis. Conclusão: O estudo focou em pessoas com quadro clínico característico para FCHIK. O sintoma mais comum nas três fases apresentadas foi a artralgia, seguido de edema e mialgia, a febre foi frequente somente na fase aguda. Todos os participantes foram negativos na avaliação do RNA viral por RT-qPCR para CHIKV, pois o vírus tem uma curta duração no organismo, e esta metodologia é limitada ao tempo de início dos sintomas e coleta de amostra, ainda assim foi encontrado RNA viral do DENV e ZIKV. Alguns participantes foram positivos para sorologia IgG. Aqueles com sorologia negativa para CHIKV, apesar de terem dor nas articulações, tinham sintomas comuns a outras arboviroses. Os níveis de PCR demonstraram-se elevados em relação aos indivíduos saudáveis.

CIENCIAS DA SAUDE

Feedback Enhancement of Antibody Responses via Complement and Fc Receptors

Dahlström, Jörgen

January 2001

<p>IgG, IgM and IgE in complex with antigen have the capacity to regulate specific immune responses. In this investigation, the role of Fc receptors for IgG (FcγRI, FcγRII and FcγRIII) and complement receptors 1 and 2 (CR1/2) for antibody-mediated enhancement of antibody responses are investigated.</p><p>IgM is known to efficiently activate complement and thereby enhance specific antibody responses but it is not known if this involves binding to CR1/2. Using CR1/2 deficient mice, immunized with sheep erythrocytes alone or together with specific IgM, we present evidence that IgM-mediated enhancement is completely dependent on CR1/2 expression, whereas IgG or IgE in complex with bovine serum albumin (BSA) induce strong antibody responses in CR1/2-deficient mice. Enhancement by IgE is mediated via the low affinity receptor for IgE (FcεRII, CD23). However, the receptors which are involved in IgG-mediated enhancement are not known. We find that γ-chain-deficient mice (lacking FcγRI and FcγRIII) have impaired antibody responses to IgG/BSA complexes. In contrast, FcγRIII deficient mice have normal responses, suggesting that FcγRI mediates the effect. Furthermore, IgG/BSA complexes induce up to 189-fold stronger antibody responses in FcγRIIB-deficient mice than in wild-type mice. The threshold dose of IgG/BSA required was lower, the response was sustained for longer and initiated earlier in FcγRIIB-deficient than in wild-type animals. The findings suggest that FcγRIIB acts as a "safety-valve" preventing excessive antibody production during an immune response. We show for the first time that IgG3/BSA complexes can mediate enhancement of specific antibody responses. Their effect does not involve known Fcγ receptors.</p>

Genetics

Mouse

transgenic/knockout

immune regulation

B lymphocytes

Fc receptors

complement

IgG

IgM

IgE

Fc-gamma-RI

Fc-gamma-RII

Fc-gamma-RIII

CR1

CR2

CD21

CD35

Genetik

Clinical genetics

Klinisk genetik

Feedback Enhancement of Antibody Responses via Complement and Fc Receptors

Dahlström, Jörgen

January 2001

IgG, IgM and IgE in complex with antigen have the capacity to regulate specific immune responses. In this investigation, the role of Fc receptors for IgG (FcγRI, FcγRII and FcγRIII) and complement receptors 1 and 2 (CR1/2) for antibody-mediated enhancement of antibody responses are investigated. IgM is known to efficiently activate complement and thereby enhance specific antibody responses but it is not known if this involves binding to CR1/2. Using CR1/2 deficient mice, immunized with sheep erythrocytes alone or together with specific IgM, we present evidence that IgM-mediated enhancement is completely dependent on CR1/2 expression, whereas IgG or IgE in complex with bovine serum albumin (BSA) induce strong antibody responses in CR1/2-deficient mice. Enhancement by IgE is mediated via the low affinity receptor for IgE (FcεRII, CD23). However, the receptors which are involved in IgG-mediated enhancement are not known. We find that γ-chain-deficient mice (lacking FcγRI and FcγRIII) have impaired antibody responses to IgG/BSA complexes. In contrast, FcγRIII deficient mice have normal responses, suggesting that FcγRI mediates the effect. Furthermore, IgG/BSA complexes induce up to 189-fold stronger antibody responses in FcγRIIB-deficient mice than in wild-type mice. The threshold dose of IgG/BSA required was lower, the response was sustained for longer and initiated earlier in FcγRIIB-deficient than in wild-type animals. The findings suggest that FcγRIIB acts as a "safety-valve" preventing excessive antibody production during an immune response. We show for the first time that IgG3/BSA complexes can mediate enhancement of specific antibody responses. Their effect does not involve known Fcγ receptors.

Genetics

Mouse

transgenic/knockout

immune regulation

B lymphocytes

Fc receptors

complement

IgG

IgM

IgE

Fc-gamma-RI

Fc-gamma-RII

Fc-gamma-RIII

CR1

CR2

CD21

CD35

Genetik

Clinical genetics

Klinisk genetik

Pesquisa de anticorpos antitoxina diftérica e fenotipagem de linfócitos T em indivíduos soronegativos e soropositivos para o HIV-1 acompanhados no Instituto de Biologia do Exército Rio de Janeiro

Francisco Almeida Braga Speranza

21 September 2010

Dados sorológicos sobre doenças imunopreveníveis são úteis para avaliar o sucesso de programas de imunização e a identificação de populações suscetíveis. Nos últimos 20 anos, as campanhas de imunização na infância foram eficientes no controle da difteria em muitos países. No entanto, uma taxa importante da população adulta continua suscetível à doença, uma vez que os níveis de anticorpos protetores reduzem com o passar do tempo. A infecção pelo HIV-1 leva a uma perda progressiva das funções imunes. Com o aumento da expectativa de vida dos pacientes HIV-1, e a maior incidência de infecções, torna-se importante a avaliação dos níveis de anticorpos antitoxina diftérica nestes grupos. O objetivo deste estudo foi avaliar os níveis de anticorpos antitoxina diftérica e a contagem de linfócitos T (LT) em indivíduos infectados ou não pelo HIV -1, assistidos no Instituto de Biologia do Exército (IBEx). Investigamos a correlação entre níveis de anticorpos específicos e os seguintes parâmetros dos grupos de estudo: sexo, faixa etária, categoria militar ou civil; vacinação prévia contra difteria; número de LT CD4+ e CD8+; e entre os indivíduos HIV-1 positivos a correlação com a carga viral e a terapia com antirretrovirais potentes (HAART). Para a quantificação de anticorpos antitoxina diftérica utilizou-se um kit ELISA (IBL Immuno-Biological Laboratories, Hamburg, Alemanha) e amostras de sangue de 180 indivíduos, sendo que 75 eram doadores de sangue e 105 eram pacientes positivos para o HIV-1. Aproximadamente 60% dos indivíduos estavam parcialmente protegidos contra a difteria (IgG específica &#8805; 0,1 < 1,0 UI/mL). Entre os doadores de sangue, 56% dos indivíduos estavam protegidos (IgG específica &#8805; 1,0 UI/mL) contra a doença, contra apenas 29 % dos indivíduos positivos para HIV-1. Em relação aos doadores de sangues de origem civil não se observou correlação entre os níveis de IgG e a idade, enquanto que, para os militares observou-se uma correlação inversa. Não houve diferença significativa na resposta de anticorpos para difteria entre os indivíduos soropositivos com CD4+ baixo ou normal. Pacientes com HAART mostraram uma resposta significativamente mais baixa de anticorpos (média geométrica de 0.39 IU/mL, n = 84) do que os pacientes não tratados (média geométrica de 0.58 IU/mL, n = 19). A diferença na idade média dos pacientes não tratados (46 anos) e tratados com HAART (35 anos) provavelmente influenciou estes resultados, já que os níveis de anticorpos contra a difteria declinam com o tempo. A existência em nossa comunidade de adultos (militares e civis) suscetíveis à difteria, incluindo os indivíduos soropositivos, reforça que a imunização a cada 10 anos e os estudos soroepidemiológicos são muito importantes e devem ser estimulados. / Serologic data on diseases that are preventable by vaccine are useful to evaluate the success of immunization programs and to identify susceptible subgroups. In the last 20 years the childhood immunization program has been efficient in the control of the diphtheria in many countries. However, an important rate of adult population remains susceptible to the illness, since diphtheria protective antibodies decline with time. HIV-1 infection leads to a progressive loss of immune functions. With the increase of life expectancy of HIV-1 patients, and also the increment of infections, it is important to known the antibody levels to diphtheria toxin in these population. The aim of this study was to evaluate the IgG levels to diphtheria toxin and T lymphocytes (LT) counts in HIV-1 infected and non- infected individuals assisted at the Instituto de Biologia do Exército (IBEx), Rio de Janeiro. We investigated the correlation between specific antibody levels and the following parameters of the study groups: gender, age-group, military or civilian origin, previous diphtheria immunization, CD4+ and CD8+ counts. For HIV-1 patients, we also analysed the correlation of specific antibodies with viral load and the use of highly active antiretroviral therapy HAART. A commercial diphtheria-ELISA kit (IBL Immuno-Biological Laboratories, Hamburg, Alemanha) was used to evaluate IgG levels in serum samples of 180 individuals. Blood donors accounted for 75 individuals and 105 subjects were HIV-1 patients. About 60% of individuals were partially protected against diphtheria (specific IgG levels &#8805; 0,1 < 1,0 IU/mL). About 56% of blood donors were protected against diphtheria (specific IgG > 1.0 IU/mL). Howerver, only 29% of HIV-1 patients showed the same level of protective antibodies. For the civilian blood donors, there were no correlation between specific antibody levels and age group. In contrast, a negative correlation was observed in the military group. There were no differences in diphtheria serology according to CD4+ counts of HIV-1 patients or blood donors. Interesting, HAART- treated (n = 84) patients showed a significantly lower antibody response (geomean of 0.39 IU/mL) than untreated patients (geomean of 0.58 IU/mL, n = 19). As tetanus and diphtheria antibodies tend to decrease with time, the difference in age between HAART-treated patients (mean of 46 years) and those not being treated (mean of 35 years) might introduce a bias in the study. Concluding, the existence of susceptible military and civilian adults in our community, including HIV-1 patients, reinforce that reliable seroepidemiological data and immunization campaigns should be routinely stimulated.

Imunoglobulina G

Anticorpos

Difteria

Pacientes infectados pelo HIV-1

Doadores de sangue

Militares

Vacinas contra difteria

IgG antitoxina diftérica

Anticorpos protetores

Difteria

Vaccine

Diphtheria protective antibodies

Militaries

Blood donors

HIV-1 infected patients

IMUNOLOGIA APLICADA

Pesquisa de anticorpos antitoxina diftérica e fenotipagem de linfócitos T em indivíduos soronegativos e soropositivos para o HIV-1 acompanhados no Instituto de Biologia do Exército Rio de Janeiro

Francisco Almeida Braga Speranza

21 September 2010

Dados sorológicos sobre doenças imunopreveníveis são úteis para avaliar o sucesso de programas de imunização e a identificação de populações suscetíveis. Nos últimos 20 anos, as campanhas de imunização na infância foram eficientes no controle da difteria em muitos países. No entanto, uma taxa importante da população adulta continua suscetível à doença, uma vez que os níveis de anticorpos protetores reduzem com o passar do tempo. A infecção pelo HIV-1 leva a uma perda progressiva das funções imunes. Com o aumento da expectativa de vida dos pacientes HIV-1, e a maior incidência de infecções, torna-se importante a avaliação dos níveis de anticorpos antitoxina diftérica nestes grupos. O objetivo deste estudo foi avaliar os níveis de anticorpos antitoxina diftérica e a contagem de linfócitos T (LT) em indivíduos infectados ou não pelo HIV -1, assistidos no Instituto de Biologia do Exército (IBEx). Investigamos a correlação entre níveis de anticorpos específicos e os seguintes parâmetros dos grupos de estudo: sexo, faixa etária, categoria militar ou civil; vacinação prévia contra difteria; número de LT CD4+ e CD8+; e entre os indivíduos HIV-1 positivos a correlação com a carga viral e a terapia com antirretrovirais potentes (HAART). Para a quantificação de anticorpos antitoxina diftérica utilizou-se um kit ELISA (IBL Immuno-Biological Laboratories, Hamburg, Alemanha) e amostras de sangue de 180 indivíduos, sendo que 75 eram doadores de sangue e 105 eram pacientes positivos para o HIV-1. Aproximadamente 60% dos indivíduos estavam parcialmente protegidos contra a difteria (IgG específica &#8805; 0,1 < 1,0 UI/mL). Entre os doadores de sangue, 56% dos indivíduos estavam protegidos (IgG específica &#8805; 1,0 UI/mL) contra a doença, contra apenas 29 % dos indivíduos positivos para HIV-1. Em relação aos doadores de sangues de origem civil não se observou correlação entre os níveis de IgG e a idade, enquanto que, para os militares observou-se uma correlação inversa. Não houve diferença significativa na resposta de anticorpos para difteria entre os indivíduos soropositivos com CD4+ baixo ou normal. Pacientes com HAART mostraram uma resposta significativamente mais baixa de anticorpos (média geométrica de 0.39 IU/mL, n = 84) do que os pacientes não tratados (média geométrica de 0.58 IU/mL, n = 19). A diferença na idade média dos pacientes não tratados (46 anos) e tratados com HAART (35 anos) provavelmente influenciou estes resultados, já que os níveis de anticorpos contra a difteria declinam com o tempo. A existência em nossa comunidade de adultos (militares e civis) suscetíveis à difteria, incluindo os indivíduos soropositivos, reforça que a imunização a cada 10 anos e os estudos soroepidemiológicos são muito importantes e devem ser estimulados. / Serologic data on diseases that are preventable by vaccine are useful to evaluate the success of immunization programs and to identify susceptible subgroups. In the last 20 years the childhood immunization program has been efficient in the control of the diphtheria in many countries. However, an important rate of adult population remains susceptible to the illness, since diphtheria protective antibodies decline with time. HIV-1 infection leads to a progressive loss of immune functions. With the increase of life expectancy of HIV-1 patients, and also the increment of infections, it is important to known the antibody levels to diphtheria toxin in these population. The aim of this study was to evaluate the IgG levels to diphtheria toxin and T lymphocytes (LT) counts in HIV-1 infected and non- infected individuals assisted at the Instituto de Biologia do Exército (IBEx), Rio de Janeiro. We investigated the correlation between specific antibody levels and the following parameters of the study groups: gender, age-group, military or civilian origin, previous diphtheria immunization, CD4+ and CD8+ counts. For HIV-1 patients, we also analysed the correlation of specific antibodies with viral load and the use of highly active antiretroviral therapy HAART. A commercial diphtheria-ELISA kit (IBL Immuno-Biological Laboratories, Hamburg, Alemanha) was used to evaluate IgG levels in serum samples of 180 individuals. Blood donors accounted for 75 individuals and 105 subjects were HIV-1 patients. About 60% of individuals were partially protected against diphtheria (specific IgG levels &#8805; 0,1 < 1,0 IU/mL). About 56% of blood donors were protected against diphtheria (specific IgG > 1.0 IU/mL). Howerver, only 29% of HIV-1 patients showed the same level of protective antibodies. For the civilian blood donors, there were no correlation between specific antibody levels and age group. In contrast, a negative correlation was observed in the military group. There were no differences in diphtheria serology according to CD4+ counts of HIV-1 patients or blood donors. Interesting, HAART- treated (n = 84) patients showed a significantly lower antibody response (geomean of 0.39 IU/mL) than untreated patients (geomean of 0.58 IU/mL, n = 19). As tetanus and diphtheria antibodies tend to decrease with time, the difference in age between HAART-treated patients (mean of 46 years) and those not being treated (mean of 35 years) might introduce a bias in the study. Concluding, the existence of susceptible military and civilian adults in our community, including HIV-1 patients, reinforce that reliable seroepidemiological data and immunization campaigns should be routinely stimulated.

Imunoglobulina G

Anticorpos

Difteria

Pacientes infectados pelo HIV-1

Doadores de sangue

Militares

Vacinas contra difteria

IgG antitoxina diftérica

Anticorpos protetores

Difteria

Vaccine

Diphtheria protective antibodies

Militaries

Blood donors

HIV-1 infected patients

IMUNOLOGIA APLICADA

Neuroteratology and Animal Modeling of Brain Disorders

Archer, Trevor, Kostrzewa, Richard M.

09 February 2016

Over the past 60 years, a large number of selective neurotoxins were discovered and developed, making it possible to animal-model a broad range of human neuropsychiatric and neurodevelopmental disorders. In this paper, we highlight those neurotoxins that are most commonly used as neuroteratologic agents, to either produce lifelong destruction of neurons of a particular phenotype, or a group of neurons linked by a specific class of transporter proteins (i.e., dopamine transporter) or body of receptors for a specific neurotransmitter (i.e., NMDA class of glutamate receptors). Actions of a range of neurotoxins are described: 6-hydroxydopamine (6-OHDA), 6-hydroxydopa, DSP-4, MPTP, methamphetamine, IgG-saporin, domoate, NMDA receptor antagonists, and valproate. Their neuroteratologic features are outlined, as well as those of nerve growth factor, epidermal growth factor, and that of stress. The value of each of these neurotoxins in animal modeling of human neurologic, neurodegenerative, and neuropsychiatric disorders is discussed in terms of the respective value as well as limitations of the derived animal model. Neuroteratologic agents have proven to be of immense importance for understanding how associated neural systems in human neural disorders may be better targeted by new therapeutic agents.

5

7-DHT

6-hydroxydopa

6-hydroxydopamine

autism

domoic acid

DSP-4

epidermal growth factor

IgG-saporin

Lesch-Nyhan disease

methamphetamine

MPTP

nerve growth factor

neuro-ontogeny

neuroteratology

neurotoxicity

neurotoxins

NMDA

Parkinson’s disease

Quinpirole

schizophrenia

tardive dyskinesia

valproate

Biomedical Sciences