Estudos dos efeitos antioxidantes e anti-inflamatórios da própolis sobre as células RAW 264.7 e na resposta inflamatória pulmonar aguda causada pela exposição à fumaça de cigarro em camundongos

A doença pulmonar obstrutiva crônica (DPOC) causa a redução da capacidade respiratória e seu desenvolvimento é associado à fumaça de cigarro. O cigarro possui mais de 4800 substâncias tóxicas e causa a morte de seis milhões de pessoas por ano no mundo. Estudos buscam meios de reverter os males causados pela fumaça de cigarro. A própolis (P) é um produto produzido por abelhas que possui várias propriedades. O objetivo deste trabalho foi avaliar os efeitos antioxidantes da P em macrófagos murinos e na inflamação pulmonar aguda induzida pela fumaça de cigarro (CS) em camundongos. A análise dos compostos fitoquímicos do extrato alcóolico da P (EAP) foi feita por cromatografia gasosa acoplada à espectrometria de massa (GC-MS). Células da linhagem RAW 264.7 foram tratadas em diversas concentrações de P durante 24 horas. Após tratamento, as seguintes análises foram realizadas: polifenóis totais; viabilidade celular (MTT); potencial redutor (DPPH); espécies reativas de oxigênio totais (ROS) e de malondialdeído (MDA). Trinta camundongos C57BL/6 foram divididos em 3 grupos (n=10/grupo): Controle+P, CS e CS+P. Ambos os grupos CS foram expostos a 6 cigarros/dia durante 5 dias. O grupo CS foi tratado com veículo. O pulmão e o lavado broncoalveolar (BAL) foram coletados para análise histológica e contagem diferencial de células. As análises para mieloperoxidase (MPO), superóxido dismutase (SOD), catalase (CAT), glutationa peroxidase (GPx), glutationa reduzida (GSH) e oxidada (GSSG), MDA, nitrito e western blotting para TNF-alfa foram realizadas. A análise fitoquímica do EAP mostrou a presença dos ácidos hidrocinâmicos e coumárico, a artepilina C e a drupanina. Foi observado o aumento concentração-dependente dos níveis de polifenóis totais (p<0,001), do MTT (p<0,001) e do DPPH (p<0,001), e o inverso com o MDA (p<0,001). Os níveis de ROS diminuem nas concentrações de 15,6 e 31,2 mg/mL (p<0,05, ambos). A histologia pulmonar do grupo Controle+P foi similar ao do CS+P e foi observado um influxo de macrófagos e neutrófilos no grupo CS (p<0,01 e p<0,001, respectivamente). Os níveis de MPO foram aumentados no grupo CS (526,534,72 mU/mg ptn, p<0,01), mas houve uma redução no grupo CS+P (385,127,64 mU/mg ptn, p<0,05) comparável ao Controle+P (13412,99 mU/mg ptn, p<0,001), o mesmo aconteceu com as enzimas antioxidantes: SOD (Controle+P: 523,529,6 U/mg ptn; CS: 523,529,6 U/mg ptn, p<0,001; CS+P: 246,815,69 U/mg ptn, p<0,001); CAT (Controle+P: 37,383,39 U/mg ptn; CS: 92,686,24 U/mg ptn, p<0,001; CS+P: 59,844,55 U/mg ptn, p<0,05); GPx (Controle+P: 2,230,17 (M/min/mg ptn) x 10-1; CS: 4,510,31 (M/min/mg ptn) x 10-1, p<0,001; CS+P: 2,640,19 (M/min/mg ptn) x 10-1, p<0,05). O inverso ocorreu com a relação GSH/GSSG (Controle+P: 1,0880,17; CS: 0,7360,07, p<0,05; CS+P: 1,2580,10, p<0,05). Os níveis de MDA (Controle+P: 0,2660,05 nMol/mg ptn; CS: 0,940,076 nMol/mg ptn, p<0,001; CS+P: 0,4980,06 nMol/mg ptn, p<0,01) e de nitrito (Controle+P: 50,014,19 Mol/mg ptn; CS: 108,77,73 Mol/mg ptn, p<0,001; CS+P: 58,843,42 nMol/mg ptn, p<0,01) estavam aumentados no CS que em outros grupos. A expressão de TNF-α foi observada no grupo CS. O tratamento da P apresentou ação anti-inflamatória e antioxidante em macrófagos e em camundongos expostos à fumaça de cigarro, possivelmente pela ação dos polifenóis presentes nela

Perfil dos peptídeos gastrointestinais na obesidade programada pelo desmame precoce e após a terapia anti-obesidade com cálcio

O desmame precoce (DP) leva ao desenvolvimento tardio de obesidade e de resistência insulínica (RI), sendo essas alterações prevenidas quando os animais são suplementados com cálcio. Sabe-se que os peptídeos gastrointestinais (GI) atuam na regulação do apetite e em diversos outros processos, podendo ter um papel relevante no desenvolvimento da obesidade e RI. Uma vez que os animais programados pelo DP são obesos e hiperfágicos, investigamos o perfil plasmático e tecidual de GLP-1, CCK e PYY (anorexígenos) de grelina (orexígena) e de seus receptores, assim como o efeito da dieta rica em cálcio sobre estes peptídeos a fim de identificar algum distúrbio no controle do apetite. Ao nascimento das proles, ratas lactantes Wistar foram separadas em: grupo DP (desmame precoce, n=20), filhotes cujas mães tiveram as mamas enfaixadas, impedindo o acesso da prole ao leite nos últimos 3 dias de lactação; e grupo C (controle, n=10), filhotes com livre acesso ao leite materno. Aos 120 dias, as proles DP foram subdivididas em: grupo DP, alimentado com ração comercial padrão, e grupo DPCa, alimentado com ração suplementada com cálcio (10g de carbonato de cálcio/Kg de ração). Os animais foram sacrificados aos 21 e 180 dias de vida. Quantificamos: GLP-1, CCK, PYY, grelina e citocinas (IL-6, TNF-α e IL-10) plasmáticas por ELISA; o conteúdo de grelina no estômago por ELISA e imunohistoquímica; o conteúdo de GLP-1 (intestino), GLP1-R (intestino, TA e ARC) e GHSR-1a (estômago e ARC) por Western blotting. Dados significativos quando p<0,05. Aos 21 dias, a prole DP apresentou aumento de GLP-1 no plasma (+168%) e GLP1-R no tecido adiposo (+72%), embora menor conteúdo de GLP-1 (-59%) e GLP1-R (-58%) no intestino. Não observamos alterações plasmáticas de grelina, CCK e PPY e no conteúdo de GHSR-1a no estômago aos 21 dias. Aos 180 dias, não verificamos diferença em nenhum dos peptídeos GI no plasma na prole DP. Porém, observamos menor conteúdo intestinal de GLP-1 tanto no grupo DP (-33%) quanto no DPCa (-32%), e uma tendência da grelina (+20%) e do GHSR-1a (+31%) a estarem elevados no estômago do grupo DP. Além de menor conteúdo de GLP1-R no tecido adiposo no grupo DP (-59%) e maior conteúdo de GLP1-R no intestino da prole DPCa (+62%). Não encontramos diferença entre os grupos na expressão de GLP1-R e GHSR-1a no ARC. O grupo DP apresentou ainda um perfil pró-inflamatório caracterizado por maior TNF-α e menor IL-10 no plasma. O DP alterou o perfil dos peptídeos GI a curto e longo prazos, o que pode ter colaborado para o desenvolvimento da obesidade, hiperfagia e RI neste modelo, uma vez que o GLP-1, único peptídeo alterado no período de imprinting, possui um possível papel adipogênico. A suplementação com cálcio foi capaz de reverter todas as alterações produzidas pelo DP. Evidenciamos, então, a importância do aleitamento materno na formação do comportamento alimentar e do balanço metabólico, bem como o papel da suplementação com cálcio no tratamento da obesidade e seus distúrbios associados, inclusive nas alterações do apetite.

Estudo do potencial anti-inflamatório e antiartrítico de Pterodon polygalaeflorus e dos seus mecanismos de ação

O gênero Pterodon pertence à família das Fabaceae e inclui quatro espécies nativas do Brasil: P. emarginatus Vog., P. apparicioi Pedersoli, P. abruptus Benth. e a espécie objeto deste estudo P. polygalaeflorus Benth.. Seus frutos são utilizados pela medicina popular devido às propriedades antirreumática, analgésica, anti-inflamatória, dentre outros. O objetivo deste trabalho foi avaliar a espécie Pterodon polygalaeflorus quanto ao seu potencial anti-inflamatório, antiartrítico e toxicológico, através da análise de seus efeitos em modelos in vitro e in vivo. Os extratos EEPpg, EHPpg e EDPpg reduziram (p<0,01) a produção in vitro de NO, por macrófagos ativados por LPS, com baixa citotoxicidade e diminuíram a celularidade (p<0,05) no exsudato inflamatório no modelo de inflamação in vivo conhecido como air pouch. O extrato mais ativo (EHPpg) foi selecionado e submetido a fracionamento em coluna de sílica gel 60 gerando quatro frações. Todas as frações (Fr I-Fr IV) reduziram: a produção de NO (p<0,001) por macrófagos ativados, com baixa ou nenhuma citotoxicidade; a migração de macrófagos in vitro (p<0,01, ensaio de wound healing) e in vivo (p<0,05, peritonite induzida por tioglicolato); e a proliferação de esplenócitos estimulados com Con A (p<0,001). As frações III e IV, mais ativas nos ensaios anteriores, mostraram ação antiartrítica (com 0,02 mg/kg), utilizando o modelo in vivo de artrite induzida por adjuvante completo de Freund (AIA), demonstrada por redução: do índice de edema de pata em 23,7% (Fr III) e 43,95% (Fr IV); das lesões histopatológicas na região tíbio-tarsal típicas de articulações com AIA (p< 0,05); do peso e celularidade do linfonodo e do baço, mas não da celularidade da medula óssea; das subpopulações de linfócitos (CD4+, CD8+ e CD19+) nos linfonodos inguinais, porém com significativo aumento das subpopulações ativadas CD4+CD69+, redução da CD8+CD69+ e aumento de CD19+CD69+ (apenas na Fr III); e redução da população de macrófagos no baço (p<0,001). As frações III e IV mostraram ação imunossupressora em nível celular e molecular, reduzindo (p<0,001) os níveis do mRNA da iNOS, assim como as citocinas IL-1β, TNF-α e IL-10, em nível de mRNA e proteína, em cultura de macrófagos. A expressão do receptor CD14, em macrófagos estimulados por LPS (31,74%), foi inibida apenas pela Fr III. A osteoclastogênese foi inibida pelas frações III e IV, sugerindo uma ação antiartrítica das frações em nível de diferenciação celular para osteoclastos (inibição). Este efeito pode resultar da inibição da expressão do fator de transcrição NFATc1, no caso da Fr III. Por fim, as frações Fr III e Fr IV não apresentaram toxicidade subaguda, potencial mutagênico (teste de Ames) ou genotóxico (teste do micronúcleo). A ausência de toxicidade in vivo das frações ficou demonstrada pela ausência de alteração no peso corporal e de órgãos, nas concentrações séricas de creatinina, ácido úrico, triglicerídeos, colesterol, ALT e ALP, ou de CYP1A1 e GSTs no fígado. Análises fitoquímicas (GC-MS e TLC) mostraram uma grande variedade de terpenos nas frações III e IV, sendo majoritários os furano-diterpenos derivados do vouacapano. O diterpeno isolado, Ppg-01, presente nas frações III (5,12%) e IV (18,47%), reduziu a produção in vitro de NO e o edema de pata induzido por carragenina (p<0,001). Em conjunto, os dados sugerem que o Ppg-01 esteja contribuindo para as ações anti-inflamatórias e imunomoduladoras das frações III e IV, e que estas propriedades estejam associadas aos efeitos antiartríticos observados.

The anti-HIV-1 effect of scutellarin

Scutellarin was purified from the plant Erigeron breuiscapus (Vant.) Hand.-Mazz. The activity against 3 strains of human immunodeficiency virus (HIV) was determined in vitro in this study. These were laboratory-derived virus (HIV-I-IIIB), drug-resistant virus (HIV-I-74V), and low-passage clinical isolated virus (HIV-1(KM018)). From syncytia inhibition study, the EC50 of scutellarin against HIV-I-IIB direct infection in C8166 cells was 26 mu M with a therapeutic index of 36. When the mode of infection changed from acute infection to cell-to-cell infection, this compound became even more potent and the EC50 reduced to 15 mu M. This suggested that cell fusion might be affected by this compound. By comparing the inhibitory effects on p24 antigen, scutellarin was also found to be active against HIV-1(74V) (EC50 253 mu M) and HIV-1(KM018) (EC50 136 mu M) infection with significant difference in potency. The mechanism of its action was also explored in this study. At a concentration of 433 mu M, scutellarin inhibited 48% of the cell free recombinant HIV-1 RT activity. It also caused 82% inhibition of HIV-1 particle attachment and 45% inhibition of fusion at the concentrations of 54 mu M. In summary, scutellarin was found to inhibit several strains of HIV-1 replication with different potencies. It appeared to inhibit HIV-1 RT activity, HIV-1 particle attachment and cell fusion. These are essential activities for viral transmission and replication. (c) 2005 Elsevier Inc. All rights reserved.

Anti-HIV Activities of the Compounds Isolated from Polygonum cuspidatum and Polygonum multiflorum

The 70% EtOH extract of Polygonum cuspidatum showed inhibitory action against HIV-1-induced syncytium formation at non-cytotoxic concentrations in vitro with a 50% effective concentration (EC50) of 13.94 +/- 3.41 mu g/mL. Through bioactivity-guided fractionation, 20 phenolic compounds, including eight stilbenoids, were isolated from the roots of Polygonum cuspidatum, and their anti-HIV-1 activities were evaluated. Results showed that compounds 1, 13, 14, and 16 demonstrated fairly strong antiviral activity against HIV-1-induced cytopathic effects in C8166 lymphocytes at non-cytotoxic concentrations, with EC50 values of 4.37 +/- 1.96 mu g/mL, 19.97 +/- 5.09, 14.4 +/- 1.34 mu g/mL, and 11.29 +/- 6.26 mu g/mL and therapeutic index (TI) values of 8.12, > 10.02, > 13.89, and > 17.71, respectively. Other compounds showed either weak or no effects. Compound 6 also showed weak inhibition (153.42 +/- 19.25 mu g/mL); however, it possesses very good water solubility and showed almost no cytotoxicity (> 2000 mu g/mL), therefore achieving a fairly good TI (13.04). The activities of the two compounds (3 and 18) from Polygonum multiflorum were also assayed. The relationship between molecular structures and their bioactivities was also discussed.

Evaluation of estrogenic activities and mechanism of action of perfluorinated chemicals determined by vitellogenin induction in primary cultured tilapia hepatocytes

Perfluorochemicals (PFCs) are emerging persistent organic pollutants (POPs) and are widely present in the environment, wildlife and humans. Recently, reports have suggested that PFCs may have endocrine-disrupting activities. In the present study, we have developed a non-competitive enzyme-linked immunosorbent assay (ELISA) method to investigate estrogenic activities of selected PFCs using vitellogenin (VTG) induction in primary cultured hepatocytes of freshwater male tilapia (Oreochromis niloticus). Cultured hepatocytes were exposed to various concentrations of perfluorooctanyl sulfonate (PFOS), pentadecafluorooctanoic acid (PFOA), 1H, 1H, 2H, 2H-nonafluoro-1-hexanol (4:2 FTOH), 1H, 1H, 2H, 2H-perfluorooctanol (6:2 FTOH) and 1H, 1H, 2H, 2H-perfluoro-1-decanol (8:2 FTOH) for 48h, while 17 beta-estradiol (E2) and 4-nonylphenol (4-NP) were used as positive controls. A dose-dependent induction of VTG was observed in E2-, 4-NP-, PFOS-, PFOA- and 6:2 FrOH-treated cells, whereas VTG levels remained unchanged in the 4:2 FTOH and 8:2 FTOH exposure groups at the concentrations tested. The estimated 48-h EC50 values for E2,4-NP, PFOS, PFOA and 6:2 FTOH were 4.7 x 10(-7), 7.1 x 10(-6), 1.5 x 10(-5), 2.9 x 10(-5) and 2.8 x 10(-5) M, respectively. In the time-course study, significant VTG induction took place at 24 h (E2), 6 It (4-NP), 48 It (PFOS), 48 It (PFOA), 72 It (4:2 FTOH), 12 h (6:2 FTOH), 72 h (8:2 FTOH), and increased further after 96 It of exposure. Co-exposure to binary mixtures of individual PFCs and E2 for 48 It significantly inhibited E2-induced hepatocellular VTG production in a dose-dependent manner except for 4:2 FTOH. The estimated 48-h IC50 (concentration of a compound that elicits 50% inhibition of maximally E2-induced VTG) values for PFOS, PFOA, 6:2 FTOH and 8:2 FTOH were 3.1 x 10(-7), 5.1 X 10(-7), 1.1 X 10(-6) and 7.5 x 10(-7) M, respectively. In order to further investigate the estrogenic mechanism of PFCs, the hepatocytes were co-exposed to binary mixtures of individual chemicals (E2,4-NP, PFOS, PFOA and 6:2 FTOH) and the known estrogen receptor inhibitor tamoxifen for 48 h; tamoxifen significantly inhibited the ability of these chemicals to stimulate vitellogenesis. The overall results demonstrated that PFOS, PFOA and FTOHs have estrogenic activities and that exposure to a combination of E2 and PFCs produced anti-estrogenic effects. The results of the estrogen receptor inhibition assay further suggested that the estrogenic effect of PFCs may be mediated by the estrogen receptor pathway in primary cultured tilapia hepatocytes. (c) 2007 Elsevier B.V. All rights reserved.

O uso clínico dos anti-inflamatórios não esteróides

Projeto de Pós-Graduação/Dissertação apresentado à Universidade Fernando Pessoa como parte dos requisitos para obtenção do grau de Mestre em Ciências Farmacêuticas

Collective action and individual choice: rethinking how we regulate narcotics and antibiotics.

Governments across the globe have squandered treasure and imprisoned millions of their own citizens by criminalising the use and sale of recreational drugs. But use of these drugs has remained relatively constant, and the primary victims are the users themselves. Meanwhile, antimicrobial drugs that once had the power to cure infections are losing their ability to do so, compromising the health of people around the world. The thesis of this essay is that policymakers should stop wasting resources trying to fight an unwinnable and morally dubious war against recreational drug users, and start shifting their attention to the serious threat posed by our collective misuse of antibiotics.

Integrating simultaneous prosocial and antisocial behavior into theories of collective action.

Trust and cooperation constitute cornerstones of common-pool resource theory, showing that "prosocial" strategies among resource users can overcome collective action problems and lead to sustainable resource governance. Yet, antisocial behavior and especially the coexistence of prosocial and antisocial behaviors have received less attention. We broaden the analysis to include the effects of both "prosocial" and "antisocial" interactions. We do so in the context of marine protected areas (MPAs), the most prominent form of biodiversity conservation intervention worldwide. Our multimethod approach relied on lab-in-the-field economic experiments (n = 127) in two MPA and two non-MPA communities in Baja California, Mexico. In addition, we deployed a standardized fishers' survey (n = 544) to verify the external validity of our findings and expert informant interviews (n = 77) to develop potential explanatory mechanisms. In MPA sites, prosocial and antisocial behavior is significantly higher, and the presence of antisocial behavior does not seem to have a negative effect on prosocial behavior. We suggest that market integration, economic diversification, and strengthened group identity in MPAs are the main potential mechanisms for the simultaneity of prosocial and antisocial behavior we observed. This study constitutes a first step in better understanding the interaction between prosociality and antisociality as related to natural resources governance and conservation science, integrating literatures from social psychology, evolutionary anthropology, behavioral economics, and ecology.

Epilobium parviflorum Schreb. - in vitro study of biological action

Epilobium parviflorum Schreb. (Onagraceae) is used for the treatment of benign prostatic hyperplasia (BPH), which is regarded as an endocrine disorder caused by age-related hormone imbalance and increased oxidative damage [1,2,3]. Epilobium can moderate the obstructive and the irritative symptoms of BPH [1] but its biological action is not entirely identified. E. parviflorum is rich in phytosterols, flavonoids (myricetin, quercetin, kaempferol and their glycosides), phenolic acids, catechins, ellagi- and gallotannins [4]. The potential biological effects of Epilobium parviflorum Schreb. have been investigated, in respect to its antioxidant, anti-inflammatory, enzyme-inhibitory and anti-androgenic effect. The whole-plant water extract showed higher antioxidant effect (IC50=1.65±0.05µg/mL) in DPPH assay than Trolox or ascorbic acid and inhibited the lipid peroxidation examined in TBA assay (IC50=2.31±0.18mg/mL). In concentrations 0.20-15.00µg/mL the extract possessed a protective effect comparable to catalase enzyme (2500 IU/mL), against oxidative damage generated on fibroblast cells. The examination of the COX-inhibitory effect showed that E. parviflorum had an anti-inflammatory effect (IC50=1.38±0.08µg/mL). Investigation of steroid receptor binding ability and the aromatase enzyme-inhibition showed negative results in the concentration range examined.

Influence of Formulation Factors on PpIX Production and Photodynamic Action of Novel ALA-loaded Microparticles

A novel 5-aminolevulinic acid (ALA)-containing microparticulate system was produced recently, based on incorporation of ALA into particles prepared from a suppository base that maintains drug stability during storage and melts at skin temperature to release its drug payload. The novel particulate system was applied to the skin of living animals, followed by study of protoporphyrin IX (PpIX) production. The effect of formulating the microparticles in different vehicles was investigated and also the phototoxicity of the PpIX produced using a model tumour. Particles formulated in propylene glycol gels (10% w/w ALA loading) generated the highest peak PpIX fluorescence levels in normal mouse skin. Peak PpIX levels induced in skin overlying subcutaneously implanted WiDr tumours were significantly lower than in normal skin for both the 10% w/w ALA microparticles alone and the 10% w/w ALA microparticles in propylene glycol gels during continuous 12 h applications. Tumours not treated with photodynamic therapy continued to grow over the 17 days of the anti-tumour study. However, those treated with 12 h applications of either the 10% w/w ALA microparticles alone or the 10% w/w ALA microparticles in propylene glycol gel followed by a single laser irradiation showed no growth. The gel formulation performed slightly better once again, reducing the tumour growth rate by approximately 105%, compared with the 89% reduction achieved using particles alone. Following the promising results obtained in this study, work is now going on to prepare particle-loaded gels under GMP conditions with the aim of initiating an exploratory clinical trial.

Towards Educational Inclusion in a Contested Society: From Critical Reflection to Cultural Action

This paper is written by democratic educators who stand for the idea that is it worth developing, through classrooms and schools, a socially just (egalitarian), anti-discriminatory society where interdependent relationships are valued. This paper significantly develops some of the ideas explored in the authors’ earlier contribution concerned with progress in Northern Ireland towards educational inclusion, and how this might more effectively advance in a post-conflict transforming society. In particular, the paper poses the ‘so what’ question, and it responds by exploring the practical implications of six key ideas thought essential for transforming learning environments supportive of cultural diversity, equity and excellence for all. In addition, it includes examples of how school staff, along with collaborating partners, might utilize these key principles in order to facilitate school improvement.

Prising open the black box: Critical realism, action research and social work

There is a growing interest in critical realism and its application to social work. This article makes a case for adopting this philosophical position in qualitative social work research. More specifically, it suggests that there is a concordance between critical realist premises and action research with its cyclical inquiry and advancement of social change. This combination of philosophy and method, it is argued, promotes anti-oppressive social work research and illuminates the processes shaping outcomes in programme evaluations. Overall, the article underscores the importance of 'depth' in qualitative inquiry by conceiving the social world in terms of five interlacing, social domains.

MODULATORY ACTION OF HELICOBACTER-PYLORI ON HISTAMINE-RELEASE FROM MAST-CELLS AND BASOPHILS IN-VITRO

Helicobacter pylori is important in the aetiology of peptic ulceration. Despite inducing an inflammatory response in the mucosa, the organism persists, suggesting that it has efficient protective mechanisms. Some bacterial and viral products modulate histamine secretion from inflammatory cells. Therefore, this study examined the modulatory effects of H. pylori preparations on histamine release from rat peritoneal mast cells and human basophils. Eleven clinical isolates of H. pylori were prepared in different ways: as whole washed bacteria, washed sonicated bacteria, and formalin-killed bacteria, and as outer-membrane and lipopolysaccharide (LPS) extracts. Histamine release from mast cells or basophils was not elicited by any of these bacterial preparations alone. However, when mixed with various secretory stimulants, the bacterial preparations caused inhibition of histamine release from rat mast cells (calcium ionophore A23187, compound 48/80, concanavalin A, anti-rat IgE) and human basophils (A23187, N-formyl Met-Leu-Phe). The degree of inhibition ranged from 48 % to 97 %. These results indicate that H. pylori exerts an inhibitory effect on cells of the immune system that contributes to its persistence within the gastric mucosa.