Plasticity of neutrophils reveals modulatory capacity

Neutrophils are widely known as proinflammatory cells associated with tissue damage and for their early arrival at sites of infection, where they exert their phagocytic activity, release their granule contents, and subsequently die. However, this view has been challenged by emerging evidence that neutrophils have other activities and are not so short-lived. Following activation, neutrophil effector functions include production and release of granule contents, reactive oxygen species (ROS), and neutrophil extracellular traps (NETs). Neutrophils have also been shown to produce a wide range of cytokines that have pro- or anti-inflammatory activity, adding a modulatory role for this cell, previously known as a suicide effector. The presence of cytokines almost always implies intercellular modulation, potentially unmasking interactions of neutrophils with other immune cells. In fact, neutrophils have been found to help B cells and to modulate dendritic cell (DC), macrophage, and T-cell activities. In this review, we describe some ways in which neutrophils influence the inflammatory environment in infection, cancer, and autoimmunity, regulating both innate and adaptive immune responses. These cells can switch phenotypes and exert functions beyond cytotoxicity against invading pathogens, extending the view of neutrophils beyond suicide effectors to include functions as regulatory and suppressor cells.

Efeitos das microcistinas sobre funções de neutrófilos / Effects of microcystins on functions of neutrophils

Microcistinas (MCs) são heptapeptídeos cíclicos produzidos por cianobactérias e possuem potente hepatotoxicidade e atividade promotora de tumor. Em intoxicações agudas induzidas por MCs ocorre infiltração leucocitária no foco inflamatório. Embora os mecanismos de hepatotoxicidade não são claros, o recrutamento de neutrófilos no fígado pode contribuir ao dano tecidual e desenvolvimento tumoral causados por xenobióticos. O objetivo dessa tese foi investigar os efeitos de três estruturalmente distintas MCs (MC-LA, MC-YR e MC-LR) nas seguintes funções de neutrófilos: síntese e expressão de moléculas de adesão, rolamento, adesão, migração e liberação de citocinas e de ROS. Nos ensaios de migração em bolsa de ar, as três MCs induziram similarmente a migração leucócitos in vivo em tecido subcutâneo de ratos e diferencialmente a secreção citocinas pró-inflamatórias (CINC, IL-1β, TNF-α, VEGF-α e MIP) no exsudato. Concentrações elevadas de CINC-2αβ foram encontradas nos exsudatos inflamatórios de animais após injeção de MC-LA, MC-LR ou MC-YR. MIP-2 elevou-se apenas em exsudatos de animais expostos a MC-LR. Não foram observadas alterações em secreção de IL-1β, TNF-α e VEGF-α...

Advanced glycosylated end products-mediated activation of polymorphonuclear neutrophils in diabetes mellitus and associated oxidative stress.

Two important consequences of hyperglycemia in diabetes are development of oxidative stress and formation of advanced glycation end products (AGE) which are known to be associated with diabetic complications. Relationship between AGE formation and development of oxidative stress (OS) is yet to be established. In the present study, the involvement of AGE in PMN-mediated ROS generation and the associated OS were investigated in type 2 diabetic mellitus (DM) patients. We assessed OS parameters (serum MDA, FRAP and GSH), PMN oxidative functions (respiratory burst and superoxide production) and total serum AGE in 90 subjects divided equally in three groups--control group, Group I consisting of type 2 diabetic patients without microvascular complications and Group II consisting of type 2 diabetic patients with microvascular complications. PMNs isolated from both groups (I and II) exhibited higher level of respiratory burst (RB) and produced increased amount of superoxide anion as compared to the controls. The increase was more pronounced in diabetes with complications, as compared to those without. Serum malondialdehyde (MDA) level was elevated, whereas glutathione (GSH) and ferric reducing ability of plasma (FRAP) levels were significantly reduced in diabetes as compared to the controls, suggesting the presence of oxidative stress in DM. A positive correlation between PMN oxidative function and OS parameters suggested the involvement of PMN in the development of OS in DM. Serum AGE level was also elevated in diabetic groups as compared to the controls. Further, the positive correlation between serum AGE level and PMN oxidative function suggested the involvement of AGE in increased RB and generation of reactive oxygen species (ROS) by resting diabetic PMN. The results of the study indicate that AGE-PMN interaction possibly upregulates NADPH oxidase, leading to enhanced ROS generation and thus contributes to the pathogenesis in diabetes.

Sepsis: emerging role of nitric oxide and selectins

Sepse – um estado de infecção bacteriana sistêmica – frequentemente leva à falência múltipla de órgãos e associa-se a altos índices de mortalidade, apesar de progressos recentes no manejo de pacientes em unidades de terapia intensiva. Muitos dos efeitos maléficos associados à sepse são atribuídos a uma resposta inflamatória patologicamente ampliada que leva a recrutamento neutrofílico e ativação das moléculas de adesão do grupo das selectinas, durante as fases iniciais do processo . O óxido nítrico e sua diversas isoformas também foram implicados nas diversas manifestações vasculares da sepse como participantes diretos da toxicidade celular. Esta revisão descreve o papel das selectinas e do óxido nítrico em situações clínicas e experimentais de sepse, bem como os respectivos efeitos de processos terapêuticos de bloqueio.

Activación de la respuesta inmune innata y específica en los pacientes con sindrome urémico hemolítico: papel dual a traves de la paticipacion en los mecanismos pagogenicos y protectores / Activation of innate and specific immune responses in hemolytic uremic syndrome (HUS)-patients

The central role of the immune system is the preservation of the health against several pathogenic microbes and injury agents. However, on special conditions defensive mechanisms triggered towards the foreign agent can damage the host. Clinical and experimental evidence indicate that inflammatory reaction triggered by the main components of Shiga toxin (Stx)-producing Escherichia coil (STEC), participate in the evolution to the complete form of HUS. When children are diagnosed of HUS, they present evidence that have suffered a very strong and early inflammatory response. These features include: the presence of a marked neutrophilia, the polymorfonuclear leucocytes (PMN) are "deactivated or exhausted" and the monocytes are differentiated towards an inflammatory phenotype (CD14-reduced and CD16-enhanced membrane expression). In addition, HUS-patients show a marked reduction in the absolute and relative number of leucocytes carrying the receptor (CX3CR1) for the chemokine "Fractalkine" (FKN, CX3CL1), which are the classic monocytes and Natural Killer cells (NK). All these cells express a high cytotoxic potencial. The chemokine FKN is expressed in endothelial and epithelial renal cells, and is involved in the pathogenic mechanism of different nephropathies. Noteworthy, we found a significant correlation between the severity of the renal damage (as days of anuria) and the alterations described above. Finally, the protective role of specific immune response, mainly through the antibody production with Stx-neutralizing capacity, is discussed.

Spontaneous neutrophil activation in HTLV-1 infected patients

Human T cell lymphotropic Virus type-1 (HTLV-1) induces lymphocyte activation and proliferation, but little is known about the innate immune response due to HTLV-1 infection. We evaluated the percentage of neutrophils that metabolize Nitroblue tetrazolium (NBT) to formazan in HTLV-1 infected subjects and the association between neutrophil activation and IFN-gamma and TNF-alpha levels. Blood was collected from 35 HTLV-1 carriers, from 8 patients with HAM/TSP (HTLV-1- associated myelopathy); 22 healthy individuals were evaluated for spontaneous and lipopolysaccharide (LPS)-stimulated neutrophil activity (reduction of NBT to formazan). The production of IFN-gamma and TNF-alpha by unstimulated mononuclear cells was determined by ELISA. Spontaneous NBT levels, as well as spontaneous IFN-gamma and TNF-alpha production, were significantly higher (p<0.001) in HTLV-1 infected subjects than in healthy individuals. A trend towards a positive correlation was noted, with increasing percentage of NBT positive neutrophils and levels of IFN-gamma. The high IFN-gamma producing HTLV-1 patient group had significantly greater NBT than healthy controls, 43±24 percent and 17±4.8 percent respectively (p< 0.001), while no significant difference was observed between healthy controls and the low IFN-gamma-producing HTLV-1 patient group (30±20 percent). Spontaneous neutrophil activation is another marker of immune perturbation resulting from HTLV-1 infection. In vivo activation of neutrophils observed in HTLV-1 infected subjects is likely to be the same process that causes spontaneous IFN-gamma production, or it may partially result from direct IFN-gamma stimulation.

Development of an experimental model of neutrophilic pulmonary response induction in mice

BACKGROUND: Several lung diseases are characterized by a predominantly neutrophilic inflammation. A better understanding of the mechanisms of action of some drugs on the airway inflammation of such diseases may bring advances to the treatment. OBJECTIVE: To develop a method to induce pulmonary neutrophilic response in mice, without active infection. METHODS: Eight adult Swiss mice were used. The study group (n = 4) received an intranasal challenge with 1 x 10(12) CFU/ml of Pseudomonas aeruginosa (Psa), frozen to death. The control group (n = 4) received an intranasal challenge with saline solution. Two days after the intranasal challenge, a bron¡choalveolar lavage (BAL) was performed with total cell and differential cellularity counts. RESULTS: The total cell count was significantly higher in the group with Psa, as compared to the control group (median of 1.17 x 10(6) and 0.08 x 10(6), respectively, p = 0.029). In addition to this, an absolute predominance of neutrophils was found in the differential cellularity of the mice that had received the Psa challenge. CONCLUSIONS: The model of inducing a neutrophilic pulmonary disease using frost-dead bacteria was successfully developed. This neutrophilic inflammatory response induction model in Swiss mice lungs may be an important tool for testing the anti-inflammatory effect of some antimicrobial drugs on the inflammation of the lower airways.

Tumor necrosis factor accounts for the neutrophil emigration activity released by cultured malignant fibrous histiocytoma cells

Cultured malignant fibrous histiocytoma (MFH) cells obtained from a spontaneous and transplantable rat tumor were studied for their ability to release tumor necrosis factor (TNF) and a factor which induces neutrophil migration in vivo. MFH cells obtained from 7-day cultures spontaneously released both activities into the supernatant (TNF: 36 ñ 9 iu tnf/ml supernatant, N = 3; neutrophil chemoattractant factor: control, Medium ip: 6 ñ 1 x 10**6; MFH supernatant: 18 ñ 1 x 106 neutrophils/cavity, H = 5). these releases were enhanced by treating MFH cells with LPS (TNF; 61 percent; neutrophil chemoattractant factor: 46 percent) and were abolished by the glucocorticoid dexamethasone (TNF: 68 percent; neutrophil chemoattractant factor: 100 percent). Anti-TNF antiserum abolished the neutrophil chemoattractant activity of the supernatants (95 percent). The release of TNF or neutrophil chemoattractant activity was reduced in cells obtained from older cultures (14 and 21 days) (TNF: 7-day culture, 36 ñ 9;14-day culture, 19ñ2;21-day culture, 19ñ 1 IU of TNF/ml; neutrophil chemoattractant activity: 7-day culture, 18 ñ 1.6; 14-day culture, 13 ñ 3;28-day culture, 8 ñ 1 x 10**6 neutrophils/cavity). The predominant cells present in 7-day cultures of MFH were histiocyte-like cells as determined by nonspecific esterase methods. The number of these cells decreased as the cultures aged (7-day culture, 71 percent; 14-day culture, 5 percent; 21-day culture, 0 percent)...

Disminución de linfocitos T supresores y activación de monocitos y neutrófilos durante la reacción inmediata del asma-inducida por ejercicio / Lymphocyte T supressors dicrease and monocyte and neutrophil activation during the early reaction of exercise induced asthma

Durante la broncoconstricción inducida por el ejercicio (AIE) en individuos asmáticos se producen cambios cuantitativos y cualitativos de los leucocitos en sangre periférica. Para estudiar la participación de células inmunes y accesorias de la reacción inflamatoria en el AIE, analizamos las modificaciones de las subpoblaciones de linfocitos T y de la expresión de los antígenos de histocompatibilidad clase II (la) en monocitos, además de la participación de los receptores para el tercer factor del complemento (C36) mediante su expresión en monocitos y su adhesión y consecuente activación en neutrófilos. Se estudió 20 pacientes asmáticos alérgicos, de los cuales 11 presentaron broncoconstricción después de una prueba de ejercicio estandarizada. En todos los individuos estudiados se produjo, 5 min después del ejercicio, un aumento significativo de los leucocitos sanguíneos totales y de los neutrófilos, linfocitos y monocitos. Los basófilos y eosinófilos aumentaron sólo en los AIE (+). También este grupo presentó eosinófilos más altos desde el nivel inicial. En los individuos con AIE (+) el aumento inicial de los linfocitos a los 5 min se produce a expensas de los linfocitos T supresores (CD8) los que luego comienzan a disminuir hasta alcanzar valores significativamente menores que el inicial a los 60 min después del ejercicio. Esto lleva a un aumemto de la relación CD4/CD8 a nivel periférico, que es simultáneo con el aumento en la expresión de los antígenos Ia en monocitos observados en los AIE (+). Además en estos pacientes se encontró un aumento en la expresión de los receptores C3b en monocitos y en la producción de radical superóxido por neutrófilos estimulados con zimusán y complemento, desde el momento que se inicia la broncoconstricción hasta los 60 min después del ejercicio. Estos hallazgos sugieren que en los asmáticos con AIE (+) se producen cambios en las células inmunocompetentes que pudieran estar relacionados con la participación de células inflamatorias y su eventual manifestación como hiperactividad bronquial