Role of Aryl Hydrocarbon Receptor (AhR) in the Regulation of Immunity and Immunopathology During Trypanosoma cruzi Infection.

Resistance to Trypanosoma cruzi infection is dependent on a rapid induction of Th1-type and CD8+ T cell responses that should be promptly balanced to prevent immunopathology. T. cruzi-infected B6 mice are able to control parasite replication but show a limited expansion of Foxp3+regulatory T (Treg) cells that results in the accumulation of effector immune cells and the development of acute liver pathology. AhR is a ligand-activated transcription factor that promotes Treg cell development and suppression of pro-inflammatory cytokine production in dendritic cells, altering the course of adaptive immune response and the development of immunopathology. Here, we used different AhR-dependent activation strategies aiming to improve the Treg response, and B6 congenic mice carrying a mutant AhR variant with low affinity for its ligands (AhRd) to evaluate the role of AhR activation by natural ligands during experimental T. cruzi infection. The outcome of TCDD or 3-HK plus ITE treatments indicated that strong or weak AhR activation before or during T. cruzi infection was effective to regulate inflammation improving the Treg cell response and regularizing the ratio between CD4+ CD25- to Treg cells. However, AhR activation shifted the host-parasite balance to the parasite replication. Weak AhR activation resulted in Treg promotion while strong activation differentially modulated the susceptibility and resistance of cell death in activated T and Treg cells and the increase in TGF-ß-producing Treg cells. Of note, T. cruzi-infected AhRd mice showed low levels of Treg cells associated with strong Th1-type response, low parasite burden and absence of liver pathology. These mice developed a Treg- and Tr1-independent mechanism of Th1 constriction showing increased levels of systemic IL-10 and IL-10-secreting CD4+ splenocytes. In addition, AhR activation induced by exogenous ligands had negative effects on the development of memory CD8+ T cell subsets while the lack/very weak activation in AhRd mice showed opposite results, suggesting that AhR ligation restricts the differentiation of memory CD8+T cell subsets. We propose a model in which a threshold of AhR activation exists and may explain how activation or inhibition of AhR-derived signals by infection/inflammation-induced ligands, therapeutic interventions or exposure to pollutants can modulate infections/diseases outcomes or vaccination efficacy.

Climatic Droplet Keratopathy in Argentina: Involvement of Environmental Agents in Its Genesis Which Would Open the Prospect for New Therapeutic Interventions.

Climatic droplet keratopathy (CDK) is a degenerative corneal disease of unknown etiology. We described CDK for the first time in Latin America in the Argentinean Patagonia (El Cuy). A deeper knowledge of CDK pathogenic mechanisms will provide new therapeutic strategies. For that reason we investigated the prevalence of CDK in El Cuy and its existence in other 3 provinces with similar climate. Patients eyes were examined, habits throughout lives were inquired about, and serum ascorbate (sAA) was determined. All individuals work outdoors for most of the day. All regions had normal O3 levels. Individuals from regions 1, 2, and 3 had very low consumption of vegetables/fruits and low sAA levels. Conversely, region 4 individuals had balanced diet and higher sAA concentrations. CDK was only found in region 3 where individuals had partial deficiency of sAA and did not use eye protection. No CDK was found in regions 1 and 2 where individuals had similar work activities and dietary habits to those in region 3 but wear eye protection. No disease was found in region 4 where individuals work outdoors, have balanced diet, and use eye protection. To summarize, the CDK existence was related not only to climate but also to the dietary habits and lack of protection from sunlight.

Ácido ascórbico: desde la química hasta su crucial función protectiva en ojo / Ascorbic acid: from chemistry to its crucial protective role in the eye

La Vitamina C o ácido L-ascórbico (AA), es una vitamina esencial y un importante agente antioxidante hidrosoluble, que se sintetiza químicamente a partir de la glucosa, mediante una serie de reacciones enzimáticas, siendo la L-gulono-g-lactona oxidasa (GLO) la última enzima involucrada. La incapacidad de sintetizar AA por ausencia de GLO ocurrió hace cientos de millones de años y se manifiesta sólo en algunas especies. La degradación del AA se lleva a cabo mediante procesos oxidativos que involucran la hidrólisis del anillo lactona para producir ácido 2,3-dicetogulónico (DCG), que posteriormente se degrada por decarboxilación, generando productos coloreados, encontrados en algunas patologías oculares. Entre las diferentes propiedades del AA cabe mencionar su capacidad de absorber radiación ultravioleta (RUV) y evitar el daño fotoquímico en órganos expuestos. En humanos, y en algunos animales (cobayos, ciertos primates, etc.) el humor acuoso tiene mayor concentración de AA que el plasma. Esto responde a un mecanismo de transporte activo especializado en el cuerpo ciliar que se encarga de transportar el AA desde la sangre hacia el humor acuoso y desde allí al epitelio corneal, transformando a la córnea en la estructura del ojo responsable de la mayor absorción de RUV.

Vitamin C or L-ascorbic acid (AA) is an essential vitamin and a water soluble important antioxidant agent, chemically synthesized from glucose, by enzymatic reactions, being the L-gulono-g-lactone oxidase (GLO) the last enzyme involved. The inability to synthesize AA by some species, due to the absence of GLO seems to have happened hundreds of millions years ago. The degradation of the AA is carried out by oxidative processes which involve the hydrolysis of the lactona ring to produce 2,3-diketogulonic acid (DCG) that is later degraded by decarboxilation, generating colored products, found in some ocular pathologies. Among the different properties of the AA, it is worth mentioning its capacity to absorb ultraviolet radiation (RUV) and to avoid the photochemical damage of exposed tissues. In humans and in some animals (guinea pigs, primates, etc) the aqueous humor has bigger concentrations of AA than plasma. This responds to a mechanism of specialized active transport in the ciliary body that transfers AA from the blood towards the aqueous humor and from there to the corneal epithelium, transforming the cornea into the structure of the eye responsible for the biggest absorption of RUV.

Cytokine polymorphisms in patients with pemphigus.

The aim of this study was to assess whether tumor necrosis factor alpha (TNF-alpha), transforming growth factor beta1 (TGF-beta1) and interleukin-10 (IL-10) polymorphisms are among the factors influencing the development of pemphigus. Whole blood from 20 patients with pemphigus and 24 control subjects was taken. Genomic DNA was obtained and cytokine genotyping for IL-10 (-1082 G/A; -819 C/T), TGFB1 (codon 10 C/T, codon 25 G/C) and TNFA (-308 G/A) was performed using the ARMS-PCR method. The distribution of IL-10 (-819) alleles was significantly different between the pemphigus and control groups (P=0.009). In particular, allele T was associated with the disease (OR 3.291, 95% CI 1.350-8.020). Similar results were observed when only pemphigus vulgaris (PV) patients were analyzed (P=0.012, OR 3.410, 95% CI 1.346-8.639). An increased frequency of the low producer IL-10 haplotype (-1082/-819 A/T) in patients with pemphigus compared with controls was observed (OR 2.714, 95% CI 1.102-6.685) and this association was also significant when only PV patients were considered (OR 2.667, 95% CI 1.043-6.816). There were no differences between patients and controls in the frequency of any other gene polymorphism analyzed. The increased frequency of the low producer IL-10 haplotype (-1082 /-819 A/T) suggest that the carriage of this haplotype might predispose to pemphigus or the high and intermediate producer haplotypes may be protective factors. The prevalence of the allele IL-10 (-819 T) in pemphigus patients cannot be explained by the current hypothesis, according to which a particular allele of the gene is associated with a different level of cytokine production and therefore affects the predisposition to a particular disease. However, this cytokine polymorphism might be linked to an unknown susceptibility factor.

Inmunodeficiencia común variable: hallazgos recientes sobre anormalidades celulares / Common variable immunodeficiency: recent findings in cellular abnormalities

La Inmunodeficiencia Común Variable (IDCV), también llamada hipogammaglobulinemia adquirida o disgammaglobulinemia, es un grupo heterogéneo de desórdenes que afecta a los linfocitos (L)T y a los LB. Constituye uno de los principales síndromes de deficiencia de anticuerpos, presenta una pérdida o disminución de la respuesta inmune humoral a antígenos específicos, particularmente polisacáridos capsulares bacterianos. Estos pacientes tienen una alta susceptibilidad a infecciones del tracto respiratorio y la IDCV tiene una estrecha relación con patologías tales como deficiencias de IgA y subclases de IgG. El objetivo de esta revisión es actualizar los conocimientos de este grupo de desórdenes inmunológicos, con especial énfasis en los nuevos criterios utilizados para el diagnóstico y seguimiento

Inmunodeficiencia común variable: hallazgos recientes sobre anormalidades celulares / Common variable immunodeficiency: recent findings in cellular abnormalities

La Inmunodeficiencia Común Variable (IDCV), también llamada hipogammaglobulinemia adquirida o disgammaglobulinemia, es un grupo heterogéneo de desórdenes que afecta a los linfocitos (L)T y a los LB. Constituye uno de los principales síndromes de deficiencia de anticuerpos, presenta una pérdida o disminución de la respuesta inmune humoral a antígenos específicos, particularmente polisacáridos capsulares bacterianos. Estos pacientes tienen una alta susceptibilidad a infecciones del tracto respiratorio y la IDCV tiene una estrecha relación con patologías tales como deficiencias de IgA y subclases de IgG. El objetivo de esta revisión es actualizar los conocimientos de este grupo de desórdenes inmunológicos, con especial énfasis en los nuevos criterios utilizados para el diagnóstico y seguimiento (AU)

Up-regulation of the chemokine CCL21 in the skin of subjects exposed to irritants.

BACKGROUND: Expression of murine CCL21 by dermal lymphatic endothelial cells (LEC) has been demonstrated to be one of the most important steps in Langerhans cell emigration from skin. Previously, our group and others have found that this chemokine is up-regulated in different human inflammatory skin diseases mediated by diverse specific immune responses. This study was carried out to investigate the involvement of CCL21 in human skin after challenge with irritant agents responsible for inducing Irritant Contact Dermatitis (ICD). RESULTS: Eleven normal individuals were challenged with different chemical or physical irritants. Two patients with Allergic Contact Dermatitis (ACD) were also challenged with the relevant antigen in order to have a positive control for CCL21 expression. Macroscopic as well as microscopic responses were evaluated. We observed typical ICD responses with mostly mononuclear cells in perivascular areas, but a predominance of polymorphonuclear cells away from the inflamed blood vessels and in the epidermis at 24 hours. Immunohistochemical studies showed up-regulation of CCL21 by lymphatic endothelial cells in all the biopsies taken from ICD and ACD lesions compared to normal skin. Kinetic study at 10, 48, 96 and 168 hours after contact with a classical irritant (sodium lauryl sulphate) showed that the expression of CCL21 was increased in lymphatic vessels at 10 hours, peaked at 48 hours, and then gradually declined. There was a strong correlation between CCL21 expression and the macroscopic response (r = 0.69; p = 0.0008), but not between CCL21 and the number of infiltrating cells in the lesions. CONCLUSIONS: These results provide new evidence for the role of CCL21 in inflammatory processes. Since the up-regulation of this chemokine was observed in ICD and ACD, it is tempting to speculate that this mechanism operates independently of the type of dermal insult, facilitating the emigration of CCR7+ cells.

Secondary lymphoid tissue chemokine (CCL21) is upregulated in allergic contact dermatitis.

Chemokines are important players in the development of allergic contact dermatitis (ACD). The participation of secondary lymphoid tissue chemokine (CCL21) is essential in the induction of the disease due to its expression in lymphatic vessels and in secondary lymphoid organs. Since there is no information about its participation during the effector phase of ACD, we studied this chemokine in patients already diagnosed with ACD, who were challenged with the relevant positive and negative (control) antigens. All patients showed a specific antigen-induced immune response characterized by early expression of inflammatory markers in blood endothelial cells followed by dermal accumulation of mononuclear cells with an important increase in infiltration of CXCR3+ but not of CCR7+ cells. In situ hybridization and immunohistochemistry showed low levels of CCL21 in lymphatic vessels at 2 h, whereas they were significantly increased at 10 and 48 h in all positive patch tests. In contrast, very low expression of this chemokine was observed in skin biopsies from the control site at 48 h. In addition, Langerin+ cells, which were present in dermis from positive patch tests at 2 h, were diminished in number at 10 and 48 h, but a significant number of those cells was still present in dermal areas of the control site at 48 h. We demonstrate for the first time that CCL21, a constitutively expressed chemokine, is strongly upregulated in human lymphatic vessels during a Th1/Tc1 allergic inflammatory response. This can provide the signal required for CCR7+ cells to leave the skin through CCL21-positive lymphatic vessels.

Early inflammatory markers in elicitation of allergic contact dermatitis.

BACKGROUND: Allergic Contact Dermatitis (ACD) is regarded as a T-cell-mediated delayed-type hypersensitivity reaction. We studied the kinetics of the expression of CS-1 fibronectin, thymus and activation-regulated chemokine (CCL17/ TARC) and different chemokine receptors (CR) in skin biopsies from individuals suffering from back problems, with the antigen responsible of their contact dermatitis and an irrelevant antigen. METHODS: Samples were taken at 2, 10, and 48 hours for histological and immunohistochemical studies using monoclonal antibodies against human CS-1 fibronectin, CCL17, CD3, CD68, CD49d, CXCR3, CCR5, and CCR3. RESULTS: At positive antigen stimulated sites there was an early expression of CS-1 fibronectin (2 hours), followed by CCL17 and a later accumulation of alplha4/beta1+ (CD49d), CD3+, CD68+, CXCR3+ and CCR5+ mononuclear cells. At 48 hours, approximately 59 % of infiltrating cells were CXCR3+, 42% CCR5+, and only 14 % CCR3+. CONCLUSIONS: These results showed for the first time a very early expression of CS-1 fibronectin which preceded production of CCL17 in blood endothelial cells (BCEs) from patients' skin with ACD. The role of these molecules in recruitment of monocytes and effector T cells in ACD is discussed.