Investigação da expressão gênica diferencial em resposta aos efeitos da proteína anti-inflamatória Anexina A1 nas células de carcinoma de colo de útero

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

Dysregulation of Anti-Inflammatory Annexin A1 Expression in Progressive Crohns Disease

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)

Deregulation of Annexin-A1 and Galectin-1 Expression in Precancerous Gastric Lesions: Intestinal Metaplasia and Gastric Ulcer

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

Inflammation and cancer: role of Annexin A1 and FPR2/ALX in proliferation and metastasis in human laryngeal squamous cell carcinoma

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

The intricate role of mast cell proteases and the annexin A1-FPR1 system in abdominal wall endometriosis

Endometriosis is a continuous and progressive disease with a poorly understood aetiology, pathophysiology and natural history. This study evaluated the histological differences between eutopic and ectopic endometria (abdominal wall endometriosis) and the expression of mast cell proteases (tryptase and chymase), annexin A1 (ANXA1) and formyl peptide receptor 1 (FPR1). Ectopic endometrium from 18 women with abdominal wall endometriosis and eutopic endometrium from 10 women without endometriosis were obtained. The endometrial samples were analysed by histopathology, immunohistochemistry and ultrastructural immunogold labeling to determine mast cell heterogeneity (tryptase and chymase positive cells) and the expression levels of ANXA1 and FPR1. Histopathological analysis of the endometriotic lesions showed a glandular pattern of mixed differentiation and an undifferentiated morphology with a significant influx of inflammatory cells and a change in mast cell heterogeneity, as evidenced by a significant increase in the number of chymase-positive cells and endogenous chymase expression. The undifferentiated glandular pattern of endometriotic lesions was positively associated with a marked increase and co-localization of ANXA1 and FPR1 in the epithelial cells. In conclusion, the co-upregulated expression of mast cell chymase and ANXA1–FPR1 system in ectopic endometrium suggests their involvement in the development of endometriotic lesions.

The essential role of annexin A1 mimetic peptide in the skin allograft survival

Immunosuppressive drugs have a critical role in inhibiting tissue damage and allograft rejection.Studies have demonstrated the anti-infl ammatory effects of the annexin A1 (AnxA1) in the regulationof transmigration and apoptosis of leucocytes. In the present study, an experimental skin allograftmodel was used to evaluate a potential protective effect of AnxA1 in transplantation survival. Micewere used for the skin allograft model and pharmacological treatments were carried out using eitherthe AnxA1 mimetic peptide Ac2-26, with or without cyclosporine A (CsA), starting 3 days beforesurgery until rejection. Graft survival, skin histopathology, leucocyte transmigration and expressionof AnxA1 and AnxA5 post-transplantation were analysed. Pharmacological treatment with Ac2-26increased skin allograft survival related with inhibition of neutrophil transmigration and inductionof apoptos is, thereby reducing the tissue damage compared with control animals. Moreover, AnxA1and AnxA5 expression increased after Ac2-26 treatment in neutrophils. Interestingly, thecombination of Ac2-26 and cyclosporine A showed similar survival of transplants when compared withthe cyclosporine A group, which could be attributed to a synergistic effect of both drugs. Investigationsin vitro revealed that cyclosporine A inhibited extracellular-signal-regulated kinase (ERK) phosphory-lation induced by Ac2-26 in neutrophils. Overall, the results suggest that AnxA1 has an essential role inaugmenting the survival of skin allograft, mainly owing to inhibition of neutrophil transmigration andenhancement of apoptosis. This effect may lead to the development of new therapeutic approachesrelevant to transplant rejection.

Investigação da ação da proteína anexina A1 sobre o processo de angiogênese induzido pelo fator de crescimento do endotélio vascular: modelos experimentais in vivo e in vitro

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

Beneficial effect of annexin A1 in a model of experimental allergic conjunctivitis

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

Ac2-26 mimetic peptide of annexin A1 inhibits local and systemic inflammatory processes induced by bothrops moojeni venom and the lys-49 phospholipase A2 in a rat model

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

Otimização dos métodos de expressão e solubilização do alérgeno fosfolipase A1 do veneno de Polybia paulista

A vespa social Polybia paulista (Hymenoptera, Vespidae) é bastante abundante e endêmica nos Estados de São Paulo e sul de Minas Gerais. Os indivíduos da espécie causam um elevado número de acidentes de importância médica. Após a ferroada a vítima pode experimentar reações imunológicas locais e/ou sistêmicas, que em alguns casos podem conduzir a anafilaxia e morte. O diagnóstico e terapia de alergia à ferroada de P. paulista é baseado no uso de extrato de veneno bruto o que se associa à ocorrência de reatividade cruzada e reações imunológicas adversas durante a imunoterapia. O uso de alérgenos recombinantes (r) tem-se mostrado como uma alternativa interessante para reduzir o impacto destas desvantagens. Neste trabalho, foram avaliadas diferentes condições para otimizar a expressão recombinante e solubilização dos corpúsculos de inclusão da fosfolipase A1 (Poly p 1) (70kDa) do veneno de P. paulista previamente obtida mediante expressão heteróloga no sistema procariótico, Escherichia coli. Os resultados aqui obtidos contribuirão para aumentar as quantidades do r Poly p 1 necessárias para sua avaliação bioquímica e imunológica, e finalmente para melhorar os resultados do diagnóstico e imunoterapia específica de alergia ao veneno de P. paulista

Otimização dos métodos de expressão e solubilização do alérgeno fosfolipase A1 do veneno de Polybia paulista

A vespa social Polybia paulista (Hymenoptera, Vespidae) é bastante abundante e endêmica nos Estados de São Paulo e sul de Minas Gerais. Os indivíduos da espécie causam um elevado número de acidentes de importância médica. Após a ferroada a vítima pode experimentar reações imunológicas locais e/ou sistêmicas, que em alguns casos podem conduzir a anafilaxia e morte. O diagnóstico e terapia de alergia à ferroada de P. paulista é baseado no uso de extrato de veneno bruto o que se associa à ocorrência de reatividade cruzada e reações imunológicas adversas durante a imunoterapia. O uso de alérgenos recombinantes (r) tem-se mostrado como uma alternativa interessante para reduzir o impacto destas desvantagens. Neste trabalho, foram avaliadas diferentes condições para otimizar a expressão recombinante e solubilização dos corpúsculos de inclusão da fosfolipase A1 (Poly p 1) (70kDa) do veneno de P. paulista previamente obtida mediante expressão heteróloga no sistema procariótico, Escherichia coli. Os resultados aqui obtidos contribuirão para aumentar as quantidades do r Poly p 1 necessárias para sua avaliação bioquímica e imunológica, e finalmente para melhorar os resultados do diagnóstico e imunoterapia específica de alergia ao veneno de P. paulista

Annexin A1 regulates neutrophil clearance by macrophages in the mouse bone marrow

Under homeostatic conditions, a proportion of senescent CXCR4(hi) neutrophils home from the circulation back to the bone marrow, where they are phagocytosed by bone marrow macrophages. In this study, we have identified an unexpected role for the anti-inflammatory molecule annexin A1 (AnxA1) as a critical regulator of this process. We first observed that AnxA1(-/-) mice have significantly increased neutrophil numbers in their bone marrow while having normal levels of GM and G colony-forming units, monocytes, and macrophages. Although AnxA1(-/-) mice have more neutrophils in the bone marrow, a greater proportion of these cells are senescent, as determined by their higher levels of CXCR4 expression and annexin V binding. Consequently, bone marrow neutrophils from AnxA1(-/-) mice exhibit a reduced migratory capacity in vitro. Studies conducted in vitro also show that expression of AnxA1 is required for bone marrow macrophages, but not peritoneal macrophages, to phagocytose apoptotic neutrophils. Moreover, in vivo experiments indicate a defect in clearance of wild-type neutrophils in the bone marrow of AnxA1(-/-) mice. Thus, we conclude that expression of AnxA1 by resident macrophages is a critical determinant for neutrophil clearance in the bone marrow.-Dalli, J., Jones, C. P., Cavalcanti, D. M., Farsky, S. H., Perretti, M., Rankin, S. M. Annexin A1 regulates neutrophil clearance by macrophages in the mouse bone marrow. FASEB J. 26, 387-396 (2012). www.fasebj.org

Carboxypeptidases A1 and A2 from the perfusate of rat mesenteric arterial bed differentially process angiotensin peptides

Here we report the isolation of carboxypeptidases A1 and A2 (CPA1 and CPA2) from the rat mesenteric arterial bed perfusate, which were found to be identical with their pancreatic counterparts. Angiotensin (Ang) I, Ang II, Ang-(1-9) and Ang-(1-12) were differentially processed by these enzymes, worthy mentioning the peculiar CPA1-catalyzed conversion of Ang II to Ang-(1-7) and the CPA2-mediated formation of Ang I from Ang-(1-12). We detected gene transcripts for CPA1 and CPA2 in mesentery and other extrapancreatic tissues, indicating that these CPAs might play a role in the renin-angiotensin system in addition to their functions as digestive enzymes. (C) 2011 Elsevier Inc. All rights reserved.