RESUMO
ABSTRACT Inulin is an effective prebiotic and its potential in modulating systemic immunity have been proposed. A subpopulation of T cells, named T regulatory cells (Tregs), expressing the Forkhead boxP3 transcription factor are key mediators of peripheral tolerance and suppress undesirable immune responses. These Tregs can be induced by cytokine transforming growth factor beta (TGF-β) and interleukin 10 (IL-10). This work aimed to evaluate inulin effects on human peripheral blood mononuclear cells (PBMC) in vitro. PBMC were incubated with inulin, and the expression of TGF-(1, FOXP3 and IL-10 was analyzed. Increased supernatant IL-10 levels were observed in PBMC of inulin-treated group (p=0.03). Moreover, FOXP3 gene expression was 7.6 fold higher in inulin-treated PBMC, whereas a trend in TGF-β1 expression was detected (p=0.055). These data suggest that inulin induces an immunosuppressive environment in cultured PBMC by promoting FOXP3 gene expression and IL-10 secretion. These studies offer prospects for further fundamental research in this field.
RESUMO
O meduloblastoma é um tumor cerebelar caracterizado como tumor neuroectodérmico primitivo prevalente em crianças, sendo as do sexo masculinos as mais afetadas. Com relação à classificação histológica,existem cinco variações: clássico, desmoplásico, anaplásico, células gigantes e de extensa nodularidade. Muitos estudos relatam que a patogênese do meduloblastoma está relacionada com mutações em fatores de crescimento do SNC, sendo que as principais vias envolvidas são: Sonic Hedgehog, NOTCH, WNT eOTX. Ainda, com respeito à imunologia, pacientes com meduloblastoma apresentaram alta taxa de IFN-γno soro e células TH17 no sangue periférico, e foi observado que o TGF-β tem sido associado à estimulação mitogênica, o que pode estar relacionado à patogênese da doença. A predominância de uma resposta TH1 relacionada à sobrevivência também foi relatada. O desenvolvimento terapêutico para o meduloblastoma,apesar de limitado, é significativo, uma vez que este vem apresentando melhora na sobrevida de seus pacientes. Entretanto, um maior conhecimento dos mecanismos envolvidos na imunopatogênese é necessário para o desenvolvimento de novos fármacos e formas de tratamento.
Medulloblastoma is a cerebellar tumor classified as primitive neuroectodermal tumor and is prevalent in children, especially male. With regard to histological classification, there are five variations: classical, desmoplastic, anaplastic, large-cell variant and with extensive nodularity. Several studies have reported that medulloblastoma pathogenesis is related to mutations in CNS growth factors, and the main pathways involved are Sonic Hedgehog, NOTCH, WNT, and OTX. Also regarding the immunology, patients with medulloblastoma have a high serum concentration of INF-γ and TH17 cells in peripheral blood, and it was observed that TGF-β has been associated with mitogenic stimulation, and possibly associated to the pathogenesis of this disease. The prevalence of a TH1 response related to the survival was also described. The development of therapies for medulloblastoma treatment, though limited, is significant, as they resultin an improvement in the patients survival. However, a better understanding of the mechanism involvedin its immunopathogenesis is still necessary for the development of new drugs and ways of treatment.
Assuntos
Criança , Meduloblastoma , Neoplasias Cerebelares , Transdução de SinaisRESUMO
A subgroup of tumor that has received attention is triple-negative breast cancer (TNBC), which presents phenotype of negative estrogen receptor, negative progesterone receptor and has no overexpression of HER2. TP53 acts as a tumor suppressor limiting the proliferation of damaged cells. A polymorphic site (rs1042522) of TP53 encodes either an arginine or a proline amino acid, but its biological significance remains unclear. This study aimed to investigate this variant and its expression in search for a possible involvement in TNBC susceptibility and clinical outcome. Genetic polymorphism was evaluated in 50 patients and 115 controls by PCR based methodology and immunohistochemistry was done with monoclonal antibody. Case-control study showed no positive or negative association (OR= 0.95; CI95%= 0.48-1.89). Comparison of genotypes and clinical outcome showed no significant results. Despite most of patients presented p53 positive staining by immunohistochemistry, there was no significant association in relation to prognostic parameters. Results demonstrated a lack of association between codon 72 polymorphism, susceptibility and prognosis of TNBC. Immunohistochemistry analysis should be done more carefully, since most of the patients had the somatic mutation of p53, which could be an indicator of prognostic value in TNBC.