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P-mapa, a promisor immunomodulator against tumor cells of colonic tissues: An investigation of the action mechanism over the TLR4 signaling pathway

机译:P-MAPA,一种针对结肠组织肿瘤细胞的主要调节剂:对TLR4信号通路的作用机制的研究

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摘要

Colorectal cancer (CRC) is a multifactorial syndrome that drives to uncontrollable cell division, genetic alterations, and functional alteration. In the present work, we evaluated the immunomodulatory properties of P-mapa, a compound extracted from Aspergillus oryzae fungus, versus Fluorouracil (5-FU) treatment in chemically induced CRC. CRC was induced by DMH in F344 rats. Animals of treated groups receive weekly 15 mg/Kg of 5-FU or 5 mg/Kg of P-mapa, over 10 weeks. Tissues were stained for aberrant crypt foci (ACF) counting and histopathology evaluation, immunostained for TLR4 pathways and quantified for TNF alpha Cytokine assay. DMH was efficient to induce hyperplastic lesions and ACF. Both treatments reduced significantly ACF formation and tumor aggressiveness. Immunohistochemistry for TLR4 signaling reveals that both treatments had no effect over the TLR4-NF kappa B signaling pathway. On the other hand, both succeed in increase interferon signaling, with activation of the TRIF-IRF3 pathway and consequently inducing IFN gamma synthesis. The present results show the immunomodulatory properties of P-mapa in chemically induced CRC model. P-mapa induced a significant increase in Type-I IFNs synthesis and subsequently immune cell recruitment, resulting in an increase of IFN gamma concentration in colorectal mucosa and its inhibitory effects over tumoral growth. In this scenario, P-mapa showed an interesting antitumoral effect by inhibiting tumor growth.
机译:结肠直肠癌(CRC)是一种多因素综合征,驱动无法控制的细胞分裂,遗传改变和功能改变。在本作工作中,我们评估了P-MAPA的免疫调节特性,从曲霉属植物毒素玉米曲霉(Asyzae Grygus)中提取的化合物,在化学诱导的CRC中处理氟尿嘧啶(5-FU)。 CRC在F344大鼠中被DMH诱导。治疗组的动物每周接受15mg / kg 5-fu或5mg / kg p-mapa,超过10周。组织被染成异常隐窝焦点(ACF)计数和组织病理学评估,用于TLR4途径的免疫染色,并为TNFα细胞因子测定量化。 DMH有效地诱导增生病变和ACF。两种治疗可显着降低ACF形成和肿瘤侵袭性。用于TLR4信号传导的免疫组织化学显示,两种治疗对TLR4-NF Kappa B信号通路没有影响。另一方面,两者都成功地增加了干扰素信号传导,激活了TRIF-IRF3途径,因此诱导IFNγ合成。本结果显示了化学诱导的CRC模型中p-MAPA的免疫调节特性。 P-MAPA诱导I ICIE-I IFNS合成和随后的免疫细胞募集的显着增加,导致结直肠粘膜中的IFNγ浓度增加及其对肿瘤生长的抑制作用。在这种情况下,P-MAPA通过抑制肿瘤生长显示有趣的抗肿瘤效果。

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