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Anti-tumour effects of antimicrobial peptides, components of the innate immune system, against haematopoietic tumours in Drosophila mxc mutants

机译:先天性免疫系统组成部分的抗菌肽对果蝇mxc突变体中造血肿瘤的抗肿瘤作用

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The innate immune response is the first line of defence against microbial infections. In Drosophila , two major pathways of the innate immune system (the Toll- and Imd-mediated pathways) induce the synthesis of antimicrobial peptides (AMPs) within the fat body. Recently, it has been reported that certain cationic AMPs exhibit selective cytotoxicity against human cancer cells; however, little is known about their anti-tumour effects. Drosophila mxcsupmbn1/sup mutants exhibit malignant hyperplasia in a larval haematopoietic organ called the lymph gland (LG). Here, using RNA-seq analysis, we found many immunoresponsive genes, including those encoding AMPs, to be upregulated in these mutants. Downregulation of these pathways by either a Toll or imd mutation enhanced the tumour phenotype of the mxc mutants. Conversely, ectopic expression of each of five different AMPs in the fat body significantly suppressed the LG hyperplasia phenotype in the mutants. Thus, we propose that the Drosophila innate immune system can suppress the progression of haematopoietic tumours by inducing AMP gene expression. Overexpression of any one of the five AMPs studied resulted in enhanced apoptosis in mutant LGs, whereas no apoptotic signals were detected in controls. We observed that two AMPs, Drosomycin and Defensin, were taken up by circulating haemocyte-like cells, which were associated with the LG regions and showed reduced cell-to-cell adhesion in the mutants. By contrast, the AMP Diptericin was directly localised at the tumour site without intermediating haemocytes. These results suggest that AMPs have a specific cytotoxic effect that enhances apoptosis exclusively in the tumour cells.
机译:天生的免疫反应是抵抗微生物感染的第一道防线。在果蝇中,先天免疫系统的两个主要途径(Toll和Imd介导的途径)诱导了脂肪体内抗菌肽(AMPs)的合成。最近,已经报道某些阳离子AMP对人癌细胞表现出选择性的细胞毒性。然而,对其抗肿瘤作用知之甚少。果蝇mxc mbn1 突变体在称为淋巴腺(LG)的幼虫造血器官中表现出恶性增生。在这里,使用RNA序列分析,我们发现许多免疫应答基因,包括那些编码AMP的基因,在这些突变体中均被上调。通过Toll或imd突变对这些途径的下调增强了mxc突变体的肿瘤表型。相反,脂肪体内五个不同AMP的异位表达显着抑制了突变体的LG增生表型。因此,我们建议果蝇先天免疫系统可以通过诱导AMP基因表达来抑制造血肿瘤的进展。研究的五种AMP中任何一种的过表达都导致突变LG中细胞凋亡增强,而对照中未检测到凋亡信号。我们观察到,循环血红细胞样细胞吸收了两个AMPs(果霉素和防御素),这些细胞与LG区域相关,并在突变体中显示出降低的细胞间粘附性。相比之下,AMP Diptericin直接定位在肿瘤部位,而没有中间的血细胞。这些结果表明,AMP具有特异的细胞毒性作用,其仅在肿瘤细胞中增强细胞凋亡。

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