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首页> 外文期刊>International Journal for Parasitology: Drugs and Drug Resistance >The anti-fecundity effect of 5-azacytidine (5-AzaC) on Schistosoma mansoni is linked to dis-regulated transcription, translation and stem cell activities
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The anti-fecundity effect of 5-azacytidine (5-AzaC) on Schistosoma mansoni is linked to dis-regulated transcription, translation and stem cell activities

机译:5-氮杂胞苷(5-AzaC)对曼氏血吸虫的抗生殖力作用与转录,翻译和干细胞活性失调有关

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Uncontrolled host immunological reactions directed against tissue-trapped eggs precipitate a potentially lethal, pathological cascade responsible for schistosomiasis. Blocking schistosome egg production, therefore, presents a strategy for simultaneously reducing immunopathology as well as limiting disease transmission in endemic or emerging areas. We recently demonstrated that the ribonucleoside analogue 5-azacytidine (5-AzaC) inhibited Schistosoma mansoni oviposition, egg maturation and ovarian development. While these anti-fecundity effects were associated with a loss of DNA methylation, other molecular processes affected by 5-AzaC were not examined at the time. By comparing the transcriptomes of 5-AzaC-treated females to controls, we provide evidence that this ribonucleoside analogue also modulates other crucial aspects of schistosome egg-laying biology. For example, S. mansoni gene products associated with amino acid-, carbohydrate-, fatty acid-, nucleotide- and tricarboxylic acid (TCA)- homeostasis are all dysregulated in 5-AzaC treated females. To validate the metabolic pathway most significantly affected by 5-AzaC, amino acid metabolism, nascent protein synthesis was subsequently quantified in adult schistosomes. Here, 5-AzaC inhibited this process by 68% ±16.7% (SEM) in male- and 81% ±4.8% (SEM) in female-schistosomes. Furthermore, the transcriptome data indicated that adult female stem cells were also affected by 5-AzaC. For instance, 40% of transcripts associated with proliferating schistosome cells were significantly down-regulated by 5-AzaC. This finding correlated with a considerable reduction (95%) in the number of 5-ethynyl-2′-deoxyuridine (EdU) positive cells found in 5-AzaC-treated females. In addition to protein coding genes, the effect that 5-AzaC had on repetitive element expression was also assessed. Here, 46 repeats were found differentially transcribed between 5-AzaC-treated and control females with long terminal repeat (LTR) and DNA transposon classes being amongst the most significant. This study demonstrates that the anti-fecundity activity of 5-AzaC affects more than just DNA methylation in schistosome parasites. Further characterisation of these processes may reveal novel targets for schistosomiasis control.
机译:针对组织捕获的卵的不受控制的宿主免疫反应会导致血吸虫病的潜在致死性病理性级联反应。因此,阻断血吸虫卵的产生提出了一种同时减少免疫病理以及限制疾病在流行地区或新兴地区传播的策略。我们最近证明,核糖核苷类似物5-氮杂胞苷(5-AzaC)抑制曼氏血吸虫产卵,卵成熟和卵巢发育。尽管这些抗生殖力作用与DNA甲基化的丧失有关,但当时未检查受5-AzaC影响的其他分子过程。通过比较5-AzaC处理的女性与对照组的转录组,我们提供了这种核糖核苷类似物还调节血吸虫卵生物生物学的其他关键方面的证据。例如,在5-AzaC处理的女性中,与氨基酸,碳水化合物,脂肪酸,核苷酸和三羧酸(TCA)稳态相关的曼氏链球菌基因产物均失调。为了验证受5-AzaC影响最大的代谢途径,即氨基酸代谢,随后在成人血吸虫中定量了新生蛋白质的合成。在这里,5-AzaC在男性血吸虫中抑制了68%±16.7%(SEM),在女性血吸虫中抑制了81%±4.8%(SEM)。此外,转录组数据表明成年雌性干细胞也受到5-AzaC的影响。例如,与增殖的血吸虫细胞相关的转录物被5-AzaC显着下调。这一发现与在5-AzaC处理的雌性中发现的5-乙炔基-2'-脱氧尿苷(EdU)阳性细胞数量显着减少(95%)有关。除了蛋白质编码基因,还评估了5-AzaC对重复元件表达的影响。在这里,发现在经5-AzaC处理的雌性和对照雌性之间差异转录了46个重复序列,其中长末端重复序列(LTR)和DNA转座子类别最为明显。这项研究表明,5-AzaC的抗生殖力活性不仅影响血吸虫寄生虫的DNA甲基化,而且影响更大。这些过程的进一步表征可能揭示血吸虫病控制的新目标。

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