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首页> 外文期刊>Annals of the New York Academy of Sciences >Circulating Nucleic Acids in Plasma/Serum and Tumor Progression: Are Apoptotic Bodies Involved? An Experimental Study in a Rat Cancer Model
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Circulating Nucleic Acids in Plasma/Serum and Tumor Progression: Are Apoptotic Bodies Involved? An Experimental Study in a Rat Cancer Model

机译:血浆/血清和肿瘤进展中的循环核酸:是否涉及凋亡小体?大鼠癌症模型的实验研究

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摘要

The "genometastasis hypothesis" proposes that cell-free tumor nucleic acids might be able to transform host stem cells, and that this might be a pathway for the development of metastases. This theory is supported by previous experimental findings and is consistent with observations of other authors. It has been suggested that tumor DNA might be horizontally transferred by the uptake of apoptotic bodies and initiate the genetic changes that are necessary for tumor formation. In addition, apoptotic bodies have been proposed as possible vehicles that protect the nucleic acids circulating in the plasma from enzymatic degradation. In the present study, we analyzed the presence of apoptotic bodies in serum and its relationship with tumor progression in a heterotopic model of colon cancer in the rat. We injected DHD/K12-PROb cancer cells subcutaneously into BD-IX rats and divided the animals into three groups according to the time between the injection of tumor cells and euthanasia. A control group of healthy animals was included (n = 6). After euthanasia, macroscopic metastases were assessed and samples of blood were collected. To detect apoptotic bodies in the sera, each sample was mixed with FITC-conjugated annexin V antibody in combination with propidium iodide and then analyzed by flow cytometry. Detection of apoptotic bodies was only significantly increased in the sera of a few tumor-bearing animals in late stages of tumor development. Thus, such particles appear not to be the vehicle of the cell-free tumor nucleic acids that are detected at early stages of cancer.
机译:“基因转移假设”提出,无细胞的肿瘤核酸可能能够转化宿主干细胞,这可能是转移发生的途径。该理论得到先前实验结果的支持,并且与其他作者的观察结果一致。已经提出,肿瘤DNA可能由于凋亡小体的摄取而水平转移,并引发肿瘤形成所必需的遗传改变。另外,已经提出凋亡小体作为保护血浆中循环的核酸免于酶促降解的可能的载体。在本研究中,我们分析了大鼠结肠癌异位模型中血清中凋亡小体的存在及其与肿瘤进展的关系。我们将DHD / K12-PROb癌细胞皮下注射到BD-IX大鼠中,并根据注射肿瘤细胞与安乐死的时间将动物分为三组。包括健康动物对照组(n = 6)。安乐死后,评估宏观转移并收集血液样本。为了检测血清中的凋亡小体,将每个样品与结合了碘化丙锭的FITC-缀合的膜联蛋白V抗体混合,然后通过流式细胞术进行分析。在肿瘤发展的后期阶段,在一些荷瘤动物的血清中仅明显增加了凋亡小体的检测。因此,这种颗粒似乎不是癌症早期阶段检测到的无细胞肿瘤核酸的载体。

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