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Normal and Cancerous Tissues Release extrachromosomal circular DNA (eccDNA) into the Circulation

机译:正常和癌变组织将染色体外环状DNA(eccDNA)释放到循环系统中

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摘要

Cell-free circulating linear DNA is being explored for non-invasive diagnosis and management of tumors and fetuses, the so-called liquid biopsy. Previously, we observed the presence of small extrachromosomal circular DNA (eccDNA), called microDNA, in the nuclei of mammalian tissues and cell lines. Now, we demonstrate that cell-free microDNA derived from uniquely mapping regions of the genome is detectable in plasma and serum from both mice and humans and that they are significantly longer (30–60% >250 bases) than cell-free circulating linear DNA (~150 bases). Tumor-derived human microDNA is detected in the mouse circulation in a mouse xenograft model of human ovarian cancer. Comparing the microDNA from paired tumor and normal lung tissue specimens reveals that the tumors contain longer microDNA. Consistent with human cancers releasing microDNA into the circulation, serum and plasma samples (12 lung and 11 ovarian cancer) collected prior to surgery are enriched for longer cell free microDNA compared to samples from the same patient obtained several weeks after surgical resection of the tumor. Thus, circular DNA in the circulation is a previously unexplored pool of nucleic acids that could complement microRNAs (miRs) and linear DNA for diagnosis and for intercellular communication.
机译:人们正在探索无细胞循环线性DNA,用于无创诊断和处理肿瘤和胎儿,即所谓的液体活检。以前,我们观察到哺乳动物组织和细胞系的核中存在小的染色体外环状DNA(eccDNA),称为microDNA。现在,我们证明了从小鼠和人类的血浆和血清中都可以检测到来自基因组独特定位区域的无细胞microDNA,并且它们比无细胞循环线性DNA更长(30–60%> 250个碱基) (〜150个碱基)。在人类卵巢癌的小鼠异种移植模型中的小鼠循环中检测到肿瘤来源的人microDNA。比较配对肿瘤和正常肺组织标本中的microDNA,发现肿瘤包含更长的microDNA。与将MicroDNA释放到循环系统中的人类癌症相一致,与从肿瘤切除后几周获得的同一名患者的样品相比,手术前收集的血清和血浆样品(12例肺癌和11例卵巢癌)中富含更长的无细胞microDNA。因此,循环中的环状DNA是先前未开发的核酸库,可以补充microRNA(miR)和线性DNA用于诊断和细胞间通讯。

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