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Spatial niche formation but not malignant progression is a driving force for intratumoural heterogeneity

机译:空间小生境形成而非恶性进展是肿瘤内异质性的驱动力

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Intratumoural heterogeneity (ITH) is a major cause of cancer-associated lethality. Extensive genomic ITH has previously been reported in clear cell renal cell carcinoma (ccRCC). Here we address the question whether ITH increases with malignant progression and can hence be exploited as a prognostic marker. Unexpectedly, precision quantitative image analysis reveals that the degree of functional ITH is virtually identical between primary ccRCCs of the lowest stage and advanced, metastatic tumours. Functional ITH was found to show a stage-independent topological pattern with peak proliferative and signalling activities almost exclusively in the tumour periphery. Exome sequencing of matching peripheral and central primary tumour specimens reveals various region-specific mutations. However, these mutations cannot directly explain the zonal pattern suggesting a role of microenvironmental factors in shaping functional ITH. In conclusion, our results indicate that ITH is an early and general characteristic of malignant growth rather than a consequence of malignant progression.
机译:肿瘤内异质性(ITH)是癌症相关致死性的主要原因。先前已经报道了在透明细胞肾细胞癌(ccRCC)中广泛的基因组ITH。在这里,我们要解决的问题是ITH是否随着恶性进展而增加,因此可以用作预后指标。出乎意料的是,精确的定量图像分析显示,最低阶段的原发性ccRCC与晚期转移性肿瘤之间的功能性ITH程度实际上是相同的。发现功能性ITH表现出阶段无关的拓扑模式,几乎仅在肿瘤外围具有峰值的增殖和信号传导活性。匹配的外周和中央原发肿瘤标本的外显子组测序揭示了各种区域特异性突变。但是,这些突变不能直接解释区带模式,暗示了微环境因子在塑造功能性ITH中的作用。总之,我们的结果表明ITH是恶性生长的早期和一般特征,而不是恶性进展的结果。

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