首页> 美国卫生研究院文献>Neuro-Oncology >PDTM-04. REDEFINING THE CELLULAR ARCHITECTURE OF DIFFUSE MIDLINE GLIOMAS WITH H3 K27M MUTATIONS THROUGH LARGE-SCALE SINGLE-CELL ANALYSES
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PDTM-04. REDEFINING THE CELLULAR ARCHITECTURE OF DIFFUSE MIDLINE GLIOMAS WITH H3 K27M MUTATIONS THROUGH LARGE-SCALE SINGLE-CELL ANALYSES

机译:PDTM-04。通过大型单细胞分析使用H3 K27M突变重新定义弥散中线胶质瘤的细胞结构

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摘要

While human tumors are shaped by the genetic evolution of cancer cells, evidence also suggests that they display superimposed hierarchies reminiscent of normal development. Yet, relating the genetic and hierarchical models of cancer organization has been limited by technical challenges. Here, studying H3 K27M-mutant diffuse midline gliomas we profiled thousands of single cells from fresh tumors by RNA-seq and reconstructed the genetic and epigenetic cellular architecture of tumors in patients. We identified a subset of cancer cells that are differentiated along specialized glial programs while a distinct subset expresses oligodendrocyte precursor expression programs. By identifying distinct genetic clones, we show that these cellular architectures evolve during the progression of the tumors, suggesting that developmental programs and genetic influences coordinately determine tumor architecture. These results provide unprecedented insight into the cellular composition of midline brain tumors at single-cell resolution and may help harmonize the cancer stem cell and the genetic models of cancer, with critical implications for disease management.
机译:虽然人类肿瘤是由癌细胞的遗传进化所塑造的,但证据还表明,它们表现出叠加的层次结构,让人联想到正常的发展。然而,将癌症组织的遗传模型和层次模型联系起来一直受到技术挑战的限制。在这里,我们研究了H3 K27M突变弥漫性中线神经胶质瘤,通过RNA-seq对来自新鲜肿瘤的数千个单细胞进行了分析,并重建了患者肿瘤的遗传和表观遗传细胞结构。我们确定了沿着专门的神经胶质程序分化的癌细胞子集,而一个不同的子集表达少突胶质细胞前体表达程序。通过鉴定不同的基因克隆,我们表明这些细胞结构在肿瘤的发展过程中发展,这表明发展计划和遗传影响协调确定肿瘤的结构。这些结果以单细胞分辨率提供了对中线脑肿瘤细胞组成的前所未有的洞察力,可能有助于协调癌症干细胞和癌症的遗传模型,对疾病管理具有至关重要的意义。

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