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染色体重排型 SHH 型髓母细胞瘤的时空转录组学研究鉴定出多个对治疗有抵抗性并导致复发的遗传克隆。

Spatio-temporal transcriptomics of chromothriptic SHH-medulloblastoma identifies multiple genetic clones that resist treatment and drive relapse.

机构信息

Division of Computational Genomics and Systems Genetics, German Cancer Research Centre (DKFZ), Heidelberg, Germany.

Group Genome Instability in Tumors, German Cancer Research Centre (DKFZ), Heidelberg, Germany.

出版信息

Nat Commun. 2024 Nov 29;15(1):10370. doi: 10.1038/s41467-024-54709-w.

Abstract

Paediatric medulloblastomas with chromothripsis are characterised by high genomic instability and are among the tumours with the worst prognosis. However, the molecular makeup and the determinants of the aggressiveness of chromothriptic medulloblastoma are not well understood. Here, we apply spatial transcriptomics to profile a cohort of 13 chromothriptic and non-chromothriptic medulloblastomas from the same molecular subgroup. Our data reveal a higher extent of spatial intra-tumour heterogeneity in chromothriptic medulloblastomas compared to non-chromothripictic tumours, which is associated with increased proliferation and stemness, but lower immune infiltration and differentiation. Spatial mapping of genetic subclones of the same tumour identify a regionally distinct architecture and clone-specific phenotypic features, with distinct degrees of differentiation, proliferation and immune infiltration between clones. We conduct temporal profiling of 11 samples from patient-derived xenografts from a patient with chromothriptic medulloblastoma, covering the transition from the minimal residual disease stage to treatment-resistant regrown tumours. In chromothriptic medulloblastoma, an ecosystem of cells from multiple genetic clones resist treatment and lead to relapse. Finally, we identify tumour microtubes in chromothriptic medulloblastoma, calling for exploration of cell network communication as a putative target.

摘要

具有染色体重排的小儿髓母细胞瘤的特点是基因组高度不稳定,属于预后最差的肿瘤之一。然而,染色体重排髓母细胞瘤的分子构成和侵袭性决定因素尚不清楚。在这里,我们应用空间转录组学对来自同一分子亚群的 13 例染色体重排和非染色体重排髓母细胞瘤进行了分析。我们的数据显示,与非染色体重排肿瘤相比,染色体重排髓母细胞瘤的肿瘤内空间异质性程度更高,这与增殖和干性增加有关,但免疫浸润和分化减少有关。同一肿瘤遗传亚克隆的空间图谱确定了具有区域独特结构和克隆特异性表型特征的区域,克隆之间的分化、增殖和免疫浸润程度存在明显差异。我们对一名染色体重排髓母细胞瘤患者来源的异种移植模型的 11 个样本进行了时间分析,涵盖了从微小残留疾病阶段到治疗耐药性复发性肿瘤的转变。在染色体重排髓母细胞瘤中,来自多个遗传克隆的细胞生态系统抵抗治疗并导致复发。最后,我们在染色体重排髓母细胞瘤中发现了肿瘤微管,这呼吁探索细胞网络通信作为一个潜在的靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/36ef/11604656/4a08089b5126/41467_2024_54709_Fig1_HTML.jpg

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