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通过单细胞RNA测序绘制患者来源的黑色素瘤培养物中的异质性

Mapping heterogeneity in patient-derived melanoma cultures by single-cell RNA-seq.

作者信息

Gerber Tobias, Willscher Edith, Loeffler-Wirth Henry, Hopp Lydia, Schadendorf Dirk, Schartl Manfred, Anderegg Ulf, Camp Gray, Treutlein Barbara, Binder Hans, Kunz Manfred

机构信息

Department of Evolutionary Genetics, Max Planck Institute for Evolutionary Anthropology Leipzig, 04103 Leipzig, Germany.

Interdisciplinary Center for Bioinformatics, University of Leipzig, 04107 Leipzig, Germany.

出版信息

Oncotarget. 2017 Jan 3;8(1):846-862. doi: 10.18632/oncotarget.13666.

Abstract

Recent technological advances in single-cell genomics make it possible to analyze cellular heterogeneity of tumor samples. Here, we applied single-cell RNA-seq to measure the transcriptomes of 307 single cells cultured from three biopsies of three different patients with a BRAF/NRAS wild type, BRAF mutant/NRAS wild type and BRAF wild type/NRAS mutant melanoma metastasis, respectively. Analysis based on self-organizing maps identified sub-populations defined by multiple gene expression modules involved in proliferation, oxidative phosphorylation, pigmentation and cellular stroma. Gene expression modules had prognostic relevance when compared with gene expression data from published melanoma samples and patient survival data. We surveyed kinome expression patterns across sub-populations of the BRAF/NRAS wild type sample and found that CDK4 and CDK2 were consistently highly expressed in the majority of cells, suggesting that these kinases might be involved in melanoma progression. Treatment of cells with the CDK4 inhibitor palbociclib restricted cell proliferation to a similar, and in some cases greater, extent than MAPK inhibitors. Finally, we identified a low abundant sub-population in this sample that highly expressed a module containing ABC transporter ABCB5, surface markers CD271 and CD133, and multiple aldehyde dehydrogenases (ALDHs). Patient-derived cultures of the BRAF mutant/NRAS wild type and BRAF wild type/NRAS mutant metastases showed more homogeneous single-cell gene expression patterns with gene expression modules for proliferation and ABC transporters. Taken together, our results describe an intertumor and intratumor heterogeneity in melanoma short-term cultures which might be relevant for patient survival, and suggest promising targets for new treatment approaches in melanoma therapy.

摘要

单细胞基因组学领域最近的技术进展使得分析肿瘤样本的细胞异质性成为可能。在此,我们应用单细胞RNA测序来测量分别从三名患有BRAF/NRAS野生型、BRAF突变型/NRAS野生型和BRAF野生型/NRAS突变型黑色素瘤转移的不同患者的三次活检中培养出的307个单细胞的转录组。基于自组织映射的分析确定了由多个参与增殖、氧化磷酸化、色素沉着和细胞基质的基因表达模块所定义的亚群。与已发表的黑色素瘤样本的基因表达数据和患者生存数据相比,基因表达模块具有预后相关性。我们研究了BRAF/NRAS野生型样本亚群中的激酶组表达模式,发现CDK4和CDK2在大多数细胞中持续高表达,这表明这些激酶可能参与黑色素瘤的进展。用CDK4抑制剂帕博西尼处理细胞对细胞增殖的限制程度与MAPK抑制剂相似,在某些情况下甚至更大。最后,我们在该样本中鉴定出一个低丰度亚群,该亚群高表达一个包含ABC转运蛋白ABCB5、表面标志物CD271和CD133以及多种醛脱氢酶(ALDH)的模块。BRAF突变型/NRAS野生型和BRAF野生型/NRAS突变型转移灶的患者来源培养物显示出更均匀的单细胞基因表达模式,具有增殖和ABC转运蛋白的基因表达模块。综上所述,我们的结果描述了黑色素瘤短期培养中的肿瘤间和肿瘤内异质性,这可能与患者生存相关,并为黑色素瘤治疗的新治疗方法提出了有前景的靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/61d6/5352202/7c5edf6d20c0/oncotarget-08-846-g001.jpg

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