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使用基于转录组的掩码在嵌合模型中进行细胞类型特异性转录组学研究。

Cell-type-specific transcriptomics in chimeric models using transcriptome-based masks.

作者信息

Naef Felix, Huelsken Joerg

机构信息

Swiss Institute for Experimental Cancer Research (ISREC), NCCR Molecular Oncology Chemin des Boveresses 155, 1066 Epalinges, Switzerland.

出版信息

Nucleic Acids Res. 2005 Jul 19;33(13):e111. doi: 10.1093/nar/gni104.

Abstract

Regulatory networks involving different cell types control inflammation, morphogenesis and tissue homeostasis. Cell-type-specific transcriptional profiling offers a powerful tool for analyzing such cross-talk but is often hampered by mingling of cells within a tissue. Here, we present a novel method that performs cell-type-specific expression measurements without prior cell separation. This involves inter-species transplantation or chimeric co-culture models among which the human mouse system is frequently used. Here, we exploit the sufficiently divergent transcriptomes of human and mouse in conjunction with high-density oligonucleotide arrays. This required a masking procedure based on transcriptome databases and exhaustive fuzzy mapping of oligonucleotide probes onto these data. The approach was tested in a human-mouse experiment, demonstrating that we can efficiently measure species-specific transcriptional profiles in chimeric RNA samples without physically separating cells. Our results stress the importance of transcriptome databases with accurate 3' mRNA termination for computational prediction of accurate probe masks. We find that most human and mouse 3'-untranslated region contain unique stretches to allow for an effective control of cross-hybridization between the two species. This approach can be applied to xenograft models studying tumor-host interactions, morphogenesis or immune responses.

摘要

涉及不同细胞类型的调控网络控制着炎症、形态发生和组织稳态。细胞类型特异性转录谱分析为分析这种相互作用提供了一个强大的工具,但常常因组织内细胞的混合而受到阻碍。在这里,我们提出了一种无需事先分离细胞就能进行细胞类型特异性表达测量的新方法。这涉及种间移植或嵌合共培养模型,其中人类-小鼠系统经常被使用。在这里,我们利用人类和小鼠足够不同源的转录组,结合高密度寡核苷酸阵列。这需要一个基于转录组数据库的屏蔽程序,以及将寡核苷酸探针详尽地模糊映射到这些数据上。该方法在一项人类-小鼠实验中进行了测试,证明我们可以在不进行细胞物理分离的情况下,有效地测量嵌合RNA样本中的物种特异性转录谱。我们的结果强调了具有准确3' mRNA末端的转录组数据库对于准确探针屏蔽的计算预测的重要性。我们发现,大多数人类和小鼠的3'非翻译区包含独特的片段,以有效控制两个物种之间的交叉杂交。这种方法可应用于研究肿瘤-宿主相互作用、形态发生或免疫反应的异种移植模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/920b/1178007/dc12a763071f/gni104f1.jpg

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