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血液中可重复性肝癌特异性配体-受体信号传导的检测

Detection of reproducible liver cancer specific ligand-receptor signaling in blood.

作者信息

Safrastyan Aram, Wollny Damian

机构信息

RNA Bioinformatics and High Throughput Analysis, Friedrich Schiller University Jena, Jena, Germany.

Genetics and Epigenetics of Aging, Leibniz Institute on Aging-Fritz Lipmann Institute (FLI), Jena, Germany.

出版信息

Front Bioinform. 2025 Jan 9;4:1332782. doi: 10.3389/fbinf.2024.1332782. eCollection 2024.

Abstract

Cell-cell communication mediated by ligand-receptor interactions (LRI) is critical to coordinating diverse biological processes in homeostasis and disease. Lately, our understanding of these processes has greatly expanded through the inference of cellular communication, utilizing RNA extracted from bulk tissue or individual cells. Considering the challenge of obtaining tissue biopsies for these approaches, we considered the potential of studying cell-free RNA obtained from blood. To test the feasibility of this approach, we used the BulkSignalR algorithm across 295 cell-free RNA samples and compared the LRI profiles across multiple cancer types and healthy donors. Interestingly, we detected specific and reproducible LRIs particularly in the blood of liver cancer patients compared to healthy donors. We found an increase in the magnitude of hepatocyte interactions, notably hepatocyte autocrine interactions in liver cancer patients. Additionally, a robust panel of 30 liver cancer-specific LRIs presents a bridge linking liver cancer pathogenesis to discernible blood markers. In summary, our approach shows the plausibility of detecting liver LRIs in blood and builds upon the biological understanding of cell-free transcriptomes.

摘要

由配体-受体相互作用(LRI)介导的细胞间通讯对于协调体内稳态和疾病中的各种生物过程至关重要。最近,通过利用从大块组织或单个细胞中提取的RNA推断细胞通讯,我们对这些过程的理解有了极大的扩展。考虑到通过这些方法获取组织活检样本的挑战,我们考虑了研究从血液中获得的无细胞RNA的潜力。为了测试这种方法的可行性,我们对295个无细胞RNA样本使用了BulkSignalR算法,并比较了多种癌症类型和健康供体的LRI谱。有趣的是,与健康供体相比,我们在肝癌患者的血液中特别检测到了特异性且可重复的LRI。我们发现肝癌患者中肝细胞相互作用的强度增加,尤其是肝细胞自分泌相互作用。此外,一组由30个肝癌特异性LRI组成的强大组合构成了一座将肝癌发病机制与可识别的血液标志物联系起来的桥梁。总之,我们的方法显示了在血液中检测肝脏LRI的合理性,并建立在对无细胞转录组的生物学理解之上。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/57a5/11754192/d6d8a0b16e34/fbinf-04-1332782-g001.jpg

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