Gene expression in soft-shell clam (Mya arenaria) transmissible cancer reveals survival mechanisms during host infection and seawater transfer.

IF 4 2区 生物学 Q1 GENETICS & HEREDITY
Samuel F M Hart, Fiona E S Garrett, Jesse S Kerr, Michael J Metzger
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引用次数: 0

Abstract

Transmissible cancers are unique instances in which cancer cells escape their original host and spread through a population as a clonal lineage, documented in Tasmanian Devils, dogs, and ten bivalve species. For a cancer to repeatedly transmit to new hosts, these lineages must evade strong barriers to transmission, notably the metastasis-like physical transfer to a new host body and rejection by that host's immune system. We quantified gene expression in a transmissible cancer lineage that has spread through the soft-shell clam (Mya arenaria) population to investigate potential drivers of its success as a transmissible cancer lineage, observing extensive differential expression of genes and gene pathways. We observed upregulation of genes involved with genotoxic stress response, ribosome biogenesis and RNA processing, and downregulation of genes involved in tumor suppression, cell adhesion, and immune response. We also observe evidence that widespread genome instability affects the cancer transcriptome via gene fusions, copy number variation, and transposable element insertions. Finally, we incubated cancer cells in seawater, the presumed host-to-host transmission vector, and observed conserved responses to halt metabolism, avoid apoptosis and survive the low-nutrient environment. Interestingly, many of these responses are also present in healthy clam cells, suggesting that bivalve hemocytes may have inherent seawater survival responses that may partially explain why transmissible cancers are so common in bivalves. Overall, this study reveals multiple mechanisms this lineage may have evolved to successfully spread through the soft-shell clam population as a contagious cancer, utilizing pathways known to be conserved in human cancers as well as pathways unique to long-lived transmissible cancers.

传播性癌症是癌细胞逃离其原始宿主并以克隆系的形式在人群中传播的独特情况,在塔斯马尼亚袋獾、狗和十种双壳类动物中都有记录。要使癌细胞反复传播到新宿主,这些细胞系必须避开强大的传播障碍,特别是类似转移的物理转移到新宿主体内以及宿主免疫系统的排斥反应。我们量化了在软壳蛤(Mya arenaria)种群中传播的可传播癌系的基因表达,以研究其成功成为可传播癌系的潜在驱动因素,并观察到基因和基因通路的广泛差异表达。我们观察到涉及基因毒性应激反应、核糖体生物发生和 RNA 处理的基因上调,以及涉及肿瘤抑制、细胞粘附和免疫反应的基因下调。我们还观察到有证据表明,广泛的基因组不稳定性会通过基因融合、拷贝数变异和转座元件插入影响癌症转录组。最后,我们将癌细胞培养在海水(假定的宿主间传播媒介)中,观察到癌细胞在停止新陈代谢、避免凋亡和在低营养环境中存活方面的一致反应。有趣的是,这些反应中有许多也存在于健康的蛤细胞中,这表明双壳类动物的血细胞可能具有固有的海水生存反应,这可能部分解释了为什么传染性癌症在双壳类动物中如此常见。总之,这项研究揭示了这一血统可能进化成在软壳蛤群体中成功传播传染性癌症的多种机制,利用了已知在人类癌症中保守的途径以及长寿命传染性癌症特有的途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
PLoS Genetics
PLoS Genetics GENETICS & HEREDITY-
自引率
2.20%
发文量
438
期刊介绍: PLOS Genetics is run by an international Editorial Board, headed by the Editors-in-Chief, Greg Barsh (HudsonAlpha Institute of Biotechnology, and Stanford University School of Medicine) and Greg Copenhaver (The University of North Carolina at Chapel Hill). Articles published in PLOS Genetics are archived in PubMed Central and cited in PubMed.
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