Transcriptional background effects on a tumor driver gene in different pigment cell types of medaka

IF 1.8 3区 生物学 Q3 DEVELOPMENTAL BIOLOGY Journal of experimental zoology. Part B, Molecular and developmental evolution Pub Date : 2023-10-25 DOI:10.1002/jez.b.23224
Shahad Abdulsahib, William Boswell, Mikki Boswell, Markita Savage, Manfred Schartl, Yuan Lu
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Abstract

The Xiphophorus melanoma receptor kinase gene, xmrk, is a bona fide oncogene driving melanocyte tumorigenesis of Xiphophorus fish. When ectopically expressed in medaka, it not only induces development of several pigment cell tumor types in different strains of medaka but also induces different tumor types within the same animal, suggesting its oncogenic activity has a transcriptomic background effect. Although the central pathways that xmrk utilizes to lead to melanomagenesis are well documented, genes and genetic pathways that modulate the oncogenic effect and alter the course of disease have not been studied so far. To understand how the genetic networks between different histocytes of xmrk-driven tumors are composed, we isolated two types of tumors, melanoma and xanthoerythrophoroma, from the same xmrk transgenic medaka individuals, established the transcriptional profiles of both xmrk-driven tumors, and compared (1) genes that are co-expressed with xmrk in both tumor types, and (2) differentially expressed genes and their associated molecular functions, between the two tumor types. Transcriptomic comparisons between the two tumor types show melanoma and xanthoerythrophoroma are characterized by transcriptional features representing varied functions, indicating distinct molecular interactions between the driving oncogene and the cell-type-specific transcriptomes. Melanoma tumors exhibit gene signatures that are relevant to proliferation and invasion, while xanthoerythrophoroma tumors are characterized by expression profiles related to metabolism and DNA repair. We conclude the transcriptomic backgrounds, exemplified by cell-type-specific genes that are downstream of xmrk effected signaling pathways, contribute the potential to change the course of tumor development and may affect overall tumor outcomes.

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不同色素细胞类型对肿瘤驱动基因的转录背景效应。
剑鱼黑色素瘤受体激酶基因xmrk是驱动剑鱼黑素细胞肿瘤发生的真正致癌基因。当它在青金石中异位表达时,它不仅在不同的青金石菌株中诱导几种色素细胞肿瘤类型的发展,而且在同一动物中诱导不同的肿瘤类型,这表明它的致癌活性具有转录组背景效应。尽管xmrk用来导致黑色素瘤的中心途径已经有了很好的记录,但到目前为止,调节致癌作用和改变疾病进程的基因和遗传途径还没有得到研究。为了了解xmrk驱动的肿瘤的不同组织细胞之间的遗传网络是如何组成的,我们从同一个xmrk转基因梅达卡个体中分离出两种类型的肿瘤,黑色素瘤和黄红细胞瘤,建立了两种xmrk驱动肿瘤的转录谱,并比较了(1)在两种肿瘤类型中与xmrk共表达的基因,以及(2)两种肿瘤类型之间的差异表达基因及其相关分子功能。两种肿瘤类型之间的转录组学比较表明,黑色素瘤和黄红细胞瘤的特征是代表不同功能的转录特征,表明驱动癌基因和细胞类型特异性转录组之间存在不同的分子相互作用。黑色素瘤肿瘤表现出与增殖和侵袭相关的基因特征,而黄红细胞瘤肿瘤的特征是与代谢和DNA修复相关的表达谱。我们得出结论,转录组背景,以xmrk影响的信号通路下游的细胞类型特异性基因为例,有可能改变肿瘤发展过程,并可能影响整体肿瘤结果。
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来源期刊
CiteScore
4.80
自引率
9.10%
发文量
63
审稿时长
6-12 weeks
期刊介绍: Developmental Evolution is a branch of evolutionary biology that integrates evidence and concepts from developmental biology, phylogenetics, comparative morphology, evolutionary genetics and increasingly also genomics, systems biology as well as synthetic biology to gain an understanding of the structure and evolution of organisms. The Journal of Experimental Zoology -B: Molecular and Developmental Evolution provides a forum where these fields are invited to bring together their insights to further a synthetic understanding of evolution from the molecular through the organismic level. Contributions from all these branches of science are welcome to JEZB. We particularly encourage submissions that apply the tools of genomics, as well as systems and synthetic biology to developmental evolution. At this time the impact of these emerging fields on developmental evolution has not been explored to its fullest extent and for this reason we are eager to foster the relationship of systems and synthetic biology with devo evo.
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