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剑尾鱼中Xmrk诱导黑色素瘤形成的遗传、生化及进化方面

Genetic, biochemical and evolutionary facets of Xmrk-induced melanoma formation in the fish Xiphophorus.

作者信息

Meierjohann Svenja, Schartl Manfred, Volff Jean-Nicolas

机构信息

Physiologische Chemie I, Biozentrum, University of Würzburg, am Hubland, D-97074 Würzburg, Germany.

出版信息

Comp Biochem Physiol C Toxicol Pharmacol. 2004 Jul;138(3):281-9. doi: 10.1016/j.cca.2004.06.002.

Abstract

Certain interspecific hybrids of the fish Xiphophorus spontaneously develop melanoma induced by the derepression of the Xmrk oncogene. Xmrk is a recent duplicate of an orthologue of the mammalian epidermal growth factor receptor gene Egfr. In addition to a specific overexpression in melanoma, amino-acid substitutions in the extracellular domain leading to ligand-independent dimerisation and constitutive autophosphorylation are responsible for the tumorigenic potential of Xmrk. The Xmrk receptor induces several signal transduction pathways mediating cell proliferation and resistance to apoptosis and initiating dedifferentiation. Moreover, Xmrk upregulates the expression of the secreted protein osteopontin, inducing an autocrine loop possibly allowing invasion and survival in the dermis as a first step in malignancy. Hence, Xmrk is able to induce pathways essential for a transformed phenotype. Some of these events are equivalent to those found downstream of the mammalian Egfr, but others have clearly evolved differently or are specific for pigment cells. Xmrk is potentially hazardous, nonessential and located in a very unstable genomic region. Nevertheless, Xmrk has been maintained under purifying selection in divergent Xiphophorus species. Hence, Xmrk has probably a beneficial function under certain conditions. The analysis of this function is a major challenge for future research in the Xiphophorus model.

摘要

鱼类剑尾鱼属的某些种间杂种会自发形成由Xmrk癌基因去抑制诱导的黑色素瘤。Xmrk是哺乳动物表皮生长因子受体基因Egfr直系同源基因的近期复制产物。除了在黑色素瘤中特异性过表达外,细胞外结构域中的氨基酸取代导致不依赖配体的二聚化和组成型自磷酸化,这是Xmrk致瘤潜力的原因。Xmrk受体诱导多种信号转导途径,介导细胞增殖和抗凋亡,并引发去分化。此外,Xmrk上调分泌蛋白骨桥蛋白的表达,诱导自分泌环,这可能是恶性肿瘤第一步中允许在真皮中侵袭和存活的原因。因此,Xmrk能够诱导转化表型所必需的途径。其中一些事件与在哺乳动物Egfr下游发现的事件相当,但其他事件显然进化方式不同或对色素细胞具有特异性。Xmrk具有潜在危险性、非必需性且位于非常不稳定的基因组区域。然而,Xmrk在不同的剑尾鱼物种中一直处于纯化选择之下。因此,Xmrk在某些条件下可能具有有益功能。对该功能的分析是剑尾鱼模型未来研究的一项重大挑战。

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