sry相关的高迁移率组框17通过拮抗无翼相关整合位点通路发挥肿瘤抑制作用。

IF 2.5 Q3 ONCOLOGY
Maha Anani, Ikuo Nobuhisa, Tetsuya Taga
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引用次数: 2

摘要

转录因子sry相关的高迁移率群盒(Sox) 17参与精子发生、心血管系统、内胚层形成等发育过程。本文首先综述了Sox17表达与肿瘤恶性关系的研究进展。虽然Sox17积极促进各种组织发育,但大多数与Sox17相关的癌症显示Sox17表达水平降低,并且Sox17表达与恶性肿瘤呈负相关。我们通过关注Sox17基因启动子中CpG位点的DNA甲基化,简要讨论了Sox17下调的机制。接下来,我们概述了Sox17在胎儿造血中的功能,特别是在妊娠小鼠胚胎的背主动脉中。Sox17在含造血干细胞(HSC)的主动脉内造血细胞簇(IAHCs)中的表达对具有造血能力的造血细胞簇的形成具有重要意义。Sox17在成人骨髓造血干细胞和背主动脉IAHCs中持续表达,表明移植实验中淋巴细胞嵌合率低,普通髓祖细胞增殖异常。然后我们总结了Sox17在癌症控制中的研究前景。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Sry-related High Mobility Group Box 17 Functions as a Tumor Suppressor by Antagonizing the Wingless-related Integration Site Pathway.

Sry-related High Mobility Group Box 17 Functions as a Tumor Suppressor by Antagonizing the Wingless-related Integration Site Pathway.

Sry-related High Mobility Group Box 17 Functions as a Tumor Suppressor by Antagonizing the Wingless-related Integration Site Pathway.

A transcription factor Sry-related high mobility group box (Sox) 17 is involved in developmental processes including spermatogenesis, cardiovascular system, endoderm formation, and so on. In this article, we firstly review the studies on the relation between the Sox17 expression and tumor malignancy. Although Sox17 positively promotes various tissue development, most of the cancers associated with Sox17 show decreased expression levels of Sox17, and an inverse correlation between Sox17 expression and malignancy is revealed. We briefly discuss the mechanism of such Sox17 down-regulation by focusing on DNA methylation of CpG sites located in the Sox17 gene promoter. Next, we overview the function of Sox17 in the fetal hematopoiesis, particularly in the dorsal aorta in midgestation mouse embryos. The Sox17 expression in hematopoietic stem cell (HSC)-containing intra-aortic hematopoietic cell cluster (IAHCs) is important for the cluster formation with the hematopoietic ability. The sustained expression of Sox17 in adult bone marrow HSCs and the cells in IAHCs of the dorsal aorta indicate abnormalities that are low lymphocyte chimerism and the aberrant proliferation of common myeloid progenitors in transplantation experiments. We then summarize the perspectives of Sox17 research in cancer control.

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