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LIN28B 异构体特异性功能对 的差异化调控。

Differential Regulation of by LIN28B Isoform-Specific Functions.

机构信息

Division of Gastroenterology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania.

Department of Medicine, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania.

出版信息

Mol Cancer Res. 2018 Mar;16(3):403-416. doi: 10.1158/1541-7786.MCR-17-0514. Epub 2018 Jan 12.

Abstract

The RNA-binding protein LIN28B plays an important role in development, stem cell biology, and tumorigenesis. LIN28B has two isoforms: the LIN28B-long and -short isoforms. Although studies have revealed the functions of the LIN28B-long isoform in tumorigenesis, the role of the LIN28B-short isoform remains unclear and represents a major gap in the field. The LIN28B-long and -short isoforms are expressed in a subset of human colorectal cancers and adjacent normal colonic mucosa, respectively. To elucidate the functional and mechanistic aspects of these isoforms, colorectal cancer cells (Caco-2 and LoVo) were generated to either express no LIN28B or the -short or -long isoform. Interestingly, the long isoform suppressed expression and activated canonical RAS/ERK signaling, whereas the short isoform did not. The LIN28B-long isoform-expressing cells demonstrated increased drug resistance to 5-fluorouracil and cisplatin through the upregulation of ERCC1, a DNA repair gene, in a -dependent manner. The LIN28B-short isoform preserved its ability to bind pre-, without inhibiting the maturation of , and competed with the LIN28B-long isoform for binding to pre- Coexpression of the short isoform in the LIN28B-long isoform-expressing cells rescued the phenotypes induced by the LIN28B-long isoform. This study demonstrates the differential antagonistic functions of the LIN28B-short isoform against the LIN28B-long isoform through an inability to degrade , which leads to the novel premise that the short isoform may serve to counterbalance the long isoform during normal colonic epithelial homeostasis, but its downregulation during colonic carcinogenesis may reveal the protumorigenic effects of the long isoform. .

摘要

RNA 结合蛋白 LIN28B 在发育、干细胞生物学和肿瘤发生中发挥重要作用。LIN28B 有两种同工型:LIN28B-长和 -短同工型。尽管研究揭示了 LIN28B-长同工型在肿瘤发生中的作用,但 LIN28B-短同工型的作用仍不清楚,这是该领域的一个主要空白。LIN28B-长和 -短同工型分别在一部分人类结直肠癌和相邻正常结肠黏膜中表达。为了阐明这些同工型的功能和机制方面,生成了结直肠癌细胞(Caco-2 和 LoVo),以表达无 LIN28B 或 -短或 -长同工型。有趣的是,长同工型抑制了 的表达并激活了经典的 RAS/ERK 信号,而短同工型则没有。LIN28B-长同工型表达的细胞通过上调 DNA 修复基因 ERCC1(一种依赖于 -的方式)表现出对 5-氟尿嘧啶和顺铂的耐药性增加。LIN28B-短同工型保留了与其结合前体的能力,而不抑制 的成熟,并且与 LIN28B-长同工型竞争结合前体。在 LIN28B-长同工型表达的细胞中共表达短同工型可挽救由 LIN28B-长同工型诱导的表型。这项研究表明,LIN28B-短同工型通过不能降解 而对 LIN28B-长同工型发挥拮抗作用,从而产生新的前提,即短同工型可能在正常结肠上皮稳态中平衡长同工型,但在结肠癌变过程中其下调可能揭示长同工型的促肿瘤作用。

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