Keratin 19 binds and regulates cytoplasmic HNRNPK mRNA targets in triple-negative breast cancer.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Arwa Fallatah, Dimitrios G Anastasakis, Amirhossein Manzourolajdad, Pooja Sharma, Xiantao Wang, Alexis Jacob, Sarah Alsharif, Ahmed Elgerbi, Pierre A Coulombe, Markus Hafner, Byung Min Chung
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Abstract

Background: Heterogeneous nuclear ribonucleoprotein K (HNRNPK) regulates pre-mRNA processing and long non-coding RNA localization in the nucleus. It was previously shown that shuttling of HNRNPK to the cytoplasm promotes cell proliferation and cancer metastasis. However, the mechanism of HNRNPK cytoplasmic localization, its cytoplasmic RNA ligands, and impact on post-transcriptional gene regulation remain uncharacterized.

Results: Here we show that the intermediate filament protein Keratin 19 (K19) directly interacts with HNRNPK and sequesters it in the cytoplasm. Correspondingly, in K19 knockout breast cancer cells, HNRNPK does not localize in the cytoplasm, resulting in reduced cell proliferation. We comprehensively mapped HNRNPK binding sites on mRNAs and showed that, in the cytoplasm, K19-mediated HNRNPK-retention increases the abundance of target mRNAs bound to the 3' untranslated region (3'UTR) at the expected cytidine-rich (C-rich) sequence elements. Furthermore, these mRNAs protected by HNRNPK in the cytoplasm are typically involved in cancer progression and include the p53 signaling pathway that is dysregulated upon HNRNPK knockdown (HNRNPK KD) or K19 knockout (KRT19 KO).

Conclusions: This study identifies how a cytoskeletal protein can directly regulate gene expression by controlling the subcellular localization of RNA-binding proteins to support pathways involved in cancer progression.

角蛋白19结合并调节三阴性乳腺癌细胞质HNRNPK mRNA靶点。
背景:异质核核糖核蛋白K (HNRNPK)调节前mrna加工和长链非编码RNA在细胞核中的定位。先前的研究表明,将HNRNPK转运到细胞质中可以促进细胞增殖和肿瘤转移。然而,HNRNPK的胞质定位机制、胞质RNA配体及其对转录后基因调控的影响尚不清楚。结果:在这里我们发现中间丝蛋白角蛋白19 (K19)直接与HNRNPK相互作用并将其隔离在细胞质中。相应地,在K19敲除的乳腺癌细胞中,HNRNPK不在细胞质中定位,导致细胞增殖减少。我们全面绘制了HNRNPK在mrna上的结合位点,结果表明,在细胞质中,k19介导的HNRNPK保留增加了在预期的富胞苷(C-rich)序列元件上结合到3'非翻译区(3' utr)的目标mrna的丰度。此外,细胞质中这些受HNRNPK保护的mrna通常参与癌症进展,包括在HNRNPK敲低(HNRNPK KD)或K19敲除(KRT19 KO)时失调的p53信号通路。结论:本研究确定了细胞骨架蛋白如何通过控制rna结合蛋白的亚细胞定位来直接调节基因表达,从而支持参与癌症进展的途径。
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
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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