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激活素和骨形态发生蛋白信号在人睾丸癌细胞系中的作用,以及核质转运蛋白 Importin-5 在它们相互作用中的作用。

Activin and BMP Signalling in Human Testicular Cancer Cell Lines, and a Role for the Nucleocytoplasmic Transport Protein Importin-5 in Their Crosstalk.

机构信息

Centre for Reproductive Health, Hudson Institute of Medical Research, 27-31 Kanooka Grove, Clayton, VIC 3168, Australia.

Department of Surgery, Royal Melbourne Hospital, University of Melbourne, Parkville, VIC 3050, Australia.

出版信息

Cells. 2023 Mar 24;12(7):1000. doi: 10.3390/cells12071000.

Abstract

Testicular germ cell tumours (TGCTs) are the most common malignancy in young men. Originating from foetal testicular germ cells that fail to differentiate correctly, TGCTs appear after puberty as germ cell neoplasia in situ cells that transform through unknown mechanisms into distinct seminoma and non-seminoma tumour types. A balance between activin and BMP signalling may influence TGCT emergence and progression, and we investigated this using human cell line models of seminoma (TCam-2) and non-seminoma (NT2/D1). Activin A- and BMP4-regulated transcripts measured at 6 h post-treatment by RNA-sequencing revealed fewer altered transcripts in TCam-2 cells but a greater responsiveness to activin A, while BMP4 altered more transcripts in NT2/D1 cells. Activin significantly elevated transcripts linked to pluripotency, cancer, TGF-β, Notch, p53, and Hippo signalling in both lines, whereas BMP4 altered TGF-β, pluripotency, Hippo and Wnt signalling components. Dose-dependent antagonism of BMP4 signalling by activin A in TCam-2 cells demonstrated signalling crosstalk between these two TGF-β superfamily arms. Levels of the nuclear transport protein, IPO5, implicated in BMP4 and WNT signalling, are highly regulated in the foetal mouse germline. knockdown in TCam-2 cells using siRNA blunted BMP4-induced transcript changes, indicating that IPO5 levels could determine TGF-β signalling pathway outcomes in TGCTs.

摘要

睾丸生殖细胞肿瘤 (TGCTs) 是年轻男性中最常见的恶性肿瘤。它们起源于未能正常分化的胎儿睾丸生殖细胞,在青春期后作为原位生殖细胞瘤出现,通过未知机制转化为明显的精原细胞瘤和非精原细胞瘤肿瘤类型。激活素和 BMP 信号之间的平衡可能会影响 TGCT 的发生和进展,我们使用精原细胞瘤 (TCam-2) 和非精原细胞瘤 (NT2/D1) 的人类细胞系模型对此进行了研究。RNA 测序在治疗后 6 小时测量的激活素 A 和 BMP4 调节的转录本显示,TCam-2 细胞中改变的转录本较少,但对激活素 A 的反应更大,而 BMP4 在 NT2/D1 细胞中改变了更多的转录本。激活素显著增加了两条信号通路中与多能性、癌症、TGF-β、Notch、p53 和 Hippo 信号相关的转录本,而 BMP4 改变了 TGF-β、多能性、Hippo 和 Wnt 信号成分。TCam-2 细胞中 BMP4 信号的激活素 A 依赖性拮抗作用表明这两个 TGF-β 超家族分支之间存在信号串扰。参与 BMP4 和 WNT 信号的核转运蛋白 IPO5 的水平在胎儿鼠生殖系中受到高度调节。用 siRNA 敲低 TCam-2 细胞中的 IPO5 减弱了 BMP4 诱导的转录本变化,表明 IPO5 水平可能决定 TGCT 中 TGF-β 信号通路的结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f71/10093041/b8f5cd205bd6/cells-12-01000-g001.jpg

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