Novel Pannexin 1 isoform is increased in cancer

Brooke L O'Donnell, Dan Stefan, Yu-Hsin Chiu, Michael Zeitz, Justin Tang, Danielle Johnston, Stephanie Leighton, Carlijn Van Kessell, Kevin Barr, Laszlo Gyenis, Taylor Freeman, John J Kelly, Samar Sayedyahossein, David W Litchfield, Kathryn Roth, James W Smyth, Matthew Hebb, John Ronald, Douglas A Bayliss, Silvia Penuela
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Abstract

Pannexin 1 (PANX1) is upregulated in many cancers, where its activity and signalling promote tumorigenic properties. Here, we report a novel ~25 kDa isoform of human PANX1 (hPANX1-25K) which lacks the N-terminus and was detected in several human cancer cell lines including melanoma, osteosarcoma,breast cancer and glioblastoma multiforme. This isoform was increased upon hPANX1 CRISPR/Cas9 deletion targeting the first exon near M1, suggesting a potential alternative translation initiation (ATI) site. hPANX1-25K was confirmed to be a hPANX1 isoform via mass spectrometry, can be N-linked glycosylated at N254, and can interact with both β-catenin and full length hPANX1. A double deletion of hPANX1 and hPANX1-25K reduces cell growth and viability in cancer cells. hPANX1-25K is prevalent throughout melanoma progression, and its levels are increased in squamous cell carcinoma cells and patient-derived tumours, compared to keratinocytes and normal skin controls, indicating that it may be differentially regulated in normal and cancer cells.
新型 Pannexin 1 同工酶在癌症中增加
Pannexin 1(PANX1)在许多癌症中上调,其活性和信号传导促进了致癌特性。在这里,我们报告了一种新的 ~25 kDa 人 PANX1 异构体(hPANX1-25K),它缺乏 N-末端,并在几种人类癌症细胞系中被检测到,包括黑色素瘤、骨肉瘤、乳腺癌和多形性胶质母细胞瘤。通过质谱分析证实 hPANX1-25K 是一种 hPANX1 异构体,可在 N254 处进行 N-连接糖基化,并能与β-catenin 和全长 hPANX1 相互作用。与角质形成细胞和正常皮肤对照组相比,hPANX1-25K 在鳞状细胞癌细胞和患者衍生肿瘤中的水平升高,这表明它在正常细胞和癌细胞中可能受到不同的调控。
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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