Abrogation of USP9X Is a Potential Strategy to Decrease PEG10 Levels and Impede Tumor Progression in Cutaneous T-Cell Lymphoma.

The Journal of investigative dermatology Pub Date : 2024-12-01 Epub Date: 2024-04-26 DOI:10.1016/j.jid.2024.02.039
Shan Xiong, Fengjie Liu, Jingru Sun, Shuaixin Gao, Catherine C L Wong, Ping Tu, Yang Wang
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Abstract

Advanced-stage cutaneous T-cell lymphomas (CTCLs) are notorious for their highly aggressive behavior, resistance to conventional treatments, and poor prognosis, particularly when large-cell transformation occurs. PEG10 has been recently proposed as a potent driver for large-cell transformation in CTCL. However, the targeting of PEG10 continues to present a formidable clinical challenge that has yet to be addressed. In this study, we report an important post-translational regulatory mechanism of PEG10 in CTCL. USP9X, a deubiquitinase, interacted with and deubiquitinated PEG10, thereby stabilizing PEG10. Knockdown of USP9X or pharmacological targeting of USP9X resulted in a prominent downregulation of PEG10 and its downstream pathway in CTCL. Moreover, USP9X inhibition conferred tumor cell growth disadvantage and enhanced apoptosis in vitro, an effect that occurred in part through its regulation on PEG10. Furthermore, we demonstrated that inhibition of USP9X obviously restrained CTCL tumor growth in vivo and that high expression of USP9X is associated with poor survival in patients with CTCL. Collectively, our findings uncover USP9X as a key post-translational regulator in the stabilization of PEG10 and suggest that targeting PEG10 stabilization through USP9X inhibition may represent a promising therapeutic strategy for advanced-stage CTCL.

削弱 USP9X 是降低 PEG10 水平和阻碍皮肤 T 细胞淋巴瘤肿瘤进展的一种潜在策略。
晚期皮肤T细胞淋巴瘤(CTCL)因其高度侵袭性、对常规治疗的耐药性和不良预后而臭名昭著,尤其是发生大细胞转化(LCT)时。最近,有人提出父系表达基因10(PEG10)是导致CTCL发生大细胞转化的强大驱动因素。然而,PEG10 的靶向治疗仍然是一项艰巨的临床挑战,目前仍有待解决。在此,我们报告了PEG10在CTCL中的一种重要的翻译后调控机制。泛素特异性蛋白酶9X(USP9X)是一种去泛素化酶,它与PEG10相互作用并去泛素化,从而稳定了PEG10。敲除 USP9X 或药物靶向 USP9X 会导致 PEG10 及其下游通路在 CTCL 中显著下调。此外,体外抑制 USP9X 可抑制肿瘤细胞生长,并增强细胞凋亡,这种效应部分是通过其对 PEG10 的调控产生的。此外,我们还证明,抑制 USP9X 能明显抑制 CTCL 肿瘤在体内的生长,而且 USP9X 的高表达与 CTCL 患者的不良生存率有关。总之,我们的发现揭示了 USP9X 是 PEG10 稳定过程中的一个关键翻译后调控因子,并表明通过抑制 USP9X 来靶向稳定 PEG10 可能是一种治疗晚期 CTCL 的有效策略。
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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