Hepatocyte growth factor promotes melanoma metastasis through ubiquitin-specific peptidase 22-mediated integrins upregulation

IF 9.1 1区 医学 Q1 ONCOLOGY
Qiong Gao , Na Li , Yujie Pan , Peng Chu , Yuanzhang Zhou , Huijun Jia , Yang Cheng , Guoqing Xue , Jiankun Song , Yue Zhang , Houyu Zhu , Jia Sun , Bin Zhang , Zhaolin Sun , Deyu Fang
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引用次数: 0

Abstract

Hepatocyte growth factor (HGF) plays a critical role in promoting tumor migration, invasion, and metastasis, partly by upregulating integrins. The molecular mechanisms behind how HGF facilitates integrin-mediated tumorigenesis are not fully understood. In this study, we demonstrate that the ubiquitin-specific peptidase 22 (USP22) is essential for HGF-induced melanoma metastasis. HGF treatment dramatically increased the expression of both USP22 and multiple integrin family members in particular ITGAV, ITGB3, and ITGA1. An unbiased analysis of the TCGA database reveals integrins as common downstream targets of both USP22 and HGF across multiple human cancer types. Notably, CRISPR-mediated deletion of USP22 completely eliminates HGF-induced integrin expression in melanoma cells. At the molecular level, USP22 acts as a bona fide deubiquitinase for Sp1, a transcription factor for the ITGAV, ITGB3, and ITGA1 genes. USP22 interacts with and inhibits Sp1 ubiquitination, protecting against Sp1 proteasomal degradation. Supporting this, immunohistology analysis detects a positive correlation among USP22, Sp1, and integrin αv in human melanoma tissues. This study identifies the death from the signature gene USP22 as a critical positive regulator for HGF-induced integrin expression by deubiquitinating the Sp1 transcription factor during melanoma metastasis.

肝细胞生长因子通过泛素特异性肽酶22介导的整合素上调促进黑色素瘤转移
肝细胞生长因子(HGF)在促进肿瘤迁移、侵袭和转移方面起着至关重要的作用,部分原因是它能上调整合素。目前还不完全清楚肝细胞生长因子如何促进整合素介导的肿瘤发生背后的分子机制。在这项研究中,我们证明泛素特异性肽酶 22(USP22)对 HGF 诱导的黑色素瘤转移至关重要。HGF 处理会显著增加 USP22 和多种整合素家族成员的表达,尤其是 ITGAV、ITGB3 和 ITGA1。对 TCGA 数据库的无偏见分析表明,整合素是 USP22 和 HGF 在多种人类癌症类型中的共同下游靶点。值得注意的是,CRISPR 介导的 USP22 基因缺失完全消除了黑色素瘤细胞中 HGF 诱导的整合素表达。在分子水平上,USP22 是 Sp1 的真正去泛素化酶,而 Sp1 是 ITGAV、ITGB3 和 ITGA1 基因的转录因子。USP22 与 Sp1 相互作用并抑制其泛素化,从而防止 Sp1 蛋白质体降解。免疫组织学分析发现,USP22、Sp1 和人类黑色素瘤组织中的整合素 αv 之间存在正相关,这也证明了这一点。这项研究确定了特征基因 USP22 的死亡是黑色素瘤转移过程中通过去泛素化 Sp1 转录因子来调节 HGF 诱导的整合素表达的关键正向调节因子。
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来源期刊
Cancer letters
Cancer letters 医学-肿瘤学
CiteScore
17.70
自引率
2.10%
发文量
427
审稿时长
15 days
期刊介绍: Cancer Letters is a reputable international journal that serves as a platform for significant and original contributions in cancer research. The journal welcomes both full-length articles and Mini Reviews in the wide-ranging field of basic and translational oncology. Furthermore, it frequently presents Special Issues that shed light on current and topical areas in cancer research. Cancer Letters is highly interested in various fundamental aspects that can cater to a diverse readership. These areas include the molecular genetics and cell biology of cancer, radiation biology, molecular pathology, hormones and cancer, viral oncology, metastasis, and chemoprevention. The journal actively focuses on experimental therapeutics, particularly the advancement of targeted therapies for personalized cancer medicine, such as metronomic chemotherapy. By publishing groundbreaking research and promoting advancements in cancer treatments, Cancer Letters aims to actively contribute to the fight against cancer and the improvement of patient outcomes.
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