VMA21: unveiling a novel oncogene that facilitates immune evasion in triple-negative breast cancer through TCIRG1 protein stability regulation.

IF 3.6 3区 医学 Q2 ONCOLOGY
American journal of cancer research Pub Date : 2024-08-25 eCollection Date: 2024-01-01 DOI:10.62347/NGSD3193
Xiangyang Guo, Zhiqiang Chen, Yongmin Miao, Guochen Zhang, Lifeng Miao
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引用次数: 0

Abstract

Background: VMA21 has been shown to be dysregulated in a number of cancers. However, no study has yet explored whether VMA21 is involved in the regulation of triple-negative breast cancer (TNBC), especially from the level of immune escape.

Methods: The Gene Expression Omnibus (GEO) database was accessed to obtain the microarray dataset identified as GSE38959, which was then subjected to an analysis aimed at identifying genes that are differentially expressed (DEGs). The researchers examined the expression of VMA21 in TNBC cell lines. After knockdown of VMA21 in TNBC cells, cell proliferation, invasion, and migration were assessed by clone formation, cell scratch, and Transwell assay, respectively. The effect of VMA21 on immune cell function was explored by cell co-culture method, which was used to assess how TNBC cells with suppressed VMA21 expression affected CD8+ T cytotoxic potential and cytokine secretion. The effect of VMA21 on TCIRG1 protein stability and ubiquitination was assessed using immunoprecipitation. The effects of VMA21 knockdown on tumor xenograft growth and CD8+ T cell immune infiltration in mice were further evaluated.

Results: VMA21 expression is significantly elevated across various cell lines of TNBC. Furthermore, the perturbation of VMA21 notably suppresses key cell viability parameters in TNBC cells, including their proliferation, invasiveness, and migratory abilities. The modulation of VMA21 in TNBC cells can lead to a substantial augmentation in CD8+ T cell effectiveness. VMA21 stabilizes TCIRG1 protein expression by inhibiting its ubiquitination degradation. Further, VMA21 is involved in regulating TNBC cell proliferation, invasion and immune escape by promoting TCIRG1 expression.

Conclusions: VMA21 is able to regulate TCIRG1 protein stability by binding to TCIRG1 protein in the form of ubiquitination, which ultimately promotes the malignant behavior as well as immune escape of TNBC cells.

VMA21:揭示通过 TCIRG1 蛋白稳定性调控促进三阴性乳腺癌免疫逃避的新型癌基因。
背景:VMA21已被证明在多种癌症中失调。然而,尚未有研究探讨 VMA21 是否参与了三阴性乳腺癌(TNBC)的调控,尤其是从免疫逃逸的层面:方法:研究人员访问了基因表达总库(GEO)数据库,获得了名为 GSE38959 的微阵列数据集,然后对该数据集进行了分析,旨在确定差异表达基因(DEGs)。研究人员检测了VMA21在TNBC细胞系中的表达情况。在 TNBC 细胞中敲除 VMA21 后,细胞增殖、侵袭和迁移分别通过克隆形成、细胞划痕和 Transwell 试验进行了评估。VMA21对免疫细胞功能的影响通过细胞共培养法进行了探讨,该方法用于评估VMA21表达被抑制的TNBC细胞如何影响CD8+ T细胞毒性潜能和细胞因子分泌。免疫沉淀法评估了VMA21对TCIRG1蛋白稳定性和泛素化的影响。进一步评估了 VMA21 敲除对小鼠肿瘤异种移植生长和 CD8+ T 细胞免疫浸润的影响:结果:在 TNBC 的各种细胞系中,VMA21 的表达均明显升高。此外,VMA21 的干扰会明显抑制 TNBC 细胞的关键细胞活力参数,包括其增殖、侵袭性和迁移能力。调控 TNBC 细胞中的 VMA21 可大幅提高 CD8+ T 细胞的有效性。VMA21 通过抑制 TCIRG1 蛋白的泛素化降解来稳定其表达。此外,VMA21通过促进TCIRG1的表达,参与调控TNBC细胞的增殖、侵袭和免疫逃逸:结论:VMA21能以泛素化的形式与TCIRG1蛋白结合,从而调节TCIRG1蛋白的稳定性,最终促进TNBC细胞的恶性行为和免疫逃逸。
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来源期刊
自引率
3.80%
发文量
263
期刊介绍: The American Journal of Cancer Research (AJCR) (ISSN 2156-6976), is an independent open access, online only journal to facilitate rapid dissemination of novel discoveries in basic science and treatment of cancer. It was founded by a group of scientists for cancer research and clinical academic oncologists from around the world, who are devoted to the promotion and advancement of our understanding of the cancer and its treatment. The scope of AJCR is intended to encompass that of multi-disciplinary researchers from any scientific discipline where the primary focus of the research is to increase and integrate knowledge about etiology and molecular mechanisms of carcinogenesis with the ultimate aim of advancing the cure and prevention of this increasingly devastating disease. To achieve these aims AJCR will publish review articles, original articles and new techniques in cancer research and therapy. It will also publish hypothesis, case reports and letter to the editor. Unlike most other open access online journals, AJCR will keep most of the traditional features of paper print that we are all familiar with, such as continuous volume, issue numbers, as well as continuous page numbers to retain our comfortable familiarity towards an academic journal.
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