A. Chakraborty, M. Pérez, N. B. Mohammed, M. Wells, J. Wilmott, J. Thompson, S. Haslam, W. Wang, R. Scolyer, G. Murphy, C. Dimitroff
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引用次数: 0
Abstract
Metastatic melanoma is a lethal disease with a dismal 5-year survival rate. Thus, intense efforts to boost novel therapeutic strategies are underway to identify early detection of melanomas with a high propensity to metastasize. We recently discovered that the loss of cell surface glycan, I-antigen, corresponds with the transition of primary melanoma to metastatic melanoma. I-antigen or I-branched glycans are synthesized by β16, N-acetylglucosaminyltransferase 2 (GCNT2) and inversely correlate with the growth and signaling potential of metastatic melanoma cells. Moreover, compared with high GCNT2 expression in normal melanocytes, nevi, and early-stage primary melanomas, GCNT2 is conspicuously lost in metastatic melanomas. We anticipate the potential utilization of GCNT2 expression as a biomarker to predict melanoma metastasis. Further, metastasis and aggressive disease progression are key phenotypes of tumor-initiating cells (TIC), which are preferentially generated in areas of hypoxia. In the vertical growth phase of primary melanomas and melanoma metastases, the tumor microenvironment is typically hypoxic (1.5% oxygen). We hypothesize that the hypoxic microenvironment aids in metastatic melanoma progression through TIC generation and immune evasion, by downregulating GCNT2 and switching I-branched glycans to linear glycans. In this study, metastatic melanoma cells grown under hypoxic conditions had reduced GCNT2 and MITF with upregulated stem cell marker KLF4 expression. Importantly, in the in vivo TIC assay, we found significantly decreased tumor formation with increased GCNT2 expression while low GCNT2 levels enabled tumor formation even when 103 cells were injected in immunocompromised mice. Since TICs are thought to evade immune clearance, we investigated whether loss of GCNT2 increased TIC characteristics and also enabled immunosuppressive features. In human PBMC - metastatic melanoma co-cultures, there was an increase in T regulatory cell generation associated with low GCNT2 compared to high GCNT2 expression in melanoma cells, suggesting that loss of GCNT2 associates with increased TIC generation, tumor formation, and immunoevasion potential. Using melanoma patient specimens, immunohistochemical analysis of GCNT2 corresponded with a significant increase in mortality with the loss of GCNT2 staining. Altogether, these findings highlight GCNT2/I-branching not only as a biomarker of melanoma virulence but reveal malignancy-associated pathways functioning in parallel with loss of GCNT2/I-branching that could offer additional targets for the treatment of metastatic melanoma. Citation Format: Asmi Chakraborty, Mariana Perez, Norhan B. B Mohammed, Michael Wells, James S. Wilmott, John F. Thompson, Stuart M. Haslam, Wei Wang, Richard A. Scolyer, George F. Murphy, Charles J. Dimitroff. Hypoxia-mediated downregulation of GCNT2/I-antigen in metastatic melanoma accelerates disease progression and mortality [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 2609.
转移性黑色素瘤是一种致命的疾病,5年生存率很低。因此,人们正在努力推动新的治疗策略,以识别具有高转移倾向的黑色素瘤的早期检测。我们最近发现,细胞表面聚糖,即i抗原的丧失,与原发性黑色素瘤向转移性黑色素瘤的转变相对应。i抗原或i支链聚糖由β16, n -乙酰氨基葡萄糖转移酶2 (GCNT2)合成,与转移性黑色素瘤细胞的生长和信号传导潜能呈负相关。此外,与GCNT2在正常黑色素细胞、痣和早期原发性黑色素瘤中的高表达相比,GCNT2在转移性黑色素瘤中明显缺失。我们期待GCNT2表达作为预测黑色素瘤转移的生物标志物的潜在应用。此外,转移和侵袭性疾病进展是肿瘤启动细胞(TIC)的关键表型,它们优先在缺氧区域产生。在原发性黑色素瘤和黑色素瘤转移的垂直生长阶段,肿瘤微环境通常为缺氧(1.5%氧气)。我们假设缺氧微环境通过TIC的产生和免疫逃避,通过下调GCNT2和将i支聚糖转换为线性聚糖,有助于转移性黑色素瘤的进展。在这项研究中,在缺氧条件下生长的转移性黑色素瘤细胞GCNT2和MITF减少,干细胞标记物KLF4表达上调。重要的是,在体内TIC实验中,我们发现GCNT2表达增加显著减少肿瘤形成,而低GCNT2水平即使在免疫功能低下的小鼠中注射103个细胞也能促进肿瘤形成。由于TIC被认为会逃避免疫清除,我们研究了GCNT2的缺失是否会增加TIC的特征,并激活免疫抑制特征。在人类PBMC -转移性黑色素瘤共培养中,与黑色素瘤细胞中GCNT2高表达相比,GCNT2低表达的T调节细胞生成增加,这表明GCNT2的缺失与TIC生成、肿瘤形成和免疫逃避潜力增加有关。使用黑色素瘤患者标本,GCNT2的免疫组织化学分析表明,随着GCNT2染色的丧失,死亡率显著增加。总之,这些发现强调了GCNT2/ i分支不仅是黑色素瘤毒力的生物标志物,而且揭示了与GCNT2/ i分支缺失并行的恶性相关通路,可以为转移性黑色素瘤的治疗提供额外的靶点。引文格式:Asmi Chakraborty, Mariana Perez, Norhan B. B. Mohammed, Michael Wells, James S. Wilmott, John F. Thompson, Stuart M. Haslam, Wang Wei, Richard A. Scolyer, George F. Murphy, Charles J. Dimitroff缺氧介导的GCNT2/ i抗原在转移性黑色素瘤中的下调加速了疾病进展和死亡率[摘要]。见:美国癌症研究协会2021年年会论文集;2021年4月10日至15日和5月17日至21日。费城(PA): AACR;癌症杂志,2021;81(13 -增刊):2609。