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N-糖基化模式与肝细胞癌的遗传亚型相关。

N-Glycosylation Patterns Correlate with Hepatocellular Carcinoma Genetic Subtypes.

机构信息

Department of Cell and Molecular Pharmacology, Medical University of South Carolina, Charleston, South Carolina.

University of Texas Southwestern Medical Center, Dallas, Texas.

出版信息

Mol Cancer Res. 2021 Nov;19(11):1868-1877. doi: 10.1158/1541-7786.MCR-21-0348. Epub 2021 Aug 11.

Abstract

Hepatocellular carcinoma (HCC) is the second leading cause of cancer deaths globally, and the incidence rate in the United States is increasing. Studies have identified inter- and intratumor heterogeneity as histologic and/or molecular subtypes/variants associated with response to certain molecular targeted therapies. Spatial HCC tissue profiling of N-linked glycosylation by matrix-assisted laser desorption ionization imaging mass spectrometry (MALDI-IMS) may serve as a new method to evaluate the tumor heterogeneity. Previous work has identified significant changes in the N-linked glycosylation of HCC tumors but has not accounted for the heterogeneous genetic and molecular nature of HCC. To determine the correlation between HCC-specific N-glycosylation changes and genetic/molecular tumor features, we profiled HCC tissue samples with MALDI-IMS and correlated the spatial N-glycosylation with a widely used HCC molecular classification (Hoshida subtypes). MALDI-IMS data displayed trends that could approximately distinguish between subtypes, with subtype 1 demonstrating significantly dysregulated N-glycosylation versus adjacent nontumor tissue. Although there were no individual N-glycan structures that could identify specific subtypes, trends emerged regarding the correlation of branched glycan expression to HCC as a whole and fucosylated glycan expression to subtype 1 tumors specifically. IMPLICATIONS: Correlating N-glycosylation to specific subtypes offers the specific detection of subtypes of HCC, which could both enhance early HCC sensitivity and guide targeted clinical therapies.

摘要

肝细胞癌 (HCC) 是全球癌症死亡的第二大主要原因,美国的发病率正在上升。研究已经确定了肿瘤内和肿瘤间的异质性,包括与某些分子靶向治疗反应相关的组织学和/或分子亚型/变体。基质辅助激光解吸电离成像质谱 (MALDI-IMS) 对 HCC 组织中 N-连接糖基化的空间分析可能成为评估肿瘤异质性的新方法。以前的工作已经确定了 HCC 肿瘤中 N-连接糖基化的显著变化,但没有考虑到 HCC 的异质性遗传和分子性质。为了确定 HCC 特异性 N-糖基化变化与遗传/分子肿瘤特征之间的相关性,我们使用 MALDI-IMS 对 HCC 组织样本进行了分析,并将空间 N-糖基化与广泛使用的 HCC 分子分类 (Hoshida 亚型) 相关联。MALDI-IMS 数据显示出可以大致区分亚型的趋势,与相邻非肿瘤组织相比,亚型 1 表现出明显失调的 N-糖基化。尽管没有可以识别特定亚型的个体 N-聚糖结构,但关于分支聚糖表达与 HCC 整体的相关性以及岩藻糖基化聚糖表达与亚型 1 肿瘤的相关性出现了趋势。意义:将 N-糖基化与特定亚型相关联提供了 HCC 亚型的特异性检测,这既可以提高早期 HCC 的敏感性,又可以指导靶向临床治疗。

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