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癌性患者恶性胸腔积液中可溶性Tn糖蛋白的生化特性

Biochemical characterization of soluble Tn glycoproteins from malignant effusions of patients with carcinomas.

作者信息

Freire Teresa, Medeiros Andrea, Reis Celso A, Real Francisco X, Osinaga Eduardo

机构信息

Depto. de Bioquímica, Laboratorio de Oncología Básica, Facultad de Medicina, Universidad de la República, Montevideo, Uruguay.

出版信息

Oncol Rep. 2003 Sep-Oct;10(5):1577-85.

Abstract

The Tn determinant (GalNAc-O-Ser/Thr) is one of the most specific human tumor markers. In normal cells Tn is a cryptic structure in the peptide core of mucin type O-glycoproteins, and it is detected in an unmasked form in most human carcinomas evaluated by immunohistochemistry. Scarce data are available regarding the characteristics of soluble Tn bearing glycoproteins. We herein report the first comparative characterization of soluble Tn glycoproteins derived from different kinds of human tumors (breast, colon, gastric, ovarian and liver). Considerable heterogeneity was observed in the physicochemical properties of Tn soluble glycoproteins from all the tumor-associated effusions evaluated. In SDS-PAGE analysis Tn glycoproteins from liver and colon effusions migrated as a broad single major component (>500 kDa), while several components of >200 kDa were identified in samples from breast, ovarian, and gastric cancer. The results of perchloric acid (PCA) treatment and CsCl gradient ultracentrifugation indicated that the Tn glycoproteins in effusion fluids correspond predominantly to mucin-like glycoproteins. However, in samples from patients with colon and liver cancer, a fraction of Tn glycoproteins formed part of the immune complexes that precipitated in PCA, suggesting that the anti-Tn immune response in vivo could modify their physicochemical properties. The four apomucins evaluated (MUC1, MUC2, MUC5AC and MUC6) carried Tn epitopes in each of the effusions, indicating that soluble apomucin detection may reflect the abnormal expression of MUC genes inherent to these tumors. Taking together, these results indicate that apomucin expression profile is responsible, at least in part, for the high heterogeneity of soluble Tn glycoproteins, and suggest that the identification of Tn determinant on the different soluble apomucins could be useful for the development of new diagnostic tools as well as to evaluate the anti-tumor immune response in patients with cancer.

摘要

Tn 决定簇(N-乙酰半乳糖胺-O-丝氨酸/苏氨酸)是最具特异性的人类肿瘤标志物之一。在正常细胞中,Tn 是粘蛋白型 O-糖蛋白肽核心中的一种隐蔽结构,在通过免疫组织化学评估的大多数人类癌组织中,它以未掩盖的形式被检测到。关于携带可溶性 Tn 的糖蛋白的特征,现有数据稀缺。我们在此报告了源自不同类型人类肿瘤(乳腺癌、结肠癌、胃癌、卵巢癌和肝癌)的可溶性 Tn 糖蛋白的首次比较特征。在所评估的所有肿瘤相关积液中,Tn 可溶性糖蛋白的物理化学性质存在相当大的异质性。在 SDS-PAGE 分析中,来自肝癌和结肠癌积液中的 Tn 糖蛋白迁移为一个宽泛的单一主要成分(>500 kDa),而在乳腺癌、卵巢癌和胃癌样本中鉴定出了几种 >200 kDa 的成分。高氯酸(PCA)处理和 CsCl 梯度超速离心的结果表明,积液中的 Tn 糖蛋白主要对应于粘蛋白样糖蛋白。然而,在结肠癌和肝癌患者的样本中,一部分 Tn 糖蛋白是 PCA 中沉淀的免疫复合物的一部分,这表明体内的抗 Tn 免疫反应可能会改变它们的物理化学性质。所评估的四种脱辅基粘蛋白(MUC1、MUC2、MUC5AC 和 MUC6)在每种积液中都带有 Tn 表位,这表明可溶性脱辅基粘蛋白检测可能反映了这些肿瘤固有的 MUC 基因的异常表达。综上所述,这些结果表明脱辅基粘蛋白表达谱至少部分导致了可溶性 Tn 糖蛋白的高度异质性,并表明鉴定不同可溶性脱辅基粘蛋白上的 Tn 决定簇可能有助于开发新的诊断工具以及评估癌症患者的抗肿瘤免疫反应。

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