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肺癌中合成血型抗原相关寡糖结合的细胞类型依赖性改变

Cell type-dependent alterations of binding of synthetic blood group antigen-related oligosaccharides in lung cancer.

作者信息

Kayser K, Bovin N V, Zemlyanukhina T V, Donaldo-Jacinto S, Koopmann J, Gabius H J

机构信息

Department of Pathology, Thoraxklinik, Heidelberg, FRG.

出版信息

Glycoconj J. 1994 Aug;11(4):339-44. doi: 10.1007/BF00731207.

Abstract

Blood group antigen-related oligosaccharides have been implicated in growth regulation, cell mobility control and adhesion; we are therefore interested in the localization of receptors for these oligosaccharides in tumour cells. Labelled neoglycoconjugates that carry synthetic sugar structures are suitable tools to determine: whether such binding sites are present in human lung cancer; whether structural alterations of the glycoligand part will affect extent of binding; and whether cell type-associated alterations can be detected. Sections from 121 cases of lung cancer, representing small cell and non-small cell lung carcinoma, mesothelioma and metastases from extrapulmonary primary carcinomas were used to study the binding of nine synthetic AH- and Le-related oligosaccharides. Probes with fucose-alpha 1-3/4-N-acetylglucosamine-beta 1-R, an A-like disaccharide and 3'-sulfated galactose as ligand appear to bind less well to small cell than to non-small cell lung cancer cases, whereas Lec-disaccharide distinguishes mesothelioma from metastatic carcinoma. The latter ligand, A-like disaccharide and H (type III)-like trisaccharide exhibit evident cell type-associated differences in extent of binding. Thus, tailor-made neoglycoconjugates constitute a promising class of histopathological tools that warrants further study.

摘要

血型抗原相关寡糖与生长调节、细胞运动控制及黏附有关;因此,我们对这些寡糖在肿瘤细胞中的受体定位感兴趣。携带合成糖结构的标记新糖缀合物是确定以下内容的合适工具:此类结合位点是否存在于人类肺癌中;糖配体部分的结构改变是否会影响结合程度;以及是否能检测到细胞类型相关的改变。来自121例肺癌(包括小细胞肺癌和非小细胞肺癌、间皮瘤以及肺外原发性癌转移灶)的切片用于研究9种合成的A抗原和Lewis抗原相关寡糖的结合情况。以岩藻糖-α1-3/4-N-乙酰葡糖胺-β1-R、一种A样二糖和3'-硫酸化半乳糖作为配体的探针似乎与小细胞肺癌的结合不如与非小细胞肺癌的结合好,而Lec-二糖可将间皮瘤与转移癌区分开来。后一种配体、A样二糖和H(III型)样三糖在结合程度上表现出明显的细胞类型相关差异。因此,量身定制的新糖缀合物构成了一类有前景的组织病理学工具,值得进一步研究。

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