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Differential expression of endogenous sugar-binding proteins (lectins) in murine tumor model systems with metastatic capacity.

作者信息

Gabius H J, Bandlow G, Schirrmacher V, Nagel G A, Vehmeyer K

出版信息

Int J Cancer. 1987 May 15;39(5):643-8. doi: 10.1002/ijc.2910390517.

DOI:10.1002/ijc.2910390517
PMID:3570557
Abstract

In order to investigate possible differences in sugar binding activities of strongly versus weakly metastatic tumors, sugar-binding molecules (endogenous lectins) of murine tumor cells differing in metastatic capacity were analyzed by affinity chromatography on supports with immobilized sugars or glycoproteins and compared. After elution with specific sugar in the absence of Ca2+-ions, the proteins were separated by sodium dodecyl sulfate-polyacrylamide slab gel electrophoresis. In comparison to a weakly metastatic subline (Eb) spontaneous strongly metastatic variants (ESb) of a murine lymphoma contained additional sugar receptors for N-acetylglucosamine (Mr 30 kDa) and maltose (Mr 64 kDa, 62 kDa, 54 kDa and 32 kDa), and lacked one sugar receptor for myoinositol (Mr 85 kDa), N-acetylglucosamine (Mr 23 kDa) and maltose (Mr 22 kDa), respectively. The strongly metastatic variant ESb expressed the common beta-galactoside-specific lectin to a higher extent and receptors for myo-inositol, melibiose and mannan to a lower extent. In another model system derived from the murine mastocytoma cell line P 815 X 2A, biochemical analysis of the liver-metastasizing variant P 815 X 2B revealed additional characteristic N-acetylgalactosamine- and maltose-specific binding proteins. This variant had reduced amounts of receptors for beta-galactosides and fucose in comparison to the parental clone. In a third tumor system a similar qualitative difference was disclosed: a metastatic variant derived from spleen metastases displayed a sugar receptor profile with 5 additional beta-galactoside-binding proteins when compared to its parental clone 6-6#3 + F, which is a virally transformed fibroblast line. The results show that metastatic variants of 3 murine tumor models consisting of lymphomas, mastocytomas and sarcomas are characterized by qualitative and quantitative alterations in the profiles of sugar-binding proteins.

摘要

相似文献

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引用本文的文献

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Inhibition of liver tumor cell colonization in two animal tumor models by lectin blocking with D-galactose or arabinogalactan.
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2
Clinical application of various plant and endogenous lectins to leukemia.
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3
Malignant and normally developing trophoblastic cells of human placenta display different characteristics defined by histochemical and biochemical mapping of endogenous lectins.
Histochemistry. 1989;92(4):283-9. doi: 10.1007/BF00500542.
4
Lineage- and differentiation-dependent alterations in the expression of receptors for glycoconjugates (lectins) in different human hematopoietic cell lines and low grade lymphomas.
不同人类造血细胞系和低度淋巴瘤中糖缀合物(凝集素)受体表达的谱系和分化依赖性改变。
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5
Membrane N-acetylglucosamine: expression by cells in rheumatoid synovial fluid, and by pre-cultured monocytes.膜N-乙酰葡糖胺:在类风湿性滑液细胞及预培养单核细胞中的表达
Br J Exp Pathol. 1989 Oct;70(5):567-77.
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Endogenous sugar receptor pattern in human glioblastomas and gangliocytomas studied by histochemical application of biotinylated (neo)glycoproteins and affinity chromatography.通过生物素化(新)糖蛋白的组织化学应用和亲和层析研究人类胶质母细胞瘤和神经节细胞瘤中的内源性糖受体模式。
Histochemistry. 1989;91(1):5-11. doi: 10.1007/BF00501903.
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