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细胞表面唾液酸化与肿瘤转移。B16黑色素瘤变体的转移潜能与其特定倒数第二个寡糖结构的相对数量相关。

Cell surface sialylation and tumor metastasis. Metastatic potential of B16 melanoma variants correlates with their relative numbers of specific penultimate oligosaccharide structures.

作者信息

Passaniti A, Hart G W

机构信息

Department of Biological Chemistry, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205.

出版信息

J Biol Chem. 1988 Jun 5;263(16):7591-603.

PMID:3372501
Abstract

Numerous investigations suggest that cell surface glycoconjugates, and in particular sialic acids, are directly involved in determining the metastatic phenotype. To further evaluate this hypothesis, we have used a variety of techniques to probe the cell surfaces of several metastatic variants of the murine B16 melanoma that were selected for experimental lung-colonizing ability (Fidler, I. (1973) Nature 242, 148-149) or for their ability to spontaneously metastasize from the site of a subcutaneous injection (Stackpole, C. W., Alterman, A. L., and Fornabaio, D. M. (1985) Invasion & Metastasis 5, 125-142). Using a highly sensitive high performance liquid chromatography sialic acid assay in conjunction with Vibrio cholerae sialidase, we find that none of these metastatic variants differ significantly in their overall levels of cell surface sialic acid. Using highly purified, linkage-specific sialyltransferases, in conjunction with specific glycosidases, to probe the cell surface saccharide topography of specific penultimate oligosaccharides, we also find no significant differences between the efficient lung-colonizing variant, B16-F10 and the poorly-colonizing B16-F1 or B16-Flr variants. In contrast, the spontaneously metastatic variants examined contain substantially different levels of specific penultimate sialylation sites. The tumorigenic but nonmetastatic B16-LM3/G3.26 variant contains 4-fold more penultimate Gal beta 1-3GalNAc sialylation sites than the tumorigenic and highly metastatic B16-LM3/G3.12 variant when CMP[3H]NeuAc and the alpha 2-3Gal beta 1-3GalNAc sialyltransferase are used to probe the melanoma cell surfaces. Several prominent glycoconjugates of apparent Mr 43,000, 40,000, and 30,000 are especially evident upon sodium dodecyl sulfate-polyacrylamide gel electrophoresis of the nonmetastatic cells. The nonmetastatic variant also contains 2-fold more Gal beta 1-4GlcNAc sialylation sites than the metastatic variant when the alpha 2-6Gal beta 1-4GlcNAc sialyltransferase is used as a cell surface probe. In this case, glycoconjugates of apparent Mr 74,000, 45,000, and 43,000 are more prominently observed on the cell surfaces of the nonmetastatic variant. These data indicate that the differences in lung-colonizing abilities of B16 melanoma metastatic variants do not correlate with the numbers or sialylation states of specific penultimate oligosaccharide structures on their surfaces. However, the relative levels of specific penultimate saccharide structures do correlate with the ability of the cells to undergo spontaneous metastasis from a subcutaneous tumor.

摘要

大量研究表明,细胞表面糖缀合物,尤其是唾液酸,直接参与了转移表型的决定。为了进一步评估这一假说,我们使用了多种技术来探测小鼠B16黑色素瘤的几种转移变体的细胞表面,这些变体是根据实验性肺定植能力(菲德勒,I.(1973年)《自然》242卷,第148 - 149页)或从皮下注射部位自发转移的能力(斯塔克波尔,C.W.,阿尔特曼,A.L.,和福尔纳巴约,D.M.(1985年)《侵袭与转移》5卷,第125 - 142页)选择的。结合霍乱弧菌唾液酸酶,使用高灵敏度的高效液相色谱唾液酸测定法,我们发现这些转移变体在细胞表面唾液酸的总体水平上没有显著差异。使用高度纯化的、连接特异性唾液酸转移酶,结合特定糖苷酶,来探测特定倒数第二个寡糖的细胞表面糖拓扑结构,我们还发现高效肺定植变体B16 - F10与定植能力差的B16 - F1或B16 - Flr变体之间没有显著差异。相比之下,所检测的自发转移变体含有显著不同水平的特定倒数第二个唾液酸化位点。当使用CMP[³H]NeuAc和α2 - 3Galβ1 - 3GalNAc唾液酸转移酶探测黑色素瘤细胞表面时,致瘤但不转移的B16 - LM3/G3.26变体比致瘤且高转移的B16 - LM3/G3.12变体含有多4倍的倒数第二个Galβ1 - 3GalNAc唾液酸化位点。在非转移细胞的十二烷基硫酸钠 - 聚丙烯酰胺凝胶电泳中,几种表观分子量为43,000、40,000和30,000的突出糖缀合物特别明显。当使用α2 - 6Galβ1 - 4GlcNAc唾液酸转移酶作为细胞表面探针时,非转移变体也比转移变体含有多2倍的Galβ1 - 4GlcNAc唾液酸化位点。在这种情况下,表观分子量为74,000、45,000和43,000的糖缀合物在非转移变体的细胞表面更显著地观察到。这些数据表明,B16黑色素瘤转移变体的肺定植能力差异与其表面特定倒数第二个寡糖结构的数量或唾液酸化状态无关。然而,特定倒数第二个糖结构的相对水平确实与细胞从皮下肿瘤自发转移的能力相关。

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