肿瘤细胞黏附性和细胞表面唾液酸化的改变会严重改变转移潜能。
Metastatic potential severely altered by changes in tumor cell adhesiveness and cell-surface sialylation.
作者信息
Fogel M, Altevogt P, Schirrmacher V
出版信息
J Exp Med. 1983 Jan 1;157(1):371-6. doi: 10.1084/jem.157.1.371.
Abstract
A plastic adherent variant line (ESb-M) of a highly invasive and metastatic murine T cell lymphoma (ESb) was found to have lost its metastatic potential while still being tumorigenic in normal syngeneic hosts. The variant retained most of its ESb-derived antigenic and biochemical characteristics but differed at binding sites for certain lectins with specificity for terminal N-acetylgalactosamine residues. Whereas such sites were masked by sialic acid on metastatic ESb cells, they became unmasked on the adherent variant line. Metastatic revertants of ESb-M cells did not express the respective lectin receptor sites because these were again masked by sialic acid. It is suggested that the masking of specific lectin receptors sites on the tumor cell surface is of crucial importance for metastatis. If freely exposed, these sites may change adherence characteristics of the cells possibly not only in vitro (to plastic) but also in vivo.
摘要
在正常同基因宿主中,一种高度侵袭性和转移性的小鼠T细胞淋巴瘤(ESb)的塑料贴壁变异株系(ESb-M)虽仍具有致瘤性,但已失去转移潜能。该变异株保留了其大部分源自ESb的抗原和生化特性,但在某些对末端N-乙酰半乳糖胺残基具有特异性的凝集素结合位点上有所不同。在转移性ESb细胞上,此类位点被唾液酸掩盖,而在贴壁变异株系上则未被掩盖。ESb-M细胞的转移性回复株不表达相应的凝集素受体位点,因为这些位点再次被唾液酸掩盖。有人提出,肿瘤细胞表面特定凝集素受体位点的掩盖对于转移至关重要。如果这些位点自由暴露,可能不仅会在体外(对塑料)而且会在体内改变细胞的黏附特性。
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