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NCAM polysialic acid can regulate both cell-cell and cell-substrate interactions

机译:NCAM聚唾液酸可以调节细胞-细胞和细胞-底物的相互作用

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摘要

We have proposed previously that the polysialic acid (PSA) moiety of NCAM can influence membrane-membrane apposition, and thereby serve as a selective regulator of a variety of contact-dependent cell interactions. In this study, cell and tissue culture models are used to obtain direct evidence that the presence of PSA on the surface membrane can affect both cell-cell and cell-substrate interactions. Using a neuroblastoma/sensory neuron cell hybrid, it was found that removal of PSA with a specific neuraminidase (endo-N) augments cell-cell aggregation mediated by the L1 cell adhesion molecule as well as cell attachment to a variety of tissue culture substrates. In studies of embryonic spinal cord axon bundling, which involves both cell-cell and cell-substrate interactions, the pronounced defasciculation produced by removal of PSA is most easily explained by an increase in cell- substrate interaction. The fact that in both studies NCAM's intrinsic adhesion function was found not to be an important variable further illustrates that regulation of the cell surface by PSA can extend beyond binding mediated by the NCAM polypeptide.
机译:先前我们已经提出NCAM的聚唾液酸(PSA)部分可以影响膜-膜的并置,从而充当各种接触依赖性细胞相互作用的选择性调节剂。在这项研究中,细胞和组织培养模型用于获得直接证据,表明表面膜上PSA的存在会影响细胞与细胞以及细胞与基质之间的相互作用。使用神经母细胞瘤/感觉神经元细胞杂合体,发现用特定的神经氨酸酶(endo-N)去除PSA可增强由L1细胞粘附分子介导的细胞-细胞聚集以及细胞对多种组织培养底物的附着。在涉及细胞-细胞和细胞-底物相互作用的胚胎脊髓轴突捆绑研究中,最容易通过细胞-底物相互作用的增加来解释由于去除PSA而产生的明显的去纤维化。在两项研究中均发现NCAM的固有粘附功能不是重要变量,这一事实进一步说明了PSA对细胞表面的调节作用可能会超出NCAM多肽介导的结合作用。

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