首页> 外文期刊>Journal of cell biology >Developmental alterations in molecular weights of proteins in the human central nervous system that react with antibodies against myelin-associated glycoprotein.
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Developmental alterations in molecular weights of proteins in the human central nervous system that react with antibodies against myelin-associated glycoprotein.

机译:人中枢神经系统中与抗髓磷脂相关糖蛋白抗体反应的蛋白质分子量的发育变化。

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By the use of a rat IgG monoclonal antibody (mab), a mouse mab and human serum containing an IgM mab, all of which react with isolated human myelin-associated glycoprotein (MAG) on immunoblots and bind only to proteins with relative mobilities identical to MAG and dMAG on immunoblots of homogenates of adult human spinal cord, we demonstrated the following: in homogenates of central nervous system tissue from human fetuses of gestational ages that antedate myelination, the anti-MAG antibodies react only with proteins with molecular weights of 250,000 or larger. During myelination the molecular weights of proteins with which the anti-MAG antibodies react shift towards the lower molecular weights found in adult myelin. Amongst those central nervous system regions examined, the shift towards the low molecular weights occurred earliest in the region that is first to become myelinated and latest in the one that is the last to myelinate. Once myelination is completed, the antibodies react only with proteins with relative mobilities identical to those of MAG and dMAG. These developmental changes in molecular weights of "MAG-related proteins" may prove useful as an index of chemical processes on the basis of which myelination occurs.
机译:通过使用大鼠IgG单克隆抗体(mab),小鼠mab和包含IgM mab的人血清,所有这些抗体均与免疫印迹上的分离的人髓磷脂相关糖蛋白(MAG)反应,并且仅结合相对迁移率与MAG和dMAG对成人脊髓匀浆的免疫印迹的作用,我们证明了以下内容:在早于髓鞘形成的胎龄胎儿的中枢神经系统组织匀浆中,抗MAG抗体仅与分子量为250,000或更大。在髓鞘形成过程中,抗MAG抗体与之反应的蛋白质的分子量向成年髓磷脂中发现的较低分子量转移。在所检查的那些中枢神经系统区域中,向低分子量的转变最早发生在最早出现髓鞘的区域,最晚出现在最后发生髓鞘的区域。一旦髓鞘化完成,抗体仅与相对迁移率与MAG和dMAG相同的蛋白质反应。这些“ MAG相关蛋白”分子量的发展变化可以证明是有用的,作为发生髓鞘化的化学过程的指标。

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