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神经细胞黏附分子和髓磷脂相关糖蛋白共享一个被单克隆抗体L2和HNK-1识别的共同碳水化合物部分。

Neural cell adhesion molecules and myelin-associated glycoprotein share a common carbohydrate moiety recognized by monoclonal antibodies L2 and HNK-1.

作者信息

Kruse J, Mailhammer R, Wernecke H, Faissner A, Sommer I, Goridis C, Schachner M

出版信息

Nature. 1984;311(5982):153-5. doi: 10.1038/311153a0.

Abstract

Cell surface molecules have been implicated in cell interactions which underlie formation of the nervous system. The analysis of the functional properties of such molecules has profited from the combined use of antibodies and cell culture systems. It has been suggested that the interplay between these molecules modulates cell-to-cell interaction at critical developmental stages. In the mouse, N-CAM and L1 antigen have been shown to mediate Ca2+-independent adhesion among neural cells. N-CAM plays a role in fasciculation of neurites and formation of neuromuscular junction. L1 is apparently not involved in synaptogenesis, but in migration of granule cell neurones in the developing mouse cerebellar cortex. The two antigens are distinct molecular and functional entities which act synergistically in aggregation of neuroblastoma and early postnatal cerebellar cells. In view of a certain similarity in function between the two groups of molecules, it was not surprising to find that structural similarities are detectable by the monoclonal antibody L2. We show here that a carbohydrate moiety recognized by L2 and HNK-1 monoclonal antibodies, is present in mouse N-CAM and L1. The L2 epitope appears on all major neural cell types but not all N-CAM molecules express it. This heterogeneity points to a previously undetected molecular diversity which may have functional implications for modulating cell adhesion during development.

摘要

细胞表面分子参与了构成神经系统基础的细胞间相互作用。对这类分子功能特性的分析受益于抗体与细胞培养系统的联合应用。有人提出,这些分子之间的相互作用在关键发育阶段调节细胞间相互作用。在小鼠中,已证明N-CAM和L1抗原介导神经细胞间不依赖Ca2+的黏附。N-CAM在神经突束化和神经肌肉接头形成中起作用。L1显然不参与突触形成,但参与发育中小鼠小脑皮质颗粒细胞神经元的迁移。这两种抗原是不同的分子和功能实体,在神经母细胞瘤和出生后早期小脑细胞聚集中协同起作用。鉴于这两组分子在功能上有一定相似性,发现单克隆抗体L2能检测到结构相似性也就不足为奇了。我们在此表明,L2和HNK-1单克隆抗体识别的碳水化合物部分存在于小鼠N-CAM和L1中。L2表位出现在所有主要神经细胞类型上,但并非所有N-CAM分子都表达它。这种异质性表明存在以前未检测到的分子多样性,这可能对发育过程中调节细胞黏附有功能影响。

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