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神经钙黏蛋白胞外结构域二的稳定性研究

Stability studies of extracellular domain two of neural-cadherin.

作者信息

Vunnam Nagamani, McCool John K, Williamson Michael, Pedigo Susan

机构信息

Department of Chemistry and Biochemistry, University of Mississippi, MS, USA.

出版信息

Biochim Biophys Acta. 2011 Dec;1814(12):1841-5. doi: 10.1016/j.bbapap.2011.08.002. Epub 2011 Aug 6.

DOI:10.1016/j.bbapap.2011.08.002
PMID:21843662
Abstract

Neural- (NCAD) and epithelial- (ECAD) cadherin are calcium-dependent cell-adhesive molecules, and are localized at excitatory and inhibitory synapses respectively. They play an important role in synaptogenesis, synapse maintenance and plasticity. The extracellular region plays a critical role in cadherin-mediated cell adhesion, and has five tandemly repeated ectodomains (EC1-EC5). Calcium binding is required for dimer formation between first two N-terminal domains (EC1-EC2). Despite similarity in the primary structure, the extracellular domains of NCAD and ECAD have different intrinsic stability, dimerization affinity and kinetics of disassembly. To investigate the origin of these differences, we are characterizing the modular domains individually. Here, we report studies of NCAD2, EC2 of NCAD. This domain is important for calcium binding and is the physical linkage between the dimerization interface in EC1 and the membrane proximal modular domains. Thermal-denaturation studies show that NCAD2 is less stable than ECAD2 and less influenced by the adjoining 7-residue, N- and C-terminal linker segments. In addition the NCAD2 constructs are less influenced by added salt. This difference is likely due to variation in the overall number and distribution of charges on these anionic proteins. Our studies indicate that despite their sequence similarity and apparently passive role in adhesive dimer formation, EC2 of E- and N-cadherins are distinctly different and may contribute to the differences in energetics and kinetics of dimerization.

摘要

神经钙黏蛋白(NCAD)和上皮钙黏蛋白(ECAD)是钙依赖性细胞黏附分子,分别定位于兴奋性和抑制性突触。它们在突触形成、突触维持和可塑性中发挥重要作用。细胞外区域在钙黏蛋白介导的细胞黏附中起关键作用,有五个串联重复的胞外结构域(EC1-EC5)。前两个N端结构域(EC1-EC2)之间形成二聚体需要钙结合。尽管一级结构相似,但NCAD和ECAD的细胞外结构域具有不同的内在稳定性、二聚化亲和力和解离动力学。为了研究这些差异的起源,我们正在分别对模块化结构域进行表征。在此,我们报告对NCAD的EC2即NCAD2的研究。该结构域对钙结合很重要,是EC1中二聚化界面与膜近端模块化结构域之间的物理连接。热变性研究表明,NCAD2比ECAD2更不稳定,且受相邻的7个残基的N端和C端连接片段影响较小。此外,NCAD2构建体受添加盐的影响较小。这种差异可能是由于这些阴离子蛋白上电荷的总数和分布不同。我们的研究表明,尽管E-钙黏蛋白和N-钙黏蛋白的EC2在序列上相似且在黏附二聚体形成中显然起被动作用,但它们明显不同,可能导致二聚化能量学和动力学的差异。

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