Computational modeling of laminin N-terminal domains using sparse distance constraints from disulfide bonds and chemical cross-linking.

Kalkhof S; Haehn S; Paulsson M; Smyth N; Meiler J; Sinz A

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Computational modeling of laminin N-terminal domains using sparse distance constraints from disulfide bonds and chemical cross-linking.

机译：使用来自二硫键的稀疏距离约束和化学交联计算层粘连蛋白N末端结构域的计算模型。

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Basement membranes are thin extracellular protein layers, which separate endothelial and epithelial cells from the underlying connecting tissue. The main noncollagenous components of basement membranes are laminins, trimeric glycoproteins, which form polymeric networks by interactions of their N-terminal (LN) domains; however, no high-resolution structure of laminin LN domains exists so far. To construct models for laminin beta(1) and gamma(1) LN domains, 14 potentially suited template structures were determined using fold recognition methods. For each target/template-combination comparative models were created with Rosetta. Final models were selected based on their agreement with experimentally obtained distance constraints from natural cross-links, that is, disulfide bonds as well as chemical cross-links obtained from reactions with two amine-reactive cross-linkers. We predict that laminin beta(1) and gamma(1) LN domains share the galactose-binding domain-like fold.

机译：基底膜是薄的细胞外蛋白层，其将内皮细胞和上皮细胞与下面的连接组织分开。基底膜的主要非胶原成分是层粘连蛋白，三聚体糖蛋白，它们通过其N端（LN）域相互作用形成聚合物网络。但是，到目前为止，尚不存在层粘连蛋白LN域的高分辨率结构。要构建层粘连蛋白β（1）和γ（1）LN域的模型，使用折叠识别方法确定了14种可能合适的模板结构。对于每个目标/模板组合，使用Rosetta创建比较模型。根据最终模型与实验获得的与天然交联剂的距离限制（即二硫键以及从与两个胺反应性交联剂的反应中获得的化学交联剂）的一致性选择最终模型。我们预测层粘连蛋白β（1）和γ（1）LN域共享半乳糖结合域样的折叠。

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《Proteins: Structure, Function, and Genetics》 |2010年第16期|共19页
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Kalkhof S; Haehn S; Paulsson M; Smyth N; Meiler J; Sinz A;
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中图分类生物化学;
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入库时间 2022-08-18 17:05:02

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1. Computational modeling of laminin N-terminal domains using sparse distance constraints from disulfide bonds and chemical cross-linking. [J] . Kalkhof S, Haehn S, Paulsson M, Proteins: Structure, Function, and Genetics . 2010,第16期

机译：使用来自二硫键的稀疏距离约束和化学交联计算层粘连蛋白N末端结构域的计算模型。
2. Protein-protein interactions within paramyxoviruses identified by native disulfide bonding or reversible chemical cross-linking. [J] . M A Markwell, C F Fox Journal of Virology . 1980,第1期

机译：通过天然二硫键或可逆化学交联鉴定的副缺斑内的蛋白质 - 蛋白质相互作用。
3. Protein-protein interactions within paramyxoviruses identified by native disulfide bonding or reversible chemical cross-linking. [J] . M A Markwell, C F Fox Journal of Virology . 1980,第1期

机译：通过天然二硫键或可逆化学交联鉴定的副缺斑内的蛋白质 - 蛋白质相互作用。
4. DISULFIDE BONDING PATTERNS OF LAMININ BETA 1 AND GAMMA 1 N TERMINAL CONSTRUCTS ANALYZED BY ESI-LTQ-ORBITRAP-MS [C] . Christian Ihling, Konstanze Witte, Manuel Keller, European Fourier Transform Mass Spectrometry Workshop . 2010

机译：通过ESI-LTQ-orbitrap-MS分析的层粘连蛋白β1和γ1N末端构建体的二硫键图案
5. Redox dependent disulfide bonding of Von Willebrand factor A1A2A2 domains [D] . Seyran, Esra 2011

机译：Von Willebrand因子A1A2A2域的氧化还原依赖性二硫键
6. Computational Modeling of Laminin N-Terminal Domains Using Sparse Distance Constraints from Disulfide Bonds and Chemical Cross-Linking [O] . Stefan Kalkhof, Sebastian Haehn, Mats Paulsson, -1

机译：二硫键和化学交联的稀疏距离约束的层粘连蛋白N-末端域的计算建模
7. Disulfide bond formation of heterodimer and heterotrimer of human laminin-332 coiled-coil domains [O] . 2015

机译：人层膜-332卷绕线圈域的异二聚体二硫键形成和杂偶联器

Computational modeling of laminin N-terminal domains using sparse distance constraints from disulfide bonds and chemical cross-linking.

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