Toward a better understanding of the interaction between TGF-β family members and their ALK receptors

被引:10
作者
Romano, Valentina [2 ]
Raimondo, Domenico [3 ]
Calvanese, Luisa [2 ]
D'Auria, Gabriella [1 ,2 ]
Tramontano, Anna [3 ]
Falcigno, Lucia [1 ,2 ]
机构
[1] CNR, Inst Biostruct & Bioimaging, I-80134 Naples, Italy
[2] Univ Naples Federico II, Dept Chem Sci, I-80126 Naples, Italy
[3] Univ Roma La Sapienza, Dept Phys, I-00185 Rome, Italy
关键词
Comparative modeling; TGF-beta protein; ALK receptor; Protein-protein docking; GROWTH-FACTOR-BETA; PROTEIN-LIGAND INTERACTIONS; VERTEBRATE DEVELOPMENT; STRUCTURE PREDICTION; SIGNAL-TRANSDUCTION; HOMOLOGY DETECTION; CRYSTAL-STRUCTURE; SCORING FUNCTION; BINDING; CANCER;
D O I
10.1007/s00894-012-1370-y
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Transforming growth factor-beta (TGF-beta) proteins are a family of structurally related extracellular proteins that trigger their signaling functions through interaction with the extracellular domains of their cognate serine/threonine kinase receptors. The specificity of TGF-beta/receptor binding is complex and gives rise to multiple functional roles. Additionally, it is not completely understood at the atomic level. Here, we use the most reliable computational methods currently available to study systems involving activin-like kinase (ALK) receptors ALK4 and ALK7 and their multiple TGF-beta ligands. We built models for all these proteins and their complexes for which experimental structures are not available. By analyzing the surfaces of interaction in six different TGF-beta/ALK complexes we could infer which are the structural distinctive features of the ligand-receptor binding mode. Furthermore, this study allowed us to rationalize why binding of the growth factors GDF3 and Nodal to the ALK4 receptor requires the Cripto co-factor, whilst binding to the ALK7 receptor does not.
引用
收藏
页码:3617 / 3625
页数:9
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