1Z6C
Solution structure of an EGF pair (EGF34) from vitamin K-dependent protein S
Summary for 1Z6C
| Entry DOI | 10.2210/pdb1z6c/pdb |
| Descriptor | Vitamin K-dependent protein S, CALCIUM ION (3 entities in total) |
| Functional Keywords | egf module, blood clotting |
| Biological source | Homo sapiens (human) |
| Cellular location | Secreted: P07225 |
| Total number of polymer chains | 1 |
| Total formula weight | 9677.00 |
| Authors | Drakenberg, T.,Ghasriani, H.,Thulin, E.,Thamlitz, A.M.,Muranyi, A.,Annila, A.,Stenflo, J. (deposition date: 2005-03-22, release date: 2005-06-21, Last modification date: 2024-10-16) |
| Primary citation | Drakenberg, T.,Ghasriani, H.,Thulin, E.,Muranyi, A.,Annila, A.,Stenflo, J. Solution Structure of the Ca(2+)-Binding EGF3-4 Pair from Vitamin K-Dependent Protein S: Identification of an Unusual Fold in EGF3. Biochemistry, 44:8782-8789, 2005 Cited by PubMed Abstract: Vitamin K-dependent protein S is a cofactor of activated protein C, a serine protease that regulates blood coagulation. Deficiency of protein S can cause venous thrombosis. Protein S has four EGF domains in tandem; domains 2-4 bind calcium with high affinity whereas domains 1-2 mediate interaction with activated protein C. We have now solved the solution structure of the EGF3-4 fragment of protein S. The linker between the two domains is similar to what has been observed in other calcium-binding EGF domains where it provides an extended conformation. Interestingly, a disagreement between NOE and RDC data revealed a conformational heterogeneity within EGF3 due to a hinge-like motion around Glu186 in the Cys-Glu-Cys sequence, the only point in the domain where flexibility is allowed. The dominant, bent conformation of EGF3 in the pair has no precedent among calcium-binding EGF domains. It is characterized by a change in the psi angle of Glu186 from 160 degrees +/- 40 degrees , as seen in ten other EGF domains, to approximately 0 degrees +/- 15 degrees . NOESY data suggest that Tyr193, a residue not conserved in other calcium-binding EGF domains (except in the homologue Gas6), induces the unique fold of EGF3. However, SAXS data, obtained on EGF1-4 and EGF2-4, showed a dominant, extended conformation in these fragments. This may be due to a counterproductive domain-domain interaction between EGF2 and EGF4 if EGF3 is in a bent conformation. We speculate that the ability of EGF3 to adopt different conformations may be of functional significance in protein-protein interactions involving protein S. PubMed: 15952784DOI: 10.1021/bi050101f PDB entries with the same primary citation |
| Experimental method | SOLUTION NMR |
Structure validation
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