1SN1
STRUCTURE OF SCORPION NEUROTOXIN BMK M1
Summary for 1SN1
Entry DOI | 10.2210/pdb1sn1/pdb |
Related | 1SN4 |
Descriptor | PROTEIN (NEUROTOXIN BMK M1) (2 entities in total) |
Functional Keywords | neurotoxin, sodium channel inhibitor, scorpion, toxin |
Biological source | Mesobuthus martensii (Chinese scorpion) |
Cellular location | Secreted: P45697 |
Total number of polymer chains | 1 |
Total formula weight | 7235.27 |
Authors | He, X.L.,Li, H.M.,Liu, X.Q.,Zeng, Z.H.,Wang, D.C. (deposition date: 1998-11-12, release date: 1999-11-17, Last modification date: 2024-11-13) |
Primary citation | He, X.L.,Li, H.M.,Zeng, Z.H.,Liu, X.Q.,Wang, M.,Wang, D.C. Crystal structures of two alpha-like scorpion toxins: non-proline cis peptide bonds and implications for new binding site selectivity on the sodium channel. J.Mol.Biol., 292:125-135, 1999 Cited by PubMed Abstract: The crystal structures of two group III alpha-like toxins from the scorpion Buthus martensii Karsch, BmK M1 and BmK M4, were determined at 1.7 A and 1.3 A resolution and refined to R factors of 0.169 and 0.166, respectively. The first high-resolution structures of the alpha-like scorpion toxin show some striking features compared with structures of the "classical" alpha-toxin. Firstly, a non-proline cis peptide bond between residues 9 and 10 unusually occurs in the five-member reverse turn 8-12. Secondly, the cis peptide 9-10 mediates the spatial relationship between the turn 8-12 and the C-terminal stretch 58-64 through a pair of main-chain hydrogen bonds between residues 10 and 64 to form a unique tertiary arrangement which features the special orientation of the terminal residues 62-64. Finally, in consequence of the peculiar orientation of the C-terminal residues, the functional groups of Arg58, which are crucial for the toxin-receptor interaction, are exposed and accessible in BmK M1 and M4 rather than buried as in the classical alpha-toxins. Sequence alignment and characteristics analysis suggested that the above structural features observed in BmK M1 and M4 occur in all group III alpha-like toxins. Recently, some group III alpha-like toxins were demonstrated to occupy a receptor site different from the classical alpha-toxin. Therefore, the distinct structural features of BmK M1 and M4 presented here may provide the structural basis for the newly recognized toxin-receptor binding site selectivity. Besides, the non-proline cis peptide bonds found in these two structures play a role in the formation of the structural characteristics and in keeping accurate positions of the functionally crucial residues. This manifested a way to achieve high levels of molecular specificity and atomic precision through the strained backbone geometry. PubMed: 10493862DOI: 10.1006/jmbi.1999.3036 PDB entries with the same primary citation |
Experimental method | X-RAY DIFFRACTION (1.7 Å) |
Structure validation
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