ISDA: 2N7F

Deposition Date 2015-09-09

Release Date 2016-04-06

Last Version Date 2024-10-30

Entry Detail

PDB ID:

2N7F

Keywords:

TOXIN

Title:

NMR solution structure of muO-conotoxin MfVIA

Biological Source:

Source Organism(s):

synthetic construct (Taxon ID: 32630)

Method Details:

Experimental Method:

SOLUTION NMR

Conformers Calculated:

Conformers Submitted:

Selection Criteria:

structures with the lowest energy

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Macromolecular Entities

Structures with similar UniProt ID

Protein Blast

Polymer Type:polypeptide(L)
Molecule:muO-conotoxin MfVIA
Chain IDs:A
Chain Length:32
Number of Molecules:1
Biological Source:synthetic construct

UniProt ID:P0DM15

Ligand Molecules

Primary Citation

Development of a mu O-Conotoxin Analogue with Improved Lipid Membrane Interactions and Potency for the Analgesic Sodium Channel NaV1.8.

Deuis, J.R, Dekan, Z, Inserra, M.C, Lee, T.H, Aguilar, M.I, Craik, D.J, Lewis, R.J, Alewood, P.F, Mobli, M, Schroeder, C.I, Henriques, S.T, Vetter, I.Show

J. Biol. Chem. 291 11829 11842 (2016)

PMID: 27026701 DOI: 10.1074/jbc.M116.721662

Abstact

The μO-conotoxins MrVIA, MrVIB, and MfVIA inhibit the voltage-gated sodium channel NaV1.8, a well described target for the treatment of pain; however, little is known about the residues or structural elements that define this activity. In this study, we determined the three-dimensional structure of MfVIA, examined its membrane binding properties, performed alanine-scanning mutagenesis, and identified residues important for its activity at human NaV1.8. A second round of mutations resulted in (E5K,E8K)MfVIA, a double mutant with greater positive surface charge and greater affinity for lipid membranes compared with MfVIA. This analogue had increased potency at NaV1.8 and was analgesic in the mouse formalin assay.

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Primary Citation of related structures

Abstact

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