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D-Maurocalcine, a pharmacologically inert efficient cell-penetrating peptide analogue.


ABSTRACT: Maurocalcine has been the first demonstrated animal toxin acting as a cell-penetrating peptide. Although it possesses competitive advantages, its use as a cell-penetrating peptide (CPP) requires that analogues be developed that lack its characteristic pharmacological activity on ryanodine-sensitive calcium channels without affecting its cell-penetrating and vector efficiencies. Here, we present the synthesis, three-dimensional (1)H NMR structure, and activity of D-maurocalcine. We demonstrate that it possesses all of the desired features for an excellent CPP: preserved structure, lack of pharmacological action, conserved vector properties, and absence of cell toxicity. This is the first report of a folded/oxidized animal toxin in its D-diastereomer conformation for use as a CPP. The protease resistance of this new peptide analogue, combined with its efficient cell penetration at concentrations devoid of cell toxicity, suggests that D-maurocalcine should be an excellent vector for in vivo applications.

SUBMITTER: Poillot C 

PROVIDER: S-EPMC2962515 | biostudies-literature | 2010 Oct

REPOSITORIES: biostudies-literature

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D-Maurocalcine, a pharmacologically inert efficient cell-penetrating peptide analogue.

Poillot Cathy C   Dridi Kaouthar K   Bichraoui Hicham H   Pêcher Julien J   Alphonse Sebastien S   Douzi Badreddine B   Ronjat Michel M   Darbon Hervé H   De Waard Michel M  

The Journal of biological chemistry 20100707 44


Maurocalcine has been the first demonstrated animal toxin acting as a cell-penetrating peptide. Although it possesses competitive advantages, its use as a cell-penetrating peptide (CPP) requires that analogues be developed that lack its characteristic pharmacological activity on ryanodine-sensitive calcium channels without affecting its cell-penetrating and vector efficiencies. Here, we present the synthesis, three-dimensional (1)H NMR structure, and activity of D-maurocalcine. We demonstrate th  ...[more]

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2018-11-07 | GSE122241 | GEO