Falkenstein_2004_J.Pept.Sci_10_342

Reference

Title : Synthesis and characterization of a chimeric peptide derived from fasciculin that inhibits acetylcholinesterase - Falkenstein_2004_J.Pept.Sci_10_342
Author(s) : Falkenstein RJ , Gornalusse GG , Pena C
Ref : J Pept Sci , 10 :342 , 2004
Abstract :

Fasciculins are peptides isolated from mamba (Dendroaspis) venoms which exert their toxic action by inhibiting acetylcholinesterase (AChE). They contain a characteristic triple stranded antiparallel beta-sheet formed by residues 22-27, 34-39 and 48-53. A chimeric peptide named Fas-C, encompassing most of these sequences was synthesized using SPPS/Boc-chemistry and characterized chemically, structurally and functionally. Fas-C has two disulfide bridges, formed sequentially using dual cysteine protection. SDS-PAGE patterns, HPLC profiles and MS proved the peptide identity. Circular dichroism indicated the presence of 13.6% and 41.6% of beta-sheet and beta-turn, respectively, comparable to values observed in the native toxin. An inhibitory effect on eel AChE was displayed by the peptide (Ki71.6 +/- 18.3 microM), although not reaching the affinity level of the parent native toxin (Ki 0.3 nM). It is confirmed that the principal binding region of fasciculin to AChE resides within loop II.

PubMedSearch : Falkenstein_2004_J.Pept.Sci_10_342
PubMedID: 15214439

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Citations formats

Falkenstein RJ, Gornalusse GG, Pena C (2004)
Synthesis and characterization of a chimeric peptide derived from fasciculin that inhibits acetylcholinesterase
J Pept Sci 10 :342

Falkenstein RJ, Gornalusse GG, Pena C (2004)
J Pept Sci 10 :342