2009
DOI: 10.1002/cmdc.200800292
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Structurally Minimized μ‐Conotoxin Analogues as Sodium Channel Blockers: Implications for Designing Conopeptide‐Based Therapeutics

Abstract: Disulfide bridges, which stabilize the native conformation of conotoxins impose a challenge in the synthesis of smaller analogs. In this work, we describe the synthesis of a minimized analog of the analgesic μ-conotoxin KIIIA that blocks two sodium channel subtypes, the neuronal NaV1.2 and skeletal muscle NaV1.4. Three disulfide-deficient analogs of KIIIA were initially synthesized in which the native disulfide bridge formed between either C1-C9, C2-C15 or C4-C16 was removed. Deletion of the first bridge only … Show more

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Cited by 51 publications
(84 citation statements)
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“…However, removal of only one of the three disulfide linkages yielded a lower k on the C2-C15 linkage (Han et al, 2009;Khoo et al, 2009). This decrease in k on fits with the KIIIA-wt pH results, the concomitant 10-fold increase in k off , together with the rapid reversibility of our observed pH effects, makes disulfide bond disruption an unlikely rationale for our observations.…”
Section: Discussionmentioning
confidence: 99%
“…However, removal of only one of the three disulfide linkages yielded a lower k on the C2-C15 linkage (Han et al, 2009;Khoo et al, 2009). This decrease in k on fits with the KIIIA-wt pH results, the concomitant 10-fold increase in k off , together with the rapid reversibility of our observed pH effects, makes disulfide bond disruption an unlikely rationale for our observations.…”
Section: Discussionmentioning
confidence: 99%
“…They illustrated that the first disulfide bridge between Cys 1 and Cys 9 in KIIIA is removable, almost without affecting the original activity of the peptide on Na v 1.2 and Na v 1.4 (34). Ultimately, the first disulfide bridge was excluded in our chimeric peptide.…”
Section: Design Strategymentioning
confidence: 91%
“…We integrated recent results by Han et al (34) into our design strategy. They illustrated that the first disulfide bridge between Cys 1 and Cys 9 in KIIIA is removable, almost without affecting the original activity of the peptide on Na v 1.2 and Na v 1.4 (34).…”
Section: Design Strategymentioning
confidence: 99%
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“…From a manufacturing perspective, exploring the removal of disulfide bonds to reduce the complexity of the peptide can be initiated early in a molecule's lifetime using standard biophysical techniques, such as nuclear magnetic resonance in combination with a functional assay, to evaluate the impact of these changes. The utility of disulfide bond deletion was demonstrated with μ-conotoxin KIIIA, a disulfide-rich venom peptide isolated from Conus kinoshitai that blocks mammalian neuronal voltage-gated sodium channels and is a potent analgesic (43). The authors systematically removed cysteine pairs, by making simple cysteine to alanine mutations, and screened for functional activity by testing the disulfide-deficient analogues against mammalian Na v 1.2 and Na v 1.4.…”
Section: Improving Chemical and Physical Stabilitymentioning
confidence: 99%