Development of ProTx-II Analogues as Highly Selective Peptide Blockers of Na v 1.7 for the Treatment of Pain.

Authors :: Adams GL
Pall PS
Grauer SM
Zhou X
Ballard JE
Vavrek M
Kraus RL
Morissette P
Li N
Colarusso S
Bianchi E
Palani A
Klein R
John CT
Wang D
Tudor M
Nolting AF
Biba M
Nowak T
Makarov AA
Reibarkh M
Buevich AV
Zhong W
Regalado EL
Wang X
Gao Q
Shahripour A
Zhu Y
de Simone D
Frattarelli T
Pasquini NM
Magotti P
Iaccarino R
Li Y
Solly K
Lee KJ
Wang W
Chen F
Zeng H
Wang J
Regan H
Amin RP
Regan CP
Burgey CS
Henze DA
Sun C
Tellers DM
Source :: Journal of medicinal chemistry [J Med Chem] 2022 Jan 13; Vol. 65 (1), pp. 485-496. Date of Electronic Publication: 2021 Dec 21.
Publication Year :: 2022
Abstract: Inhibitor cystine knot peptides, derived from venom, have evolved to block ion channel function but are often toxic when dosed at pharmacologically relevant levels in vivo . The article describes the design of analogues of ProTx-II that safely display systemic in vivo blocking of Na <subscript>v</subscript> 1.7, resulting in a latency of response to thermal stimuli in rodents. The new designs achieve a better in vivo profile by improving ion channel selectivity and limiting the ability of the peptides to cause mast cell degranulation. The design rationale, structural modeling, in vitro profiles, and rat tail flick outcomes are disclosed and discussed.

Subjects :: Animals
Cell Degranulation drug effects
Cystine chemistry
Drug Design
Hot Temperature
Mast Cells drug effects
Models, Molecular
Pain Measurement drug effects
Rats
Spider Venoms pharmacology
NAV1.7 Voltage-Gated Sodium Channel drug effects
Pain drug therapy
Sodium Channel Blockers chemical synthesis
Sodium Channel Blockers pharmacology
Spider Venoms chemical synthesis

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