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15 research outputs found

Phosphoinositide Conversion Inactivates R-RAS and Drives Metastases in Breast Cancer

Author: Belabed H.
De Santis M. C.
Di Fiore P. P.
Forni M.
Gulluni F.
Haucke V.
Hirsch E.
Hsu M. Y.
Li H.
Margaria J. P.
Martini M.
Nazare M.
Novelli F.
Pece S.
Porporato P. E.
Prever L.
W. -T. Lo
Zanini C.
Publication venue: 'Wiley'
Publication date: 01/01/2022
Field of study

Institutional Research Information System University of Turin

A pharmacological master key mechanism that unlocks the selectivity filter gate in K+ channels

Author: Baukrowitz T
Belabed H
Carpenter EP
Conrad LJ
Constantin C
De Groot BL
Decher N
Fakler B
Gonzalez W
Kiper AK
Mackenzie A
Mert Ü
Musinszki M
Nazare M
Pike ACW
Pryde DC
Schewe M
Schulz F
Sun H
Tegtmeier M
Tucker SJ
Vowinkel KS
Publication venue: 'American Association for the Advancement of Science (AAAS)'
Publication date: 01/01/2019
Field of study

Potassium (K+) channels have been evolutionarily tuned for activation by diverse biological stimuli, and pharmacological activation is thought to target these specific gating mechanisms. Here we report a class of negatively charged activators (NCAs) that bypass the specific mechanisms but act as master keys to open K+ channels gated at their selectivity filter (SF), including many two-pore domain K+ (K2P) channels, voltage-gated hERG (human ether-à-go-go–related gene) channels and calcium (Ca2+)–activated big-conductance potassium (BK)–type channels. Functional analysis, x-ray crystallography, and molecular dynamics simulations revealed that the NCAs bind to similar sites below the SF, increase pore and SF K+ occupancy, and open the filter gate. These results uncover an unrecognized polypharmacology among K+ channel activators and highlight a filter gating machinery that is conserved across different families of K+ channels with implications for rational drug design.</jats:p

Oxford University Research Archive

A pharmacological master key mechanism that unlocks the selectivity filter gate in K<sup>+</sup> channels.

Author: Baukrowitz T.
Belabed H.
Carpenter E.
Conrad L.
Constantin C.
de Groot B.
Decher N.
Fakler B.
Gonzalez W.
Kiper A.
Mackenzie A.
Mert Ü.
Musinszki M.
Nazare M.
Pike A.
Pryde D.
Schewe M.
Schulz F.
Sun H.
Tegtmeier M.
Tucker S.
Vowinkel K.
Publication venue: 'American Association for the Advancement of Science (AAAS)'
Publication date: 01/01/2019
Field of study

Potassium (K+) channels have been evolutionarily tuned for activation by diverse biological stimuli, and pharmacological activation is thought to target these specific gating mechanisms. Here we report a class of negatively charged activators (NCAs) that bypass the specific mechanisms but act as master keys to open K+ channels gated at their selectivity filter (SF), including many two-pore domain K+ (K2P) channels, voltage-gated hERG (human ether-à-go-go-related gene) channels and calcium (Ca2+)-activated big-conductance potassium (BK)-type channels. Functional analysis, x-ray crystallography, and molecular dynamics simulations revealed that the NCAs bind to similar sites below the SF, increase pore and SF K+ occupancy, and open the filter gate. These results uncover an unrecognized polypharmacology among K+ channel activators and highlight a filter gating machinery that is conserved across different families of K+ channels with implications for rational drug design

Oxford University Research Archive

MDC Repository

MPG.PuRe