Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
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Enzyme
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Query: EC:4.2.3.23 (
GAS
)
957
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Trimeric acid-sensing ion channels (ASICs) contribute to neuronal signaling by converting extracellular acidification into excitatory sodium currents. Previous work with homomeric ASIC1a implicates conserved leucine (L7') and consecutive glycine-alanine-serine (
GAS
belt) residues near the middle, and conserved negatively charged (E18') residues at the bottom of the pore in ion permeation and/or selectivity. However, a conserved mechanism of ion selectivity throughout the ASIC family has not been established. We therefore explored the molecular determinants of ion selectivity in heteromeric ASIC1a/
ASIC2a
and homomeric
ASIC2a
channels using site-directed mutagenesis, electrophysiology, and molecular dynamics free energy simulations. Similar to ASIC1a, E18' residues create an energetic preference for sodium ions at the lower end of the pore in
ASIC2a
-containing channels. However, and in contrast to ASIC1a homomers, ion permeation through
ASIC2a
-containing channels is not determined by L7' side chains in the upper part of the channel. This may be, in part, due to
ASIC2a
-specific negatively charged residues (E59 and E62) that lower the energy of ions in the upper pore, thus making the
GAS
belt more important for selectivity. This is confirmed by experiments showing that the L7'A mutation has no effect in
ASIC2a
, in contrast to ASIC1a, where it eliminated selectivity.
ASIC2a
triple mutants eliminating both L7' and upper charges did not lead to large changes in selectivity, suggesting a different role for L7' in
ASIC2a
compared with ASIC1a channels. In contrast, we observed measurable changes in ion selectivity in
ASIC2a
-containing channels with
GAS
belt mutations. Our results suggest that ion conduction and selectivity in the upper part of the ASIC pore may differ between subtypes, whereas the essential role of E18' in ion selectivity is conserved. Furthermore, we demonstrate that heteromeric channels containing mutations in only one of two ASIC subtypes provide a means of functionally testing mutations that render homomeric channels nonfunctional.
...
PMID:Determinants of ion selectivity in ASIC1a- and ASIC2a-containing acid-sensing ion channels. 3195 79
