GtoPdb is requesting financial support from commercial users. Please see our sustainability page for more information.

Zn2+   Click here for help

GtoPdb Ligand ID: 566

Synonyms: zinc | zinc ion
Compound class: Inorganic
Click here for help

Ligand Activity Visualisation Charts

These are box plot that provide a unique visualisation, summarising all the activity data for a ligand taken from ChEMBL and GtoPdb across multiple targets and species. Click on a plot to see the median, interquartile range, low and high data points. A value of zero indicates that no data are available. A separate chart is created for each target, and where possible the algorithm tries to merge ChEMBL and GtoPdb targets by matching them on name and UniProt accession, for each available species. However, please note that inconsistency in naming of targets may lead to data for the same target being reported across multiple charts.

View interactive charts of activity data across species
Natural/Endogenous Targets
Target
5-HT3A
β2-adrenoceptor
GABAA receptor α1 subunit
GABAA receptor α2 subunit
GABAA receptor α3 subunit
GABAA receptor α4 subunit
GABAA receptor α5 subunit
GABAA receptor α6 subunit
Glycine Receptor (All subtypes)
glycine receptor α1 subunit
glycine receptor α2 subunit
glycine receptor α3 subunit
glycine receptor β subunit
GPR39
ZAC
Cofactor in Enzyme Reactions
Enzyme Reference
geranylgeranyl diphosphate synthase 23
NG,NG-Dimethylarginine dimethylaminohydrolase 1
Endothelial NOS
Inducible NOS
Neuronal NOS
3-Mercaptopyruvate sulfurtransferase
Transporters Moving this Compound Across a Lipid Membrane
Transporter EC number Reaction Reference
Solute carrier family 41 member 1 7
Selectivity at GPCRs
Key to terms and symbols Click column headers to sort
Target Sp. Type Action Value Parameter Concentration range (M) Reference
β2-adrenoceptor Ligand is endogenous in the given species Hs Allosteric modulator Positive 5.3 pKi - 20-21
pKi 5.3 [20-21]
β2-adrenoceptor Ligand is endogenous in the given species Hs Allosteric modulator Negative 3.3 pKi - 20-21
pKi 3.3 [20-21]
GPR83 Mm Agonist Full agonist 5.0 pEC50 - 18
pEC50 5.0 (EC50 1.02x10-5 M) [18]
GPR39 Ligand is endogenous in the given species Hs Agonist Agonist - - - 8
[8]
Selectivity at ion channels
Key to terms and symbols Click column headers to sort
Target Sp. Type Action Value Parameter Concentration range (M) Reference
Kir2.3 Hs Channel blocker Antagonist - - 5x10-5 - 3x10-4 4
Conc range: 5x10-5 - 3x10-4 M [4]
Voltage: -100.0 – 0.0 mV
5-HT3A Ligand is endogenous in the given species Mm Allosteric modulator Biphasic - - 1x10-6 - 3x10-4 6,10
Conc range: 1x10-6 - 3x10-4 M Positive (1-10μM): increased potency of 5-HT, decreased desensitization rate, reduced effect in the presence of Mg2+ or Ca2+. Negative (30-300μM). [6,10]
Glycine Receptor (All subtypes) Ligand is endogenous in the given species Hs Allosteric modulator Inhibition - - 1x10-5 14-15,17
Conc range: 1x10-5 M [14-15,17]
Glycine Receptor (All subtypes) Ligand is endogenous in the given species Hs Allosteric modulator Potentiation - - 2x10-8 - 1x10-5 2,14-15,17
Conc range: 2x10-8 - 1x10-5 M [2,14-15,17]
Glycine Receptor (All subtypes) Ligand is endogenous in the given species N/A Subunit-specific Inhibition - - < 1x10-6 16
Conc range: < 1x10-6 M α1, α2 >> α1β, α2β [16]
Glycine Receptor (All subtypes) Ligand is endogenous in the given species N/A Subunit-specific Potentiation - - < 1x10-8 17
Conc range: < 1x10-8 M α1, α1β > α2, α2β [17]
glycine receptor α1 subunit Ligand is endogenous in the given species Hs Allosteric modulator Potentiation 7.4 pEC50 -
pEC50 7.4 (EC50 3.7x10-8 M) endogenous; not affected by β subunit co-expression
glycine receptor α2 subunit Ligand is endogenous in the given species Hs Allosteric modulator Potentiation 6.3 pEC50 -
pEC50 6.3 (EC50 5.4x10-7 M) endogenous; not affected by β subunit co-expression
ZAC Ligand is endogenous in the given species Hs Agonist Agonist 3.3 – 3.7 pEC50 - 5,22
pEC50 3.3 – 3.7 [5,22]
TRPA1 Mm Activator Activation 2.3 pEC50 - 1,9
pEC50 2.3 Zinc has similar activity at the human TRPA1 [1,9]
Description: Calcium imaging
Conditions: HEK293 cells expressing human TRPA1 and mouse dorsal root ganglia neurons loaded with Fura-2
ASIC1 Hs Channel blocker - ~8.2 pIC50 - 3
pIC50 ~8.2 (IC50 ~7x10-9 M) ASIC1a [3]
TRPM1 Ligand is endogenous in the given species Hs Channel blocker - 6.0 pIC50 -
pIC50 6.0 (IC50 1x10-6 M)
TRPM2 Ligand is endogenous in the given species Hs Channel blocker - 6.0 pIC50 -
pIC50 6.0 (IC50 1x10-6 M)
Hv1 Hs Channel blocker - ~5.7 – 6.3 pIC50 -
pIC50 ~5.7 – 6.3 (IC50 ~2x10-6 – 5x10-7 M)
glycine receptor α1 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition 4.8 pIC50 -
pIC50 4.8 (IC50 1.5x10-5 M) endogenous
glycine receptor β subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition 3.7 – 4.9 pIC50 -
pIC50 4.9 (IC50 1.3x10-5 M) endogenous; when co-expressed with the α1 subunit
pIC50 3.7 (IC50 1.8x10-4 M) endogenous; when co-expressed with the α2 subunit
ClC-4 Hs Channel blocker - 4.3 pIC50 - 19
pIC50 4.3 (IC50 5x10-5 M) [19]
Maxi Cl- Hs Channel blocker (extracellular Zn2+) - 4.3 pIC50 - 19
pIC50 4.3 (IC50 5x10-5 M) [19]
ASIC3 Hs Channel blocker - 4.2 pIC50 - 11
pIC50 4.2 (IC50 6.1x10-5 M) [11]
glycine receptor α3 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition 3.8 pIC50 -
pIC50 3.8 (IC50 1.5x10-4 M) endogenous
glycine receptor α2 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition 3.4 pIC50 -
pIC50 3.4 (IC50 3.6x10-4 M) endogenous
GABAA receptor α1 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition - - -
GABAA receptor α2 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition - - -
GABAA receptor α3 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition - - -
GABAA receptor α4 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition - - -
GABAA receptor α5 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition - - -
GABAA receptor α6 subunit Ligand is endogenous in the given species Hs Allosteric modulator Inhibition - - -
Kv12.1 Mm Gating inhibitor - - - - 24
[24]
Description: 1 mM Zn2+ slows activation 10-fold and shifts V0.5 for activation by ~+47 mV
Conditions: Heterologous expression in Xenopus oocytes
ClC-1 Hs Channel blocker - - - -
ClC-2 Hs Channel blocker - - - -
Additional information and targets (data relate to human unless otherwise stated)
Description Data Reference
Other channel blockers at TRPV5 Pb2+ = Cu2+ = Gd3+ > Cd2+ > Zn2+ > La3+ > Co2+ > Fe2
Targets where the ligand is described in the comment field
Target Comment
GABAA receptor β1 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
GABAA receptor β2 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
GABAA receptor β3 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
GABAA receptor γ2 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
GABAA receptor γ3 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
GABAA receptor α5 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
GABAA receptor δ subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively
GABAA receptor α2 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
GABAA receptor α1 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
GABAA receptor α6 subunit Diazepam and flunitrazepam are not active at channels containing this subunit. Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]. [3H]Ro154513 selectively labels α6-subunit and α4-subunit-containing receptors in the presence of a saturating concentration of a 'classical' benzodiazepine (e.g. diazepam). Sieghart et al. (2022) provides a review of the pharmacology of α6-containing GABAA receptors.
GABAA receptor α4 subunit Diazepam and flunitrazepam are not active at this subunit. Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]. [3H]Ro154513 labels α4βγ2 and α6βγ2 receptors in the presence of a saturating concentration of a 'classical' benzodiazepine (e.g. diazepam).
GABAA receptor γ1 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13], So far, the only publication investigating the pharmacology of more than three or four ligands at γ1 receptors was Khom et al. (2006) [12].
GABAA receptor α3 subunit Zn2+ is an endogenous allosteric regulator and causes potent inhibition of receptors formed from binary combinations of α and β subunits, incorporation of a δ or γ subunit causes a modest, or pronounced, reduction in inhibitory potency, respectively [13]
Ligand mentioned in the following text fields
Glycine receptors overview
ZAC overview
Acid-sensing (proton-gated) ion channels (ASICs) comments
Glycine receptors comments
Ionotropic glutamate receptors comments