to be distributed in specific regions of the brain. In the resting state the channels are
closed, but the binding of glutamate leads to the production of a second messenger
that triggers the opening of the channel and the movement of ions. The channel then
becomes desensitised and closes as the glutamate begins to dissociate returning the
receptor to its resting state. The receptors are targets for a number of drugs such as the
benzodiazepines. mGluRs contain an allosteric site that is a potential target for drugs
involved in the treatment of Parkinson’s disease (mGluR4), schizophrenia (mGluR5)
and addiction (mGluR2).- Frizzled/Taste family: These two subgroups of the same family have 11 and 25
members respectively. The Frizzled receptors are named after theDrosophilatissue
polarity gene known asfrizzled. The receptors bind Wnt glycoproteins involved in
transduction pathways for the control of gene expression in embryonic development
and regulation.
G-protein structure
G-proteins are heterotrimeric, consisting of one of each of three subunits,a(40–45 kDa),
b(36–40 kDa) andg(8 kDa), which are loosely attached to the inner surface of the
cellular membrane through lipophilic tails on theaandgsubunits. Thebandg
subunits are firmly attached to each other but the linkage to theasubunit is weaker.
In addition to the binding site for thebsubunit, theasubunit has a binding siteDGsPPDZArr GRKRAMPs SH2SH3GiFig. 17.7Schematic diagram of a hypothetical G-protein-coupled receptor. Labels denote general regions of
interaction of the receptor with other cellular proteins including different G-proteins (Giand Gs), PDZ, SH2 and
SH3-domain proteins, receptor-activity-modifying proteins (RAMPs), arrestin (Arr), G-protein-coupled receptor
kinase (GRK), sites for dimerisation with other GPCRs (D), and phosphorylation sites that lead to uncoupling
and internalisation (P). Any one of these active processes could be considered a form of expression of efficacy.
The figure is a general description of various loci for protein interactions, but does not represent accurate
locations, as, in most cases, these are not well characterised. (Reproduced from Kenakin, T. (2002). Efficacy
at G-protein-coupled receptors.Nature Reviews Drug Discovery, 1 , 103–110, by permission of Nature
Publishing Group.)691 17.4 Mechanisms of signal transduction