Receptors and Signalling – Summary
Introduction
Pharmacology – the study of drugs
o Naming of drugs + targets of drug action + selectivity of drugs + measuring ratio of beneficial to
unwanted effects
Naming drugs
o Classification according to:
Therapeutic use
Molecular mechanism of action
Chemical structure
o Approved name + brand name
Targets of drug action
o Selective toxicity
Drugs bind to other sites of action in addition to main site resulting in unwanted effects
o Magic bullet
Drug might act selectively at intended site of action
Has high affinity for cell – only targets main site by aiming with specific chemicals
Has little effect for organism – minimising damage
Selectivity of drugs
o Pharmacokinetics – drug motion
Study of time course of drug absorption + distribution + metabolism + excretion
Aim to achieve a higher concentration of drug at desired site of action
o Pharmacodynamics – drug power
Study of biochemical and physiological effects of drugs
Design drug to have a higher affinity for desired site of action
o Drug targets
Action at a specific binding site
Specific macromolecular targets may have high affinity for drug + high specificity –
due to stereochemistry of substrate cofactor binding
o Hormone / neurotransmitter receptors – antagonists or agonists
o Enzymes
o Transporters
o Ion channels
o DNA
Action not involving a specific binding site
Drug without identifiable binding site – acts at higher concentrations
o Action of drug is less affected by changes in chemical structure
Measuring ratio of beneficial to unwanted effects of drugs
o Amount of risk acceptable – influenced by severity of medical condition
o Ehrlick’s therapeutic index
Ehrlick’s therapeutic index = maximum non-toxic dose / minimum effective dose
Has difficulties with measurements – due to individual variations to drug
o Therapeutic index – uses better defined doses producing effects in
50% of subjects
Therapeutic index = TD50 / ED50 = toxic dose / effective dose
Dose response curve
o Toxicity
In animal studies – death can be used as a measure of
toxicity
Therapeutic index = LD50 / ED50 = lethal dose / effective dose
, Receptors and Signalling – Summary
Receptor Structure
Receptors = protein involved in mediating the effects of intercellular signalling molecules
o Site of action of: neurotransmitters + hormones + growth factors + other intercellular signalling
molecules
o Four structurally distinct families
Transmembrane receptors
Ligand-gated ion channels (LGICs)
G-protein-coupled receptors (GPCRs)
Kinase-linked and related receptors
Intracellular receptors
Nuclear receptors
Ligand-Gated Ion Channels – LGICs
Ligand-gated ion channels – AKA
o Agonist-activated ion channels
o Neurotransmitter-gated ion channels
o Ionotropic receptors
Structure
o Multi-subunit (oligomeric) transmembrane proteins – contain a central integral ion channel
Multiple subunits co-assemble with each other forming a ring-like structure
Pentameric – 5 complexes
o nAChRs
o GABAARs
o GlyRs
o 5-HT3Rs
Tetrameric – 4 complexes
o GluRs
Trimeric – 3 complexes
o ATP(P2X)Rs
o Extracellular agonist binding site – linked by conformational change to narrow portion of channel
located within lipid bilayer = channel gate
o Neurotransmitter bind to site on extracellular domain causing conformational change opening
integral ion channel (excitatory or inhibitory)
Cation channel = excitatory – causes membrane depolarisation
Acetylcholine (ACh)
o Nicotinic acetylcholine receptor (nAChR)
5-hydroxytryptpamine (5-HT)
o 5-HT(serotonin) type 3 receptor (5-HT3R)
Glutamate (Glu)
o Glutamate receptor (GluR)
Adenosine triphosphate (ATP)
o ATP (P2X) receptor
Anion channel = inhibitory – causes membrane hyperpolarisation
g-aminobutyric acid (GABA)
o GABAA receptor (GABAAR)
Glycine (Gly)
o Glycine receptor (GluR)
o Subunit structure
Pentameric LGICs
Each of the 5 subunits are a single polypeptide
Introduction
Pharmacology – the study of drugs
o Naming of drugs + targets of drug action + selectivity of drugs + measuring ratio of beneficial to
unwanted effects
Naming drugs
o Classification according to:
Therapeutic use
Molecular mechanism of action
Chemical structure
o Approved name + brand name
Targets of drug action
o Selective toxicity
Drugs bind to other sites of action in addition to main site resulting in unwanted effects
o Magic bullet
Drug might act selectively at intended site of action
Has high affinity for cell – only targets main site by aiming with specific chemicals
Has little effect for organism – minimising damage
Selectivity of drugs
o Pharmacokinetics – drug motion
Study of time course of drug absorption + distribution + metabolism + excretion
Aim to achieve a higher concentration of drug at desired site of action
o Pharmacodynamics – drug power
Study of biochemical and physiological effects of drugs
Design drug to have a higher affinity for desired site of action
o Drug targets
Action at a specific binding site
Specific macromolecular targets may have high affinity for drug + high specificity –
due to stereochemistry of substrate cofactor binding
o Hormone / neurotransmitter receptors – antagonists or agonists
o Enzymes
o Transporters
o Ion channels
o DNA
Action not involving a specific binding site
Drug without identifiable binding site – acts at higher concentrations
o Action of drug is less affected by changes in chemical structure
Measuring ratio of beneficial to unwanted effects of drugs
o Amount of risk acceptable – influenced by severity of medical condition
o Ehrlick’s therapeutic index
Ehrlick’s therapeutic index = maximum non-toxic dose / minimum effective dose
Has difficulties with measurements – due to individual variations to drug
o Therapeutic index – uses better defined doses producing effects in
50% of subjects
Therapeutic index = TD50 / ED50 = toxic dose / effective dose
Dose response curve
o Toxicity
In animal studies – death can be used as a measure of
toxicity
Therapeutic index = LD50 / ED50 = lethal dose / effective dose
, Receptors and Signalling – Summary
Receptor Structure
Receptors = protein involved in mediating the effects of intercellular signalling molecules
o Site of action of: neurotransmitters + hormones + growth factors + other intercellular signalling
molecules
o Four structurally distinct families
Transmembrane receptors
Ligand-gated ion channels (LGICs)
G-protein-coupled receptors (GPCRs)
Kinase-linked and related receptors
Intracellular receptors
Nuclear receptors
Ligand-Gated Ion Channels – LGICs
Ligand-gated ion channels – AKA
o Agonist-activated ion channels
o Neurotransmitter-gated ion channels
o Ionotropic receptors
Structure
o Multi-subunit (oligomeric) transmembrane proteins – contain a central integral ion channel
Multiple subunits co-assemble with each other forming a ring-like structure
Pentameric – 5 complexes
o nAChRs
o GABAARs
o GlyRs
o 5-HT3Rs
Tetrameric – 4 complexes
o GluRs
Trimeric – 3 complexes
o ATP(P2X)Rs
o Extracellular agonist binding site – linked by conformational change to narrow portion of channel
located within lipid bilayer = channel gate
o Neurotransmitter bind to site on extracellular domain causing conformational change opening
integral ion channel (excitatory or inhibitory)
Cation channel = excitatory – causes membrane depolarisation
Acetylcholine (ACh)
o Nicotinic acetylcholine receptor (nAChR)
5-hydroxytryptpamine (5-HT)
o 5-HT(serotonin) type 3 receptor (5-HT3R)
Glutamate (Glu)
o Glutamate receptor (GluR)
Adenosine triphosphate (ATP)
o ATP (P2X) receptor
Anion channel = inhibitory – causes membrane hyperpolarisation
g-aminobutyric acid (GABA)
o GABAA receptor (GABAAR)
Glycine (Gly)
o Glycine receptor (GluR)
o Subunit structure
Pentameric LGICs
Each of the 5 subunits are a single polypeptide
