Receptor - General WM

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RECEPTOR
A General Introduction with Diagrams
Important Definitions
Pharmacology- Pharmacology is made-up of two main words- ‘Pharma’ + ‘Logy’ in some books there is Pharmakon
in the place of Pharma, but to make you better understand we have made little changes. Pharma is related with drug or
medicine and logy means- to study. So if we merge these two words together, this will become- PHARMACOLOGY.
“To study the complete life cycle of drugs as per pharmacodynamic and pharmacokinetic profile is known as
Pharmacology” now again we have got two new words- Pharmacodynamic and pharmacokinetic. Let’s understand
them also. https://www.facebook.com/pharmavideo/

Pharmacodynamic- Pharmacodynamic is a study of drug’s effect on body, so we can say it’s a study of- what
does DRUG do to the BODY. Let’s illustrate it in a very easy language.
Pharmacokinetic- “What does BODY do to the DRUG ” we have simple interchanged the BODY and DRUG to
make a definition. And as per the definition our body responds to any drug by giving ADME effects.
A stands for - Absorption
D stands for - Distribution
M stands for - Metabolism
E Stands for- Excretion or elimination

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Principle of Drug Action
Principle of drug action means how any drug produce the effect for which it has been administered. These are working methodology of drugs.

Principle Explanation Example


Irritation Senna and some other drug used in constipation irritate the intestine and increase Counter Irritant like- drugs
defecation. Other balm in case of headache will irritate the forehead tissue and gives for constipation
relief from pain for short duration. Solution Pharmacy- https://www.facebook.com/pharmavideo/
Stimulation Stimulation means to increase the function of any specialized organ, which will result in Adrenaline. Stimulates heart,
extra work, like in case of fear or fight adrenaline is get secreted and heart rate increase pilocarpine stimulates
which give FFF response. Solution Pharmacy- https://www.facebook.com/pharmavideo/ salivary glands
Depression The simple meaning of depression is the reduction of specialized activity. For example- Barbiturate depresses CNS,
Barbiturate and benzodiazepine depress the CNS and give depression action. As same Quinidine depresses heart,
Omeprazole reduce gastric acid secretion. and Omeprazole depress
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Replacement When any hormone or biochemical substance is in inadequate quantity and there Levodopa in Parkinson’s,
recovery is not possible then there is one option of replacement. The replacement is Insulin in diabetes and Iron
done for insulin in case of insulin dependent diabetes; here insulin is given by injection in Anemia.
to maintain the requirement Solution Pharmacy- https://www.facebook.com/pharmavideo/
Cytotoxic When there is entry of any parasite, or there is no other option to control the growth of Penicillin, Zidovudine,
own body cell then Cytotoxic drugs are used. They kill the microorganism of kill the Chloroquine,
uncontrolled and excessive growing cells. cyclophosphamide
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Mechanism of Drug Action
Majority of drug produce their effect by interacting with specific target molecule which are basically are proteins.

Functional protein that are target of drug action can be grouped into four major categories- (1) Enzymes (2) Ion Channels (3) Transporters (4) Receptors

Enzymes- Almost all biological reaction are carried out under the influence of enzymes and this is the reason why
enzymes are very useful target for drug action. Drugs can either increase or decrease the rate of enzymatically mediated
reactions. However in physiological system enzyme activities are in optimum condition and amount.
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Enzyme Inhibition- some chemicals like heavy metals, strong acids and base, formaldehyde and phenols denature the
protein and inhibit all enzyme no selectively. Selective inhibition of a particular enzyme is a common mode of drug
action. Enzyme inhibition may be either competitive or non competitive.

Competitive Inhibitors- these drugs are structurally similar and competes with the normal substrate for the catalytic
binding sites of the enzymes so that the product is not formed or the non functional product is formed. But if the
substrate concentration is sufficiently increased then it can displace the inhibitor and same action is achieved again.
This is equilibrium type of competitive inhibition. But if the inhibitor forms strong bond with site of enzyme bonding
and substrate can not displace inhibitor again.
Example- The comitative inhibitors of Cholinesterase and xanthine oxidase are- Physostigmine and Allopurinol.
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Substrate Inhibitor

Desirable Un-Desirable

Enzyme

Biological Action No product or Non-functional Group

Product Enzyme- Major types of bio macromolecular target of drug action


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Ion Channels
Ion channels are the path or way through which any molecule move in or out in corresponding to cell membrane.
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Protein which act as ion selective channels participate in transmembrane signalling and regulate intracellular
ionic composition. These makes them a common target of drug action. Drugs can affect ion channels, some of
which actually are receptors, because they are operated by specific signal molecule either directly and are
called ligand gated channels or through G protein and called G protein regulated ion channels.

Drugs can also act on voltage operated and stretch sensitive channels by direct binding to the channel and
affecting ion movement through it. Example- Local anaesthetic which block the voltage sensitive ion
channels. Solution Pharmacy- https://www.facebook.com/pharmavideo/

Some drugs modulate opening and closing of the channels.


Example- (1) Quinidine blocks myocardial Na+ channels
(2) Nicorandil opens ATP sensitive K+ channels.
(3) Nifedipine block L-Type of voltage sensitive Ca2+ channel.
(4) Phenytoin modulate voltage sensitive neuronal Na+ channel.
(5) Ethosuximide inhibit T type of Ca2+ channels in thalamic neuron.
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Sodium Channel Calcium Channel Chloride Channel
Na+ Ca+
Cl-

Voltage Sensor

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K+
Potassium Channel
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Transporters
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These are the specific carriers which transport drug molecule from one region to another according to concentration gradient.
Several substrate are translocated across membrane by binding to specific transporter (Carriers)which either facilitate diffusion
in the direction of the concentration gradient or pump the metabolite against the concentration gradient using metabolic energy.

Example-Amphetamine selectively block dopamine reuptake of 5HT by interacting with serotonin transporter.

Inhibitor

Substrate

Transporter

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RECEPTOR
Receptors are the macromolecule or binding site located on the surface or inside the effector cell that serve to
recognize the signal molecule or drug and initiate the response to it, but they don’t have other functions.

The largest number of drug that do not bind directly to the effectors like- Enzyme, Channels, Transporter structural
protein, template biomolecule but act through specific regulatory macromolecule or the site on them which bind and
interact with the drugs are called “Receptor”

Few Basic terms related to receptor and drug-receptor complex Solution Pharmacy- https://www.facebook.com/pharmavideo/

1. Agonist- Agonist are the agent which activates the receptor to produce an effect similar to the of the
physiological signal molecule
2. Antagonist- Antagonists are agent which prevent the action of agonist on a receptor or the subsequent response,
but does not have any effect of its own
3. Inverse Agonist- Inverse Agonist is the agents which activates a receptor to produce an effect in the opposite
direction to that of the agonist
4. Partial Agonist- An agent who activates receptors to produce a sub maximal effect but antagonize the effect of
full agonist.
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Receptor Occupation Theory
When a drug bind to a receptor it makes DRUG+ RECEPTOR Complex. Single drug without receptor and single
receptor without drug will not be able to produce any of effect.

Drug + Receptor = Drug-Receptor Complex Biological Action


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Drug
Drug/Signal

Drug-Receptor
Complex
Receptor

Biological Action Biological Action Receptor Biological Action

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Classification of Receptors
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1. Pharmacological Criteria- This is based on relative potency of selective agonist and antagonist. This was used
in delineating M and N cholinergic, Alpha and Beta adrenergic, H1 and H2 histaminergic receptors etc.
2. Tissue distribution- the relative organ/tissue distribution is basis for designing the subtype. Example- The
cardiac Beta adrenergic receptor as- Beta 1 while bronchial as Beta2 Solution Pharmacy- https://www.facebook.com/pharmavideo/
3. Ligand binding- Measurement of specific binding of high affinity radio-labelled ligand to cellular fragment in
vivo and its displacement by various selective agonist and antagonist is used to find receptor subtypes. Multiple
5-HT receptors were distinguish by this approach.
4. Transducer pathway- receptor subtypes may be distinguish by the mechanism through which their activation
is linked to response. Example- M cholinergic receptors acts through G-protein, while N cholinergic receptors
get influx of Na+ ions, Alfa adrenergic receptors via IP3-DAG pathway and by decreasing cAMP pathway.
5. Molecular cloning- The receptor protein is cloned and its detailed amino acid sequence as well as three
dimensional structure is worked out.
Silent receptor- These are sites which bind specific drug but no pharmacological response is elicited.

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G-protein Coupled Receptors (Gpcrs)
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Important points and steps to be remember about GPCRs

1. This is a large family of cell membrane receptors


2. The molecule have 7 Alfa helical membrane spanning hydrophobic amino acid (AA)
3. There are 06 loops- 03 extracellular and 03 intracellular
4. It have 03 subunits- Alfa, Beta and Gamma
5. Agonist binding site is located somewhere in between helices on extracellular faces.
6. In the inactive state GDP is bound to Alfa subunits at the exposed domain.
7. Activation through the receptor leads to displacement of GDP by GTP.
8. The activated alfa subunits carrying dissociate from the other two subunits and either activate or inhibit
effectors. Solution Pharmacy- https://www.facebook.com/pharmavideo/

9. The remaining Beta- Gamma diamer has also been shown to activate receptor operated K+ channels, to
inhibit voltage gated Ca2+ channels and to promote desensitization at higher rates of activation.
10. The bound GTP is slowly hydrolysed to GDP then Alfa subunits dissociate from effectors and re-join its
other subunits.

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03 loop at extra cellular region Ligand binding to the receptor

1 2 3

Plasma Membrane
Extra Cellular

1 2 3 4 5 6 7 1 2 3 4 5 6 7

Intra Cellular

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03 loop at Intra cellular region Alpha Beta Active G-Protein Alpha Beta

GTP GDP GDP


Gamma GTP
Gamma
Inactive G-Protein Intracellular Response
Phospholipase C- IP3-DAG Pathway
To make the concept clear we have converted paragraph into points, so this pathway contains following important points
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1. Activation of phospholipase C by the activated GTP carrying Alfa subunits of Gq hydrolyses the membrane
phospholipids inositol 4,5 bisphosphate to generate the second messenger inositol 1,4,5 triphosphate (IP3)and
diacylglycerol (DAG)
2. the IP3 being water soluble diffuse to the cytosol and mobilize ca2+ from endoplasmic reticulum depot.
3. The lipophilic DAG remain within the membrane but recruits protein kinase and activate it with the help of
Ca2+
4. The activated protein kinase phosphorylates many intra cellular proteins and mediates various physiological
response. That’s why it serve in signalling function.
5. The cytosolic concentration of Ca2+ is kept very low (About 100nM) by specific pumps located at plasma
membrane and at the endoplasmic reticulum.
6. Triggering by IP3 the released Ca2+ (3rd Messenger) act as a highly versatile regulator acting through
calmodulin.

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Ion Channel Receptors
1. The extracellular portion of ligand-gated ion channels usually contains the ligand binding site.
2. This site regulates the shape of pore through which ions can flow across the cell membrane
3. The channel is usually closed until the receptor is activated by an agonist, which opens the
channel briefly for a few milliseconds. Solution Pharmacy- https://www.facebook.com/pharmavideo/
4. Depending on the ion conducted through these channels, these receptors mediates various
function like- neurotransmission, cardiac or muscle contraction. Example- stimulation of
nicotinic receptor by acetylcholine result in sodium influx and potassium outflux, generating
action potential in a neuron.
5. Agonist stimulation of GABA receptor increase chloride influx and hyperpolarizing of neurons.
6. Thus in these receptors the agonist directly operate ion channels, without the intervention of nay
coupling protein or second messenger.
7. The onset and offset of response through this class of receptors are fastest.
Example- GABA A, Glycine, Excitatory AA glutamate and 5HT3 receptors are the example.

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Intracellular Receptor
1. This is entirely different from other receptors because it is present in the intracellular region.
2. Ligand must diffuse into the cell to interact with the receptor.
3. In order to move across the target cell the target cell membrane the ligand must have sufficient lipid solubility
4. The primary target of these ligand-receptor of these ligand-receptor complex are transcription factor in the cell
nucleus. Solution Pharmacy- https://www.facebook.com/pharmavideo/

5. Binding of ligand with its receptor generally activates the receptor via dislocation from a variety of binding
proteins.
6. The activated ligand-receptor complex is then translocate to nucleus, where it often dimerizes before binding to
transcription factor that regulate gene expression. Example- steroid hormones exert there action on target cell via
intracellular receptor.
7. The activation and inactivation of these factors causes the transcription of DNA to RNA and translocation of RNA
into an array of protein Solution Pharmacy- https://www.facebook.com/pharmavideo/

8. Other target of intracellular ligands are structural proteins, enzymes, RNA and ribosome.

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Drug

Target Cell
Drug

Activated Receptor Complex


Drug

Inactive Receptor

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The drug receptor complex binds


Gene
to chromatin, activating the
transcription of specific gene

Nucleus

mRNA

Mechanism of Intracellular Receptor


mRNA

Specific Protein
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Biological Effects
Function of Receptors

Receptors have various functions. Few of Important functions are-

1. To propagate regulatory signals from outside to inside the effector cell when the molecular species
carrying the signal can’t itself penetrate the cell membrane .
2. To amplify the signals Solution Pharmacy- https://www.facebook.com/pharmavideo/
3. To integrate various extracellular and intracellular regulatory signals.
4. To adapt to short term and long term changes in the regulatory melieu and maintain homeostasis.

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Agonist
Competitive Antagonist

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Agonist
Receptor Definitions

* All diagrams are made by- Solution- Pharmacy (Reference- KDT & Lippincott)
1. Agonist- Agonist are the agent
which activates the receptor to
produce an effect similar to the of
Allosteric Site Resting State Allosteric Site
RESPONSE the physiological signal molecule

Image 2- Site of action for antagonist 2. Antagonist- Antagonists are agent


Image 1- Site of action for agonist & antagonist
which prevent the action of
Agonist agonist on a receptor or the
Agonist Competitive Antagonist subsequent response, but does not
Partial Agonist
have any effect of its own

3. Partial Agonist- An agent who


activates receptors to produce a
sub maximal effect but antagonize
the effect of full agonist.

4. Competitive Antagonist- The


antagonist is chemically similar to
Allosteric Site No Response the agonist an compete with it for
Sub Maximal Response Antagonism of Agonist
the binding site.
Image 3- Partial Agonist Image 4- Competitive Antagonist

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