Intrinsic Activity
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Intrinsic activity (IA) and efficacy refer to the relative ability of a drug-
receptor Receptor may refer to: * Sensory receptor, in physiology, any structure which, on receiving environmental stimuli, produces an informative nerve impulse *Receptor (biochemistry), in biochemistry, a protein molecule that receives and responds to a ...
complex to produce a maximum functional response. This must be distinguished from the
affinity Affinity may refer to: Commerce, finance and law * Affinity (law), kinship by marriage * Affinity analysis, a market research and business management technique * Affinity Credit Union, a Saskatchewan-based credit union * Affinity Equity Par ...
, which is a measure of the ability of the drug to bind to its molecular target, and the EC50, which is a measure of the
potency Potency may refer to: * Potency (pharmacology), a measure of the activity of a drug in a biological system * Virility * Cell potency, a measure of the differentiation potential of stem cells * In homeopathic dilutions, potency is a measure of how ...
of the drug and which is proportional to both efficacy and affinity. This use of the word "efficacy" was introduced by Stephenson (1956) to describe the way in which agonists vary in the response they produce, even when they occupy the same number of receptors. High efficacy agonists can produce the maximal response of the receptor system while occupying a relatively low proportion of the receptors in that system. There is a distinction between efficacy and intrinsic activity.


Mechanism of efficacy

Agonists of lower efficacy are not as efficient at producing a response from the drug-bound receptor, by stabilizing the active form of the drug-bound receptor. Therefore, they may not be able to produce the same maximal response, even when they occupy the entire receptor population, as the efficiency of transformation of the inactive form of the drug-receptor complex to the active drug-receptor complex may not be high enough to evoke a maximal response. Since the observed response may be less than maximal in systems with no spare receptor reserve, some low efficacy agonists are referred to as partial agonists. However, it is worth bearing in mind that these terms are relative - even partial agonists may appear as full agonists in a different system/experimental setup, as when the number of receptors increases, there may be enough drug-receptor complexes for a maximum response to be produced, even with individually low efficacy of transducing the response. There are actually relatively few ''true'' full agonists or silent antagonists; many compounds usually considered to be full agonists (such as DOI) are more accurately described as high efficacy partial agonists, as a partial agonist with efficacy over ≈80-90% is indistinguishable from a full agonist in most assays. Similarly many antagonists (such as
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) are in fact partial agonists or inverse agonists, but with very low efficacy (less than 10%). Compounds considered partial agonists tend to have efficacy in between this range. Another case is represented by silent agonists, which are ligands that can place a receptor, typically an ion channel, into a desensitized state with little or no apparent activation of it, forming a complex that can subsequently generate currents when treated with an allosteric modulator.


Intrinsic activity

Intrinsic activity of a test agonist is defined as: :\mathrm=\frac


Stevenson's efficacy

R. P. Stephenson (1925-2004) was a British pharmacologist. Efficacy has historically been treated as a proportionality constant between the binding of the drug and the generation of the biological response. Stephenson defined efficacy as: :S=ep where p is the proportion of agonist-bound receptors (given by the Hill equation) and S is the stimulus to the biological system. The response is generated by an unknown function f(S), which is assumed to be
hyperbolic Hyperbolic is an adjective describing something that resembles or pertains to a hyperbola (a curve), to hyperbole (an overstatement or exaggeration), or to hyperbolic geometry. The following phenomena are described as ''hyperbolic'' because they ...
. This model was arguably flawed in that it did not incorporate the equilibrium between the ''inactivated'' agonist-bound-receptor and the ''activated'' agonist-bound-receptor that is shown in the del Castillo Katz model.


Furchgott's efficacy

Robert F. Furchgott Robert Francis Furchgott (June 4, 1916 – May 19, 2009) was a Nobel Prize-winning American biochemist who contributed to the discovery of nitric oxide as a transient cellular signal in mammalian systems. Early life and education Furchgott ...
later improved on Stephenson's model with the definition of efficacy, e, as :S=\underbrace_\cdot p where \varepsilon is the ''intrinsic efficacy'' and ce is the total concentration of receptors. Stevenson and Furchgott's models of efficacy have been criticised and many more have been developed. The models of efficacy are shown in Kirkeby (2009).


References

{{Receptor agonists and antagonists Pharmacodynamics