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IC50 versus EC50
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IC50 versus EC50
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The IC50 represents the concentration of a drug that is required for 50% inhibition of viral replication in vitro (can be corrected for protein binding etc).
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The EC50 represents the plasma concentration/AUC required for obtaining 50% of the maximum effect in vivo.
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http://www.fda.gov/ohrms/dockets/ac/00/slides/3621s1d/tsld036.htm
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IC50
From Wikipedia, the free encyclopedia
The half maximal inhibitory concentration (IC50) is a measure of the effectiveness of a compound in inhibiting biological or biochemical function. Often, the compound in question is a drug candidate. This quantitative measure indicates how much of a particular drug or other substance (inhibitor) is needed to inhibit a given biological process (or component of a process, i.e. an enzyme, cell, cell receptor or microorganism) by half. In other words, it is the half maximal (50%) inhibitory concentration (IC) of a substance (50% IC, or IC50). It is commonly used as a measure of antagonist drug potency in pharmacological research. Sometimes, it is also converted to the pIC50 scale (-log IC50), in which higher values indicate exponentially greater potency. According to the FDA, IC50 represents the concentration of a drug that is required for 50% inhibition in vitro.[1] It is comparable to an EC50 for agonist drugs. EC50 also represents the plasma concentration required for obtaining 50% of a maximum effect in vivo.[1]
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[edit] Determination IC50 of a drug
[edit] Functional antagonist assay
The IC50 of a drug can be determined by constructing a dose-response curve and examining the effect of different concentrations of antagonist on reversing agonist activity. IC50 values can be calculated for a given antagonist by determining the concentration needed to inhibit half of the maximum biological response of the agonist.[2]
IC50 values are very dependent on conditions under which they are measured. In general, the higher the concentration of inhibitor, the more agonist activity will be lowered. IC50 value increases as enzyme concentration increases. Furthermore depending on the type of inhibition other factors may influence IC50 value; for ATP dependent enzymes IC50 value has an interdependency with concentration of ATP, especially so if inhibition is all of it competitive. IC50 values can be used to compare the potency of two antagonists.
[edit] Competition binding assays
In this type of assay, a single concentration of radioligand (usually an agonist) is used in every assay tube. The ligand is used at a low concentration, usually at or below its Kd value. The level of specific binding of the radioligand is then determined in the presence of a range of concentrations of other competing non-radioactive compounds (usually antagonists), in order to measure the potency with which they compete for the binding of the radioligand. Competition curves may also be computer-fitted to a logistic function as described under direct fit.
In this situation the IC50 is the concentration of competing ligand which displaces 50% of the specific binding of the radioligand. The IC50 value is converted to an absolute inhibition constant Ki) using the Cheng-Prusoff equation (see Ki).[3][2]
[edit] IC50 and affinity
IC50 is not a direct indicator of affinity although the two can be related at least for competitive agonists and antagonists by the Cheng-Prusoff eqtn.[4]
![K_i = frac{IC_{50}}{1+frac{[S]}{K_m}}](http://upload.wikimedia.org/math/1/5/0/1504611269ebb94adfb0ebffed40bf85.png)
where Ki is the binding affinity of the inhibitor, IC50 is the functional strength of the inhibitor, [S] is substrate concentration and km is the affinity of the substrate for the enzyme.Whereas the IC50 value for a compound may vary between experiments depending on radioligand concentration, the Ki is an absolute value. Ki is the inhibition constant for a drug; the concentration of competing ligand in a competition assay which would occupy 50% of the receptors if no radioligand were present.[3]
Half maximal effective concentration
From Wikipedia, the free encyclopedia
(Redirected from EC50)
The term half maximal effective concentration (EC50) refers to the concentration of a drug, antibody or toxicant which induces a response halfway between the baseline and maximum after some specified exposure time.[1] It is commonly used as a measure of drug potency and toxicity.
The EC50 of a graded dose response curve therefore represents the concentration of a compound where 50% of its maximal effect is observed[2]. The EC50 of a quantal dose response curve represents the concentration of a compound where 50% of the population exhibit a response[3].
It is also related to IC50 which is a measure of a compound's inhibition (50% inhibition). For competition binding assays and functional antagonist assays IC50 is the most common summary measure of the dose-response curve. For agonist/stimulator assays the most common summary measure is the EC50.[4]
Concentration measures typically follow a Sigmoidal curve, increasing rapidly over a relatively small change in concentration. The point at which the effectiveness slows with increasing concentration is the IC50. This can be determined mathematically by derivation of the best-fit line. However, it is more easily observed from a graph and estimated rather than through complex calculus equations[citation needed].
Equation
Many different equations can be used to derive an EC50. One possible function is:
Y = Bottom + (Top - Bottom)/(1 + (X/EC50)(Hill coefficient))
where Y is the observed value, Bottom is the lowest observed value, Top is the highest observed value, and the Hill coefficient gives the largest absolute value of the slope of the curve.
And an alternate form of the equation is:
Y = Bottom + (Top - Bottom)/(1+ 10((Log(EC50)-X) * (Hill coefficient)))
[edit] Limitations
The effects of a stressor or drug generally depend on the exposure time. Therefore, the EC50 (and similar statistics) will be a function of exposure time. The exact shape of this time function will depend upon the stressor (e.g., the specific toxicant), its mechanism of action, the organism exposed, etcetera. This time dependency hampers the comparison of potency or toxicity between compounds and between different organisms.
LC50:半数致死浓度,引起受试对象50%个体死亡的药物浓度。
IC50:半数抑制浓度 ,一种药物能将细胞生长、病毒复制等抑制50%所需的浓度。
EC50:半数效应浓度,引起受试对象50%个体产生一种特定效应的药物剂量。
What is the difference between an IC50 and an EC50 and an ED50? FAQ# 1332
The differences are just nomenclature, and not conceptual.
"EC" means effective concentration, and is used for dose-response curves that go up hill.
"IC" means inhibitory concentration, so is used for dose-response curves that go downhill, because the drug inhibits a response.
In both cases, "C" stands for concentration. In some experiments, you vary the administered dose, but don't know the effective concentration. In these cases, the midpoint is called the ED50.
Half maximal effective concentration
From Wikipedia, the free encyclopedia
The term half maximal effective concentration (EC50) refers to the concentration of a drug, antibody or toxicant which induces a response halfway between the baseline and maximum after some specified exposure time.[1] It is commonly used as a measure of drug potency and toxicity.
The EC50 of a graded dose response curve therefore represents the concentration of a compound where 50% of its maximal effect is observed[2]. The EC50 of a quantal dose response curve represents the concentration of a compound where 50% of the population exhibit a response[3].
It is also related to IC50 which is a measure of a compound's inhibition (50% inhibition). For competition binding assays and functional antagonist assays IC50 is the most common summary measure of the dose-response curve. For agonist/stimulator assays the most common summary measure is the EC50.[4]
Concentration measures typically follow a Sigmoidal curve, increasing rapidly over a relatively small change in concentration. The point at which the effectiveness slows with increasing concentration is the IC50. This can be determined mathematically by derivation of the best-fit line. However, it is more easily observed from a graph and estimated rather than through complex calculus equations[citation needed].
Equation
Many different equations can be used to derive an EC50. One possible function is:
Y = Bottom + (Top - Bottom)/(1 + (X/EC50)(Hill coefficient))
where Y is the observed value, Bottom is the lowest observed value, Top is the highest observed value, and the Hill coefficient gives the largest absolute value of the slope of the curve.
And an alternate form of the equation is:
Y = Bottom + (Top - Bottom)/(1+ 10((Log(EC50)-X) * (Hill coefficient)))
[edit] Limitations
The effects of a stressor or drug generally depend on the exposure time. Therefore, the EC50 (and similar statistics) will be a function of exposure time. The exact shape of this time function will depend upon the stressor (e.g., the specific toxicant), its mechanism of action, the organism exposed, etcetera. This time dependency hampers the comparison of potency or toxicity between compounds and between different organisms.
LC50:半数致死浓度,引起受试对象50%个体死亡的药物浓度。
IC50:半数抑制浓度 ,一种药物能将细胞生长、病毒复制等抑制50%所需的浓度。
EC50:半数效应浓度,引起受试对象50%个体产生一种特定效应的药物剂量。
| What is the difference between an IC50 and an EC50 and an ED50? FAQ# 1332 | |
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The differences are just nomenclature, and not conceptual. "EC" means effective concentration, and is used for dose-response curves that go up hill. "IC" means inhibitory concentration, so is used for dose-response curves that go downhill, because the drug inhibits a response. In both cases, "C" stands for concentration. In some experiments, you vary the administered dose, but don't know the effective concentration. In these cases, the midpoint is called the ED50. |
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