Measurement of Drug Absorption Flashcards

1
Q

Define bioavailability

A
  • The extent and rate of absorption of a drug OR
  • the amount of drug reaching systemic circulation that is able to have an effect
  • determined by analyzing pharmacokinetics by measure plasma drug concentration
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2
Q

how is absolute bioavailability calculated

A

F = AUC oral/AUC IV x Dose iv/Dose oral

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3
Q

extent of absorption is more important for drugs with non-linear or linear pk

A

linear

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4
Q

how is extent of absorption measured?

A
  • total AUC under plasma level vs. time curve
  • e.g. F x D = Cl x AUC0->infinity OR
    • FD = Cl x (AUC0-t+ Ct/ß) where
      • F = fraction of dose administered which is absorbed
      • ß = rate constant of terminal elimination phase
        • for one compartment model this =K (the loss rate constant)
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5
Q

Absolute bioavailability compares

A
  • the bioavailability of the active drug in systemic circulation following non-intravenous administration with the bioavailability of the same drug following intravenous administration.
  • often obtained in a cross over study
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6
Q

the comparison of AUC of a test product to a standard product is

A

relative bioavailability

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7
Q

what is the most common method used to calculate AUC

A

linear trapezoidal rule

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8
Q

the larger the number of trapezoids, the less or more accurate the AUC

A

more accurate

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9
Q

describe the trapezoidal method

A
  • the area under the plasma concentration time curve is divided into trapezoids
  • the area of each trapezoid is added to obtain cumulative AUC
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10
Q

how is the area of the trapezoid calculated?

A
  • Area = 1/2 (c + d) (t2-t1)
    • where c is plasma cocentration at the first timepoint and d is the plasma conc at the next timepoint
    • t2-t1 = the time interval for the trapezoid
  • the last trapezoid is calculated by
    • Area = Cp(last concentration)/k
      • where K is the slope
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11
Q

Differences in the shape of profiles with same AUC are a result of differences in the

A

Rate of absorption

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12
Q

differences in the rate of absorption between products may be shown by comparing

A

the mean peak plasma concentration (Cpk) or the mean time to peak (tpk) fore each product and showing significanct difference between them

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13
Q

True or False: more rapidly absorbing products have higher Cpk and shorter tpk

A

True

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14
Q

When is the Wagner Nelson model is used to measure absorption profiles for drugs that obey one or two compartment models?

A

for drugs that obey one compartment open model

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15
Q

True or False: the AUC method for measurign extent of absorption is accruate for drugs obeying any linear multicompartment model

A

True

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16
Q

the absorption phase is described by single or multiple exponential equations?

A

Single

17
Q

what is Cpk

A

mean peak plasma concentration

18
Q

what is tpk

A

mean time to peak concentration

19
Q

what is required to estimate Cpk and tpk

A

a continuous concentration vs. time profile

20
Q

absorption profile at any time following administration of a drug (At) is calculated by these two equations

A

At = Ab + Ae

where Ab = amount in body

Ae = amount eliminated

Or

At = VCp + VK (K0 to infinity) Cp Dt

21
Q

what is needed to be known to estimate At

A

Volume of Distribution (V) and K (rate constant)