Question 1

The drug concentration between MEC and MSC represents the&#8230;.&#10;A)Therapeutic Index&#10;B)Therapeutic range&#10;C)Therapeutic outcome&#10;D)Therapeutic ratio

Accepted Answer

The therapeutic range is the concentration range of a drug in the bloodstream that is effective for treatment without being toxic. It lies between the minimum effective concentration (MEC) and the minimum toxic concentration (MSC).

Question 2

Dissolution test apparatus I as per IP is&#8230;..&#10;A)Paddle&#10;B)Basket&#10;C)Rotating basket&#10;D)Rotating paddle

Accepted Answer

Paddle apparatus is used in Dissolution test apparatus I as per IP.

Question 3

Non-invasive measurement of drug concentration includes &#8230;&#8230;&#8230;.sampling.&#10;A)hair&#10;B)urine&#10;C)saliva&#10;D)All of the above

Accepted Answer

All of the options listed (hair, urine, and saliva) are non-invasive methods for measuring drug concentration, as they do not require penetrating the skin or a body cavity.

Question 4

Ex-vivo models refer to&#8230;&#8230;.&#10;A)in the body&#10;B)in the computer&#10;C)outside the body&#10;D)none of the above

Accepted Answer

Ex-vivo models refer to experiments or studies conducted on tissues or organs outside of the living organism from which they were derived, hence the term "outside the body."

Question 5

USP dissolution test apparatus type-II is also called as&#8230;..&#10;A)Hansen paddle type&#10;B)paddle over disc&#10;C)Rotating basket type&#10;D)none of the above

Accepted Answer

USP dissolution test apparatus type-II is referred to as the Hansen paddle type.

Question 6

Bioavailability from IV route is&#8230;&#8230;%&#10;A)10&#10;B)100&#10;C)1000&#10;D)10000

Accepted Answer

Bioavailability from the intravenous (IV) route is 100% because the drug is directly introduced into the bloodstream, ensuring complete absorption.

Question 7

Bioavailability of drug from topical administration is affected by&#8230;..&#10;A)Skin condition&#10;B)Topical vehicle&#10;C)Application condition&#10;D)all of the above

Accepted Answer

The bioavailability of a drug from topical administration is influenced by various factors including the condition of the skin (e.g., intact, damaged, diseased), the composition and characteristics of the topical vehicle (e.g., cream, ointment, gel), and the conditions under which the drug is applied (e.g., covered with an occlusive dressing, amount of drug applied, area of application). All these factors can affect how much of the drug penetrates the skin and becomes available to exert its therapeutic effect.

Question 8

What is bioavailability?&#10;A)The time of absorption of the drug from its dosage form&#10;B)The rate of absorption of the unchanged drug from its dosage form&#10;C)The time of absorption of the unchanged drug from its dosage form&#10;D)The rate of absorption of the drug from its dosage form

Accepted Answer

Bioavailability refers to the rate and extent to which the active ingredient or active moiety is absorbed from a drug product and becomes available at the site of action.

Question 9

What is the equation of bioavailable fraction?&#10;A)1/Bioavailable dose&#10;B)1/Administered dose&#10;C)Bioavailable dose/Administered dose&#10;D)Administered dose/Bioavailable dose

Accepted Answer

The bioavailable fraction is calculated as the ratio of the bioavailable dose (the amount of drug that reaches systemic circulation) to the administered dose. This reflects the proportion of the administered dose that is actually available for therapeutic effect.

Question 10

Which of the following is not an objective of bioavailability studies?&#10;A)Primary stages of development of suitable dosage form for new drug&#10;B)Determination of the influence of excipients, patient-related factors, etc&#10;C)Development of new formulations of the existing drugs&#10;D)Control the quantity of the drug to be administered

Accepted Answer

Bioavailability studies are primarily focused on understanding how well and how quickly a drug is absorbed and becomes available at the site of action. They aim to optimize drug formulations (A and C) and understand the influence of various factors on drug absorption (B). Controlling the quantity of the drug to be administered is more related to dosing and prescription guidelines rather than the objectives of bioavailability studies.

Question 11

Single-dose bioavailability studies are simple and common.&#10;A)True&#10;B)False&#10;C)none&#10;D)all

Accepted Answer

The answer of Single-dose bioavailability studies are simple and common.&#10;A)True&#10;B)False&#10;C)none&#10;D)all...

Question 12

Multiple dose study is better since we can understand the peak, valley, drug blood levels, etc.&#10;A)True&#10;B)False&#10;C)none&#10;D)all

Accepted Answer

The answer of Multiple dose study is better since we...

Question 13

Which of the following is the pharmacodynamics method of studying bioavailability?&#10;A)Acute pharmacologic response&#10;B)Plasma-level time studies&#10;C)Urinary excretion studies&#10;D)Stool excretion studies

Accepted Answer

The answer of Which of the following is the pharmacodynamics...

Question 14

Which of the following is not an important parameter of plasma level time studies?&#10;A)Cmax&#10;B)Tax&#10;C)The area under the plasma level-time curve&#10;D)Steady state level

Accepted Answer

The answer of Which of the following is not an...

Question 15

What is the equation for bioavailability?&#10;A)[AUC]std Dstd ?test / [AUC]test Dtest ?std&#10;B)[AUC]test Dtest ?std / [AUC]std Dstd ?test&#10;C)[AUC]test Dstd ?test / [AUC]std Dtest ?std&#10;D)1 / [AUC]std Dtest ?std

Accepted Answer

The answer of What is the equation for bioavailability?&#10;A)[AUC]std Dstd...

Question 16

The urinary excretion of the unchanged drug is directly proportional to the plasma concentration of a drug.&#10;A)True&#10;B)False&#10;C)none&#10;D)all

Accepted Answer

The answer of The urinary excretion of the unchanged drug...

Question 17

Which of the following will not be a parameter that should be examined for urinary excretion data?&#10;A)(dXu/dt) max&#10;B)(tu)max&#10;C)Xu&#10;D)Cmax

Accepted Answer

The answer of Which of the following will not be...

Question 18

Which of the following is not measured in acute pharmacological response study?&#10;A)ECG&#10;B)EEG&#10;C)Pupil diameter&#10;D)Serum drug level

Accepted Answer

The answer of Which of the following is not measured...

Question 19

Therapeutic response is based on observing the clinical response to a drug formulation.&#10;A)True&#10;B)False&#10;C)none&#10;D)all

Accepted Answer

The answer of Therapeutic response is based on observing the...

Question 20

In vitro determination of bioavailability by dissolution rate is not the best way to determine therapeutic efficacy.&#10;A)True&#10;B)False&#10;C)none&#10;D)all

Accepted Answer

The answer of In vitro determination of bioavailability by dissolution...

Question 21

The time period for which the plasma concentration of drug remains above minimum effective concentration is known as ______________&#10;A)Onset of time&#10;B)Onset of action&#10;C)Duration of drug of action&#10;D)Therapeutic range

Accepted Answer

The answer of The time period for which the plasma...

Question 22

Poor bioavailability means poor aqueous solubility.&#10;A)True&#10;B)False&#10;C)none&#10;D)all

Accepted Answer

The answer of Poor bioavailability means poor aqueous solubility.&#10;A)True&#10;B)False&#10;C)none&#10;D)all...

Question 23

A drug with poor stability means higher bioavailability.&#10;A)True&#10;B)False&#10;C)none&#10;D)all

Accepted Answer

The answer of A drug with poor stability means higher...

Question 24

Which of the following is not an approach for overcoming bioavailability problems?&#10;A)Pharmaceutic approach&#10;B)Pharmacokinetic approach&#10;C)Biologic approach&#10;D)Partition coefficient approach

Accepted Answer

The answer of Which of the following is not an...

Question 25

What will be the particle size after micronization of drugs?&#10;A)1-10 micron&#10;B)10-20 micron&#10;C)20-30 micron&#10;D)1-5 micron

Accepted Answer

The answer of What will be the particle size after...

Deck 18: Bioavailability Studies and Related Concepts