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180+ Dosage Form Design 2 Solved MCQs

These multiple-choice questions (MCQs) are designed to enhance your knowledge and understanding in the following areas: Bachelor of Pharmacy (B. Pharma) .

1.

Oral controlled release drugs release the drug only inside the intestine.

A. True
B. False
C. none
D. all
Answer» B. False
2.

What are the characteristics of continuous release systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Release only at a specific drug
D. Release as soon as comes in contact to the saliva
Answer» B. Prolonged their residence in the GIT and release
3.

What is the characteristic of delayed transit and continuous release systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Release only at a specific drug
D. Release as soon as comes in contact to the saliva
Answer» B. Prolonged their residence in the GIT and release
4.

What is the characteristic of delayed release systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Release only at a specific drug
D. Release as soon as comes in contact to the saliva
Answer» C. Release only at a specific drug
5.

What is the characteristic of dissolution controlled release systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Release only at a specific drug
D. Very slow dissolution rate
Answer» D. Very slow dissolution rate
6.

What is the characteristic of matrix dissolution-controlled release systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Release only at a specific drug
D. Employ waxes to control the rate of dissolution
Answer» D. Employ waxes to control the rate of dissolution
7.

What is the characteristic of encapsulation or coating dissolution-controlled release systems?

A. Microencapsulation using slowly dissolving materials
B. Prolonged their residence in the GIT and release
C. Release only at a specific drug
D. Employ waxes to control the rate of dissolution
Answer» A. Microencapsulation using slowly dissolving materials
8.

What are the characteristics of diffusion-controlled release systems?

A. Release the drug along the entire length of GIT
B. Diffusion of the dissolved drug
C. Release only at a specific drug
D. Employ waxes to control the rate of dissolution
Answer» B. Diffusion of the dissolved drug
9.

What are the characteristics of Matrix diffusion-controlled release systems?

A. Release the drug along the entire length of GIT
B. Drug disperse in an insoluble matrix of rigid hydrophobic materials
C. Release only at a specific drug
D. Employ waxes to control the rate of dissolution
Answer» B. Drug disperse in an insoluble matrix of rigid hydrophobic materials
10.

What are the characteristics of reservoir devices-controlled release systems?

A. Release the drug along the entire length of GIT
B. Drug disperse in the insoluble matrix of rigid hydrophobic materials
C. Hollow systems containing drug surrounded by a polymer membrane
D. Employ waxes to control the rate of dissolution
Answer» C. Hollow systems containing drug surrounded by a polymer membrane
11.

What are the characteristics of ion exchange resin drug complexes?

A. Release the drug along the entire length of GIT
B. Drug disperse in an insoluble matrix of rigid hydrophobic materials
C. Hollow systems containing drug surrounded by a polymer membrane
D. Formation of complexes between the drug and anion/cation exchange resins
Answer» D. Formation of complexes between the drug and anion/cation exchange resins
12.

What is the characteristic of pH-independent formulations?

A. Buffering agents that adjust pH to the desired value
B. Drug disperse in the insoluble matrix of rigid hydrophobic materials
C. Hollow systems containing drug surrounded by a polymer membrane
D. Formation of complexes between the drug and anion/cation exchange resins
Answer» A. Buffering agents that adjust pH to the desired value
13.

What are the characteristics of osmotic pressure-controlled systems?

A. Buffering agents that adjust pH to the desired value
B. Releases the drug at a zero-order kinetics
C. Hollow systems containing drug surrounded by a polymer membrane
D. Formation of complexes between the drug and anion/cation exchange resins
Answer» B. Releases the drug at a zero-order kinetics
14.

Osmotic pressure controlled systems work on the principle of osmotic pressure releasing the drug at constant 1st order kinetics.

A. True
B. False
C. none
D. all
Answer» B. False
15.

What are the characteristics of hydrodynamic pressure controlled systems?

A. Buffering agents that adjust pH to the desired value
B. Drug disperse in an insoluble matrix of rigid hydrophobic materials
C. Generated by swelling hydrophilic hum
D. Formation of complexes between the drug and anion/cation exchange resins
Answer» C. Generated by swelling hydrophilic hum
16.

What is the characteristics of altered density systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Release only at a specific drug
D. Use of high or low density pellets
Answer» D. Use of high or low density pellets
17.

What is the characteristics of floating or buoyant capsule systems?

A. Release the drug along the entire length of GIT
B. Granule drug with hydro gel
C. Release only at a specific drug
D. Use of high or low density pellets
Answer» B. Granule drug with hydro gel
18.

What is the characteristics of mucoadhesive systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Usage of bio adhesive polymer
D. Use of high or low density pellets
Answer» C. Usage of bio adhesive polymer
19.

Enteric coating are used for which systems?

A. Intestinal release systems
B. Colonic release systems
C. Size based systems
D. Mucoadhesive systems
Answer» A. Intestinal release systems
20.

Drugs cannot be delivered to the colon.

A. True
B. False
C. none
D. all
Answer» B. False
21.

What is the characteristics of intestinal release systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Usage of polymers that dissolves only in the alkaline pH of colon
D. Use of enteric coating
Answer» D. Use of enteric coating
22.

What is the characteristics of colonic release systems?

A. Release the drug along the entire length of GIT
B. Prolonged their residence in the GIT and release
C. Usage of polymers that dissolves only in the alkaline pH of colon
D. Use of enteric coating
Answer» C. Usage of polymers that dissolves only in the alkaline pH of colon
23.

Liposomes are spherical structures, usually between in diameter:

A. 80nm-100nm
B. 60nm-100nm
C. 55nm-1000nm
D. 15nm-1000nm
Answer» D. 15nm-1000nm
24.

Liposomes consists of a bilayer of

A. Hydrophilic molecules
B. Hydrophobic molecules
C. Both a and b
D. None
Answer» C. Both a and b
25.

Liposomes have half life

A. Longer
B. Shorter
C. Intermediate
D. Both a and b
Answer» B. Shorter
26.

Liposomes have solubility

A. Lower
B. Higher
C. Both a and b
D. None
Answer» A. Lower
27.

Liposome phospholipids undergoes

A. Oxidation
B. Hydrolysis
C. Acetylation
D. Both a and b
Answer» D. Both a and b
28.

The diameter of Small unilamellar vesicles is

A. 20-100nm
B. 20-1000nm
C. 10-100nm
D. 100nm-400nm
Answer» A. 20-100nm
29.

Intermediate sized unilamellar vesicles are prepared by

A. Sonication
B. High pressure extrusion technique
C. Detergent dialysis
D. Both b and c
Answer» D. Both b and c
30.

Tranfersome belongs to the classification according to

A. Composition
B. Application
C. Function
D. None of the above
Answer» C. Function
31.

Liposomes with ___________number of lamella are called as “pauci -lamellar liposomes”

A. Lower
B. Higher
C. Single
D. None of the above
Answer» A. Lower
32.

Loading of the entrapped agents before/during the manufacture procedure is known as

A. Active loading
B. Passive loading
C. Both a and b
D. None of the above
Answer» B. Passive loading
33.

Passive Loading Technique includes

A. Lyophilization
B. Proliposomes
C. Solvent dispersion
D. Both a and b
Answer» C. Solvent dispersion
34.

Drawback of Lipid hydration method is

A. Low internal volume
B. High encapsulation efficiency
C. Size distribution is homogenous
D. None of the above
Answer» A. Low internal volume
35.

Tip of sonicator is directly engrossed into liposome dispersion in

A. Bath sonication
B. Probe sonication
C. None of the above
D. all
Answer» B. Probe sonication
36.

The resulting liposomes from French pressure cell extrusion are ______than sonicated SUVs

A. Smaller
B. Equal
C. Larger
D. all
Answer» C. Larger
37.

To produce a microemulsion of small vesicles at least _______ circulations are required

A. at least 20 circulation but not greater than 200
B. 10 circulations
C. at least 200 circulation but not greater than 2000
D. at least 2 circulations but not greater than 10
Answer» A. at least 20 circulation but not greater than 200
38.

Dried reconstituted vesicles method is performed in

A. Solvent dispersion
B. Mechanical dispersion
C. Both a and b
D. none
Answer» B. Mechanical dispersion
39.

Solvent vaporization is also known as

A. Ether injection
B. Ethanol injection
C. Double emulsification
D. Reverse-phase evaporation
Answer» A. Ether injection
40.

Amphotericin B liposomes are given

A. Lungs
B. Oral
C. Transdermal
D. Intravenous
Answer» B. Oral
41.

Ketoconazole liposomes are given by

A. Lungs
B. Oral
C. Transdermal
D. Intravenous
Answer» C. Transdermal
42.

Temperature used for Ether Injection method is______ or under reduced pressure

A. 15-25 0C
B. 55-65 0C
C. 55-85 0C
D. None of the above
Answer» B. 55-65 0C
43.

Which of the following drugs cannot be given as transdermal administration?

A. Drugs with very short half-lives
B. Drugs with narrow therapeutic indices
C. Easy removal and termination
D. Drugs against peptic ulcer
Answer» D. Drugs against peptic ulcer
44.

Which of the following characteristics is suitable for transdermal drug?

A. Large drug dose
B. Large molecular size
C. Drugs with narrow therapeutic indices
D. Drugs which are metabolized in the skin
Answer» C. Drugs with narrow therapeutic indices
45.

What are the characteristics of the monolithic devices?

A. The drug has a large therapeutic index
B. Aqueous solutions
C. Control drug release by partitioning the drug from the oil
D. Administration of emulsions
Answer» A. The drug has a large therapeutic index
46.

The rate at which monolithic devices transfer drugs to the patient body is proportional to _______________ of time

A. Square of time
B. The square root of time
C. Twice the time
D. Half the time
Answer» B. The square root of time
47.

What are the characteristics of the reservoir or membrane devices?

A. The drug has a large therapeutic index
B. Drug permeation rate is high
C. Control drug release by partitioning the drug from the oil
D. Administration of emulsions
Answer» B. Drug permeation rate is high
48.

What are the characteristics of the mixed monolithic-reservoir devices?

A. The drug has a large therapeutic index
B. Drug permeation rate is high
C. The drug-polymer matrix is layered by rate-controlling membrane
D. Administration of emulsions
Answer» C. The drug-polymer matrix is layered by rate-controlling membrane
49.

The absorption of the ophthalmic drug does not depend on which of the following?

A. Physicochemical properties of the permeating molecule
B. Drainage of tears
C. Output of tears
D. Size of the eyeball
Answer» D. Size of the eyeball
50.

Which of the following is false in regarding reservoir devices?

A. These devices are used when the drug permeation rate is rapid
B. The release of the drug is controlled
C. Suitable for low therapeutic indices
D. The drug is contained in a powder form floating on liquid
Answer» D. The drug is contained in a powder form floating on liquid

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