a) Tablet Weight Variation Test. b) Tablet hardness Test. c) Tablet friability Test. d) Tablet disintegration Test. e) Tablet dissolution Test. f) Leakage test of Packaging of tablets / capsules. g) Capsule weight variation test h) Determination of Binding Sites and Association constant.

1. Page 1 of 10
INDEX
Serial No. Date Name of the experiment Page No.
01 Determinations of the uniformity of weight of
Paracetamol 500 mg Tablet.
2 –3
02 Friability test of Paracetamol 500 mg Tablet 4 – 4
03 Determinations of the Hardness of Paracetamol 500 mg
Tablet
5-6
04 Determination of Disintegration Time of Paracetamol
500 mg Tablet.
7-7
05 Determination of Dissolution Time of Paracetamol 500
mg Tablet.
8-10

2. Page 2 of 10
Principle
The uniformity of tablet dosage form can be demonstrated by either by weight variation or content
uniformity test. Weight variation is a compendia test for tablet dosage form and performed when
tablets to be tested. A tablet contains 50 mg or more of a single active ingredient comprising 50% or
more by weight of the tablet dosage form unit. If the drug forms greater part of the tablet, any
variation in the tablet weight obviously indicates a variation in the active ingredient.
Tablet dosage form uniformity by weight variation is determined by selecting not less than 30 tablets
form each production batch and weighing accurately at least 10 t5ablets individually and calculating
the average weight was followings:-
Average weight= (Total weight of tablets) (Number of Tablets)
i.e. Average weight of Tablets X=(X1+X2+X3+……+Xn)÷ n
Where, n=Total number of tablets weighted.
And,
Percent deviation (error) of a tablet=
weightAverage
100xweight)Average-weightindividualofWeight(
i.e. % Deviation=
X
XXi 100x)( 
……..(i)
Where, i=1, 2, 3…….n
Pharmacopoeal Requirements:
Not more than two of the individual tablet weights deviate from thre3 average weight by more than
the specified limit mentioned in the following table and none deviates by more than twice that%.
Pharmacopoea Average weight of Tablet Maximum % Deviation
USP Tablet less than 120 mg ±10%
Range from 120-300 mg ±7.5%
More Than 300 mg ±5.0%
BP 80 mg or Less ±10%
>80 mg and <250 mg ±7.5%
250 mg or more ±5.0%
Since, the average weight X of Paracetamol500 mg tablet is more than 250 mg
(according to BP) allowed parent deviation should be ±5.0% and not more than two of the individual
tablet weights should deviate by ±5.0% and more should deviate by ±10%
Instrumentation:
Electronic Balance
Experiment Number: 01 Date:18.09.2012
Name of The Experiment: Determinations of the uniformity of weight of
Paracetamol 500 mg Tablet

3. Page 3 of 10
Procedure:
20 tablets were weighted individually .Then the average weigh was calculated and percentage of
weight variation was calculated by using the equation ( i) i.e.
X
XXi 100x)( 
Where, Xi=Sample 1, 2, 3………..20
X=Average weight of 20 tablets.
Data:
Tablet number
(n)
Individual weight
(Xi)
Average weight
[X=
20
100x)( XXi 
Percent Deviation
X
XXi 100x)( 
1st
2nd
3rd
4th
5th
6th
7th
8th
9th
10th
11th
12th
13th
14th
15th
16th
17th
18th
19th
20th
Total weight=
Test result:
1. The percentage of weight variation ranges from to .
2. Number of Tablet (tablet number……..) deviated by ±5.0% and this deviation (% error….) is less
than ±10%.
Comments:
The uniformity of weight if 20 tablets comply with the mentioned specification .So the bath may be
declared as passed.

4. Page 4 of 10
Principle:
Friability is the tendency of tablet to crumble. It is impor4tent for the tablet to resist attrition .Friction
and shocks are the forces that most often cause tablets to chip, crack or break. The friability test is
designed to evaluate the ability of the tablet to withstand abrasion in packaging, handling and
shipping. Another application of friability test is to detect incipient capping or laminate when stressed
by attrition inside the rotating cylinder present on the friability tester. It is usually measured by the use
of a Roche Friabilitor .A number of tablets is weighted and placed in the apparatus where they are
exposed to rolling and repeated shocks as they fall 6 inches in each turn within the apparatus. The
value is expressed as percentage.The accepted limit of weight loss after this experiment should not be
more than 1 percent% of the total weight of the tablets.
The percent of weight loss can be calculated by using the following formula .
Percentage of weight loss or friability =
weightInitial
weightFinal-weightInitial
Instrumentation: 1. Electronic Balance
& 2. Roche Friabilitor (which consists of plastic chamber divided into two parts and revolves at a speed of 25 rpm.)
Procedure:
1. Tablets were weighted as not less than 6 gm and taken in the plastic chamber of Friabilator.If the
individual weight of tablet is≤600 mg then more than 10 tablets were taken.
2. The chamber was allowed to rotate for about 4 minutes at 25 rpm and then the weight of tablets was
taken again. The loss in weight indicates the friability.
3. Finally, The percentage of weight loss was calculated.
Calculation:
Initial weight of tablets =
Final weight of tablets =
Percent loss or Friability tablets =
weightInitial
weightFinal-weightInitial
=
=
Result:
The Friability of the tablets were found to be = Percent (%) W/W
Comments: The uniformity of weight if 20 tablets comply with the mentioned specification .So the
bath may be declared as passed.
Experiment Number: 02 Date:18.09.2012
Name of The Experiment: Friability test of Paracetamol 500 mg Tablet

5. Page 5 of 10
Theory:
Tablets should be sufficiently hard to resist breaking during normal, handling, packaging and shipping
and must be soft enough to disintegrate properly after swallowing. So the resistance of tablets to
capping, abrasion or breaking under conditions of storage, transportation and handling before usage
depends on its hardness.
Hardness of the tablet is a non-compendial test and is controlled by the degree of the pressure applied
during the compression stage. Hardness is an important criterion, since it can affect disintegration and
subsequent dissolutuion.If the tablet is too hard, it may not disintegrate in the required period of time
to meet the dissolution specifications; if it is too soft it may not be able to withstand the handling
during subsequent processing such as coating, packaging and shipping operations.
The test measures crushing strength property; defined as ‘‘the compressional force applied
diametrically to a tablet, which just fracture (break) it’’.The force required to break the tablet is
measured in kilograms. Force of about 4 kg is considered the minimum requirement for a satisfactory
tablet.
Measuring Units:
The moist tablet testing is performed using international system of units. The Newton is the preferred
unit of the force as is recognized by the SI system. However the kilogram is also used.
1. Kilogram (Kg): It is the primary unit of mass recognized by SI system.
2. Newton (N): Newton is the SI unit of force and should not be used for tablet hardness testing.
1 Kilogram = 9.807 Newton’s
3.Pound (lb): Technically a unit of mass but can also be used for force. 1 Kilogram = 2.204 Pounds
4.Kilopounds (kp): A unit of force also called kilogram of force.1 Kilopounds =1 kgf.
5. Strong cob (sc): It us an arbitrary unit. 1.4 Strong cob = 1 kg
Interrelationship of the units:
l kg = 9.807 New tons
1 kg = 2.204 pounds
1 kg = 1.4 strong cobs
l kg = 1 kilopond.
Experiment Number: 03 Date:18.09.2012
Name of The Experiment: Determinations of the Hardness of Paracetamol 500 mg
Tablet

6. Page 6 of 10
Instrument used:
Several devices have been used to test tablet hardness. These include-
1. Monsanto hardness tester.
2. Pfizer hardness tester
3. Strong coble hardness tester.
Monsanto hardness tester is generally used to measure tablet hardness.
Procedure:
The tablet to be tested was held between a fixed and moving tank and the reading of the indicator was
adjusted to zero. The force applied to the edge of the tablet was gradually increased by moving screw
knob forward until the tablet breaks.
The reading was noted from the scale which indicates the required pressure in kg to break the tablet.
Precaution:
Tablet Hardness may be affected by speed of testing, geometry of the tablet contact points, debris in
the testing area, variation in temperature humidity, tablet age etc. so, care should be taken.
Data :
No. of table Hardness in kg
1st
Tablet 2.5 kg 4.5 kg
2nd
Tablet 5.5 kg 5.0 kg
3rd
Tablet 6 kg 4.5 kg
4th
Tablet 6 kg 4.0 kg
5th
Tablet 5 kg 5. kg
6th
Tablet 4.6 kg 4.5 kg
Result:
The range of six readings: 4.6 to 6 kg
Comments: The average hardness of supplied Paracetamil 500 mg was 5.43 kg which is within the
expected limit.

7. Page 7 of 10
Theory:
The disintegration test is a measure of the time required under a given set of conditions for a group of
tablets to break down into particles which will pass through a 10 mesh screen.
If one or two tablets fail to disintegrate, the test should be repeated using 12 tablets.
Instrumentation:
1. Disintegration Tester
2. Glass beaker 1 Litre
3. Thermometer
The disintegration tester consists of a basket rack holding 6 plastic tubes, open at the top and bottom.
The bottom of the lube is covered by a 10-mesh screen. The basket is immersed in a bath of suitable
liquid held at 37°C, preferably in a 1 Liter beaker.
Test condition:
1
Temperature of simulated Gastric fluid: 37°C ± 0.5 Procedure:
One tablet was placed in each plastic tube and a plastic disc is placed over the tablet. The basket was
positioned in one liter beaker containing 900ml gastric simulated fluid at 37°C in such a way that at
the highest position of the tube, the screen remains below the surface of liquid surface.
The machine was agitated until the tablet disintegrated. The end point of the lest was achieved when
no tablet fragments was remaining on the screen. The time of disintegration was recorded.
Data:
No. of table Disintegration time (min-sec)
1st
Tablet 6.5 sec 1 min 41
2nd
Tablet 68 sec 1 min 17
3rd
Tablet 70 sec 2.06
4th
Tablet 72 sec 1.38
5th
Tablet 75 sec 1.34
6th
Tablet 77 sec 2.50
Result:
The disintegration time of the supplied tablets ranges from 65 sec to 77 sec.
Experiment Number: 04 Date:18.09.2012
Name of The Experiment: Determination of Disintegration Time of Paracetamol
500 mg Tablet.

8. Page 8 of 10
Theory:
When a drug administered orally in the form of tablet, the rate of absorption is often controlled how
fast the drag is dissolved in GIT fluid of the absorption site.
Drug in solid dosage form in GIT fluid
Kd
drug in solution Drug in blood
Elimination GIT fluid.
Here Kd represents the rate constant governing dissolution of drug in the GI fluid very often Ka>>Kd
and dissolution is the rate limiting step in the overall absorption process. As a result, the onset
intensity and the duration of action as well as the extent of drug absorption or bioavailability may be
altered by change in the dissolution rate.
The objective of in vitro dissolution test is as follows-
1. Whether the drug release is 100% or not.
2. Whether the rate of drug dissolution is uniform from batch to batch or not.
3. According to BP and USP the range of percentage release of drug should be ±5%.
Apparatus:
1. USP dissolution lest apparatus
2. Test tube rack
3. Filter paper
4. Pipette.
5. Volumetric flask
6. Measuring flask
7. Spcctrophotometer.
USP dissolution test apparatus:
It consists of 1000ml vessel made up of glass or inert transparent material, a variable speed motor and
a cylindrical dissolution basket. The vessel can be immerged in a suitable water bath at any contention
at size that permits keeping the water continuously in motion and holding the temperature at
37±().5()°c. The basket is detectable and made up of'16 mesh stainless steel set formed into cylinder
3.66cm height of 25 cm in diameter.
Reagents:
1. Gastric simulated fluid
2. N/10 NaOH solution
3. Distilled water
Experiment Number: 05 Date:18.09.2012
Name of The Experiment: Determination of Dissolution Time of Paracetamol 500 mg
Tablet.

9. Page 9 of 10
Preparation of simulated gastric fluid:
2gm of NaCl and 7 ml of cone, MCI taken in a large beaker containing distilled water then the
content was transferred in a volumetric flask and the final volume was made 1000 ml by adding
sufficient distilled wetter.
Procedure:
1. The beaker was filled with 1000ml gastric simulated fluid and the fluid was heated up to 37°c
by adjusting temperature.
2. The tablet was put into the beaker and the instrument was stirred immediately the speed of the
stirrer was 50 rpm.
3. After 30 minutes l0 ml of sample from the beaker was taken in a test tube and was filtered.
4. 2 ml of filtrate was taken and 0.1N NaOH was added to it up to 100ml &s it sample solution.
Preparation of blank solution:
2 ml of gastric simulated fluid was taken in to 100 ml volumetric flask and 0.1N NaOH added it to
make. It was the blank solution.
Preparation of standard solution:
Each paracetamol tablet contains 500mg active ingredient pracelamol BP. A tablet was dissolved in
100.0 ml fluid. So, 1000 ml fluid contains 500 mg of paracetamol
1 ml fluid contain =
500
1000 mg of paracetamol
100 ml fluid contain = 1000
100500 
mg of paracetamo
= 50gm of paracetamol
Approximately 50mg (0.0gm) paracetamol was dissolved in gastric fluid was made the
100 ml with it. 10 ml was taken from the solution and was filtered.
From the filtrate 2ml was taken in a measuring cylinder and 0.1N NaOH and added to make the
volume 100 ml. It was the/standard solution.
Now the absorbance of blank solution sample solution & standard solution were taken at 254 nm in a
spectrophotometer.
At first the absorbance of the blank solution were taken and the apparatus was done at auto zero. So,
this reading was not necessary.
After this reading the absorbance of sample standard was taken then, the percentage of content of
paracetamol in the solution was calculated.
1000 ml simulated fluid conation = 500 mg of paracetamol
1 ml simulated fluid contain = 100
500
mg of paracetamol
= 0.5 gm of paracetamol
Therefore, the concentration of standard solution was 0.5 mg/ml of pracetamol.

10. Page 10 of 10
Concentration of sample solution can be calculated by using following formula
Csd
Cs
Asd
As

mlmg
Asd
CsdAs
Cs /4646.0
651.0
5.0605.0
1............. 




Where, Cs is concentration of sample solution = 0.4646 mg/ml.
concentration of standard solution Csd = 0.5 mg/ml
Absorbance of sample solution As = 0.605
Absorbance of sample solution Asd = 0.651
Now,
1 ml fluid contain = 0.4646
1000 ml fluid contain = 0.46461000
We know that, = 646.6 mg
% Release of drug = 100
dragofamount
ountofdrugdeclaredam
obtaining
Result:
Percentage release of peacetime was 92.93%