ISSN:2230-7346
Available online [Link]
Research Article
Journal of Global Trends in Pharmaceutical Sciences
Vol.2, Issue 1, pp 1-10, JanuaryMarch 2011
STUDIES ON DISSOLUTION RATE OF PARACETAMOL TABLETS BY USING
DIFFERENT POLYMERS
B.HanumanKishore1*, T.Venkareswararao1, [Link] Sankar2, [Link] Rao3
1. Department of Pharmaceutics, Bapatla College of Pharmacy, Bapatla, Guntur,A.P, India
2. Sri Sai Aditya Institute of Pharmaceutical Sciences & Research, Surampalem,
East Godavari, A.P, India
3. Birla Institute of Technology and Science (BITS), Pilani, Rajasthan, India.
Corresponding author E-Mail: [Link]@[Link]
ABSTRACT
Paracetamol is an analgesic and anti-pyretic drug which is poorly soluble in water.
Trend towards formulations of dispersible tablets is evident throughout the world. The main of
this study is to formulate Paracetamol fast dissolving tablets and to study the effect of various
hydrophilic polymers and disintegrating agents on drug releasing characteristics of the prepared
Paracetamol dispersible tablets. Magnesium sterate, Talc, Polyvinyl pyrolidine (PVP), potato
starch, Hydroxy propyl methyl cellulose (HPMC-4000), Primogel are used as excipients.
Paracetamol dispersible tablets are prepared by wet granulation method. The prepared
formulations were passed the evaluation test that is weight variations, Percentage drug content,
and disintegration, Uniformity of dispersion, Hardness & friability. When compared to potato
starch, the Primogel is showing better increase in rate of dissolution of prepared tablets. Out of
those three formulations F2, F3 and F4 in which Primogel (5%) used as extra disintegrating
agents was used.F4 was showing better increase in rate of dissolution of drug.F4 was prepared
by solid dispersion of Paracetamol with PVP. First order rate constant values: K2<K3<K4
Regression Coefficient values: R2<R3<R4.
KEY WORDS: Paracetamol, Primogel, Potato starch, Talc, HPMC, PVP, Dissolution rate.
�INTRODUCTION:
The oral route of administration is the most
forms have also other disadvantages when
important method of administering drugs for
compared to the tablets2.
systemic effects .Nevertheless ,it is probable
Paracetamol is an analgesic and anti pyretic
that at least 90% of all drugs used to
drug which is poorly soluble in water.
produce systemic effects are administered
Formulation
by the oral route .Tablets are intended for
dissolving tablets are advantageous over the
oral administration, some are swallowed
conventional as they disintegrates easily and
whole, some after being chewed. Some are
enhancing fast dissolving their by fast
dissolved or dispersed in water before being
absorption and fast onset of action, resulting
administered and some are retained on the
in faster exhibition of therapeutic responses
mouth, where the active ingredients are
.hence, these Paracetamol rapid dissolving
liberated .tablets are mainly used for
tablets are preferable than conventional .this
systemic effect drug delivery. For systemic
also help to improve patient compliance.
use drug must be released from tablets that
The
dissolved in fluids of the mouth, stomach
dispersible tablets is evident throughout the
and intestine and then absorbed in to
world. for example, it is understood that all
systemic circulation by which it shows its
the tablets marked in nevertheless must have
trend
of
Paracetamol
towards
as
formulations
rapid
of
therapeutics effects .
the ability to form adequate dispersion when
Tablets and capsules represent unit dosage
placed
form in which one usual dose of the drug
characteristics of other solid dosage forms.
has been accurately placed1. By comparison,
The dispersible tablets are uncoated tablets
liquid dosage form are usually designed to
that produce a uniform dispersion in water3.
contain one dose of
medication in 5-
The main of this study is to formulate
[Link] patient is then asked to measure his
Paracetamol fast dissolving tablets4 and to
or her own medication using teaspoon
study the effect of various hydrophilic
,tablespoon or other measuring devices.
polymers and disintegrating agents on drug
Such dosage measurements are typically
releasing characteristics of the prepared
error by a factor ranging from 20-50% when
Paracetamol dispersible tablets.
the drug itself the patient. Liquid dosage
2
in
water.5They
have
stability
�and ethyl alcohol was added drop wise to get
APPARATUS AND EQUIPMENTS:
tester,
the damp mass. this damp mass was passed
IP/BP/USP
through a sieve no:16. The obtained
standards (Campbell electronics, Bombay),
granules were dried in hot air oven at
Digital
[Link] obtained dried granules were
Monsanto
disintegration
electronic
electronics,
automatic
test
hardness
machine
balance
Bombay)
single
punch
(Campbell
cadmach
semi
again passed through sieve no: 120. Now
tablets
press
potato starch (5%)
as extra granular
(cadmach type no: CMS -25, Serial No:
disintegrating agent. the bolted Magnesium
H/464/98, Ahamadabad)Digital Rou Digital
sterate, Talc-(2%) were added one by one to
electronic balance (Campbell electronics,
obtained granules and mixed uniformly.
Bombay) cadmach semi automatic single
By using Primogel as Super-
punch tablets press (cadmach type no: CMS
disintegrating agent:
-25, Serial No: H/464/98, Ahmadabad)
The Required quantity of Paracetamol9,
Digital
Polyvinyl pyrolidine (PVP-2%) were mixed
Roches
friabilator(Campbell
electronics, Bombay)
thoroughly in a mortar and The obtained
CHEMICALS:
ethyl alcohol was added drop wise to get the
Paracetamol,
damp mass. this damp mass was passed
Magnesium Sterate, Talc-YarrowChem.
through a sieve no:[Link] were dried in
Products, Dombivli), Polyvinyl pyrolidine
hot air oven at [Link] obtained dried
(PVP), potato starch, Hydroxy propyl
granules were again passed through sieve
methyl cellulose (HPMC-4000), Primogel
no: 16. Now Magnesium sterate passed
from S.D Fine chem. LTD.
through sieve no: 120. Now Primogel (5%),
the bolted Magnesium sterate, Talc-(2%)
METHOD OF PREPARATION:
were added one by one to obtained granules
WET GRANULATION METHOD:
and mixed uniformly.
By using potato starch as disintegrating
agent
The Required quantity of Paracetamol,
Polyvinyl pyrolidine (PVP-2%) and potato
starch-5% as inter granular disintegrating
agent were mixed thoroughly in a mortar
3
�polymers
The granules of F1, F2, F3,
(HPMC,PVP) and Primogel as Super-
and F4 were compressed with 9mm punches
disintegrating agent:
by Cadmach semi automatic single punch
By
using
two
different
The Required quantity of
press the hardness of the tablets was
Paracetamol, Polyvinyl pyrolidine (PVP-
adjusted to optimum levels with required
10%), HPMC-4000(10%) were weighed. in
amount of compression force. The resultant
two different beakers. Sufficient quantity of
tablets were stored in container.
ethyl alcohol was taken. Required quantity
EVALUATION OF TABLETS:
of Paracetamol was dissolved in to beaker
The formulated tablets were
containing ethyl alcohol. Dissolve PVP in
evaluated for the following physicochemical
one beaker containing paracetamol solution
characteristics.
and HPMC in another beaker. There were
General
mixed thoroughly and kept in hot air oven at
tablets were assessed
90C. For evaporation of ethyl alcohol
appearance.
solvent.
The
Weight
mixtures
were
resultant
taken
drug-polymer
separately
in
appearance:
variation:
The
formulated
for its
general
Formulated
matrix
tablets were tested for weight uniformity.20
[Link]-2%was added to each of the
tablets were weighed
above mixtures and mixed uniformly. To
individually .from the collective weight,
this ethyl alcohol was added drop wise to get
average weight was calculated. Each tablet
the damp mass. This damp mass was passed
weight was then compared with average
through a sieve no: 16. The obtained
weight to ascertain whether it is within
granules were dried in hot air oven at
permissible limits or not.
[Link] obtained dried granules were
Hardness:
again passed through sieve no: 16. Now
determined by using Monsanto hardness
Magnesium sterate passed through sieve no:
tester. The lower plunger was placed in
120. Now Primogel (5%), the bolted
contact with the tablets and a zero reading
Magnesium sterate (2%), Talc-(2%) were
was taken. The plunger was then forced
added one by one to obtained granules and
against a spring by tuning a threaded bolt
mixed uniformly7.
until the tablet fractured .as the spring was
FORMULATION OF TABLETS:
4
Hardness
collectively and
of
tablets
was
�compressed a pointer rides along a gauge in
the barrel to indicate the force8.
Friability:
test
potassium dihydrogen phosphate in 200ml
apparatus was used to determine the
volumetric flask, add 44.5ml of 0.2M NaoH
friability of the tablets 20 pre-weight tablets
and then add water to final volume.
The
Roche
friability
were placed in the apparatus, which was
POTASSIUM DIHYDROGEN
given 100 revaluations. After which the
PHOSPHATE (O.2M): Dissolved 27.218
tablets were reweighed. The percentage
gms of potassium dihydrogen phosphate in
friability was calculated.
water and dilute with water to 1000ml.
ASSAY OF PARACETAMOL:
PROCEDURE:
Weigh
20
At first 900ml of dissolution
tablets .weighed accurately a quantity of
medium was placed in bath container. The
powder
of
tablet was introduced in to the bath
paracetamol and 50ml of 0.1M NaoH,
container, the paddle was rotated at 50RPM
diluted with 100ml of water, shacked for 15
up to 1 hr .5ml of sample solution was
minutes and add sufficient water to produce
withdrawn from batch container and again
[Link] and filtered and diluted 10ml
5ml of fresh dissolution medium was
of filtrate to 100ml with water. To 10ml of
replaced into the bath container to maintain
resulting solution add 10ml of 0.1 M NaoH
the constant volume.
equivalent
and
to
powdered
0.15gms
dilute to 100ml with water and measure the
Thus the sample withdrawn
absorbance of the resulting solution at about
within the specified time intervals such as
256nm.
5,10,15,20,25,30,35,40,45,50,55
DISSOLUTION TEST: Dissolution test
minutes. The obtained sample solution were
were carried out to determine the amount of
subjected to 1 in 10 dilutions by using
drug released during a specific period of
phosphate
time using I.P apparatus-I.
sample solutions optical densities were
REQUIREMENTS:
measured at maximum at about249nm
Phosphate buffer PH-7.8, Digital
buffer
[Link]
and
60
obtained
against the blank using spectrophotometer.
dissolution rate test apparatus of Campbell
The absorbance values were noted.
electronics.
PREPARATION OF PHASPHATE
BUFFER PH-7.8: Place 50ml of 0.2M
5
�TABLE: 1: The percentage drug release from the formulation:
Time (Min)
F1
F2
F3
18.1
10.1
12.6
13.5
10
23.3
13.6
23.7
14.5
15
35.1
22.1
32.4
23.3
20
40.7
28.1
45.3
35.5
25
47.4
37.6
55.2
43.4
30
53.5
52.6
62.6
56.5
35
54.8
54.4
68.4
77.1
40
57.3
56.6
76.8
78.1
45
62.5
60.3
80.4
84.5
50
64.9
70.9
81.5
85.1
F4
GRAPH: 1The percentage drug release from the formulation:
�TABLE: 2 Dissolution characteristics of Paracetamol dispersible tablet formulation:
Formulation
K value
R value
F1
0.0239
0.9871
F2
0.0238
0.9825
F3
0.0349
0.9870
F4
0.0422
0.9722
GRAPH: 2 Dissolution characteristics of Paracetamol dispersible tablet formulation
TABLE: 3 Hardness, Friability, Diameter & Thickness of the tablets formulation:
Formulation
Hardness(Kg/cm) Friability
Diameter(mm)
Thickness(mm)
F1
2.5%
0.4%
9.05
1.68
F2
3.4%
0.5%
9.06
1.84
F3
3.1%
0.75%
8.96
1.66
F4
3.5%
0.9%
9.04
1.78
�TABLE: 4 Disintegration and %Drug content of formulation:
Formulation
Disintegration
%Drug content
F1
4.9
98.6
F2
3.7
101.5
F3
2.5
96.7
F4
2.5
104.5
TABLE: 5 Weight variations of tablets of the formulation F1, F2, F3 and F4:
[Link]
Formulation-I
Formulation-II
Formulation-III
Formulation-IV
Weight
Percentage
Weight
Percentage
Weight of
Percentage
Weight of each
Percentage
deviation
each tablet
deviation
each tablet
deviation
tablet
deviation
each
of
tablet(mg)
of
(mg)
(mg)
(mg)
140
-5.6
154
4.5
150
2.3
152
-3.1
153
2.8
155
5.3
155
2.4
153
-2.6
148
-0.7
152
3.1
149
1.3
155
-1.8
152
3.4
156
3.7
160
1.9
152
2.2
150
-1.5
153
5.5
163
-3.1
150
3.1
155
2.4
150
3.8
162
4.1
149
2.9
153
3.5
149
-1.4
159
2.0
148
3.2
151
4.6
147
2.1
155
1.0
146
2.9
149
1.5
146
1.9
154
3.9
145
1.0
�RESULT AND DISCUSSION:
Then the resultant mixtures were
The main objective of the study is to prepare
the
Paracetamol
tablets.
subjected to granulation by using same wet
aqueous
granulation method and Primogel (5%) as
solubility. To improve its dissolution rate,
extra granular disintegrating agent in both
various disintegrating agents i.e. Potato
the formulations F3&F4 respectively. All
starch
the
Paracetamol
and
is
dispersible
having
Primogel
poor
and
different
remaining
process
was
same
as
hydrophobic polymers such as HPMC-4000
explained above for the preparation of
&PVP were employed.
tablets. The dissolution study revealed that
At first two formulations (F1&F2) were
among these two formulations, F4 shows
prepared by using Potato starch (10%), 5%
better release of drug than F3.
as inter
Finally it was concluded that formulation F4
9
and 5% as
in which Primogel (5%) used as extra
extra granular disintegrating agent .and F2
disintegrating agents, solid dispersion of
was prepared by using Primogel (5%) as
Paracetamol with PVP was made, showed
extra granular disintegrating agent. both F1
the better release of the drug than other three
& F2 are prepared by wet granulation
formulations F1, F2, F3.
method by using the same solvent ethyl
DISSOLUTION RATE: F1<F2<F3<F4:
alcohol as granulating fluid. and remaining
The prepared formulations were passed the
excipients that is PVP (2%) as binder,
evaluation test that is weight variations,
Magnesium sterate (2%), Talc-(2%) were
Percentage drug content, and disintegration,
common8. After dissolution study it was
Uniformity of dispersion, Hardness &
revealed that Primogel used formulation F2
friability as per I.P Limits.10
was showing better release of drug than
CONCLUSION:
granular disintegrating agent
potato starch used formulation F1.
When compared to potato starch, the
Later solid dispersion of Paracetamol and
Primogel is showing better increase in rate
hydrophilic polymer such as HPMC-4000,
of dissolution of prepared tablets. Out of
PVP were prepared in the same ratio 10:1
those three formulations F2, F3 and F4 in
were prepared by physical mixing.
which
Primogel
(5%)
used
as
extra
disintegrating agents was used.F4 was
9
�showing better increase in rate of dissolution
Regression Coefficient values: R2<R3<R4
of drug.F4 was prepared by solid dispersion
of Paracetamol with PVP.
First order rate constant values:
K2<K3<K4
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