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BUCCALDRUG DELIVERY SYSTEM
1
Seminar/Assignment-I
For the Subject
Drug Delivery System (MPH102T)
Submitted to
Drs. Kiran & Pallavi Patel Global
University (KPGU)
Guided by:
Dr. Meenaxi Patel
Professor
M Pharm. PhD.
KSP
Presented by:
Dhavalkumar Rathod
M. Pharm Sem-I
Pharmaceutics Branch
En. No. 2103313001
Krishna School of Pharmacy & Research (KSP)
Krishna Edu Campus ,Vadodara Mumbai NH#8, Varnama, Vadodara
DHAVALKUMAR RATHOD
2
CONTENT
Introduction
What Is BDDS (buccal drug delivery system)
Principle Of Mucoadhesion / bioadhesion
Mechanism of Mucoadhesion
Theory of Mucoadhesion
Advantages of BDDS
Limitation of BDDS
Formulations in BDDS
Evaluations of BDDS
Reference
DHAVALKUMAR RATHOD
3
INTRODUCTION
 Amogst the varios roures of the drug delivery, oral rute is most preferred to
the patient and clinical alike
 However Certain drugs have lack of efficacy due to decreased
bioavailability, GI intolerance, unpredictable and erratic absorption, first
pass metabolism or pre-systemic elimination of other potential route for
administration.
 So other absorptive mucosa are considered as potential sites for the drug
administration
 Bioadhesive drug delivery formulations were introduced in 1947 when gum
tragacanth was mixed with dental adhesive powder to apply penicillin to the
oral mucosa.
 The recent development in the drug delivery has intensified the investigation
of mucosal drug delivery. Such route includes oral, buccal, ocular, nasal and
pulmonary routes etc[1,2].
DHAVALKUMAR RATHOD
4
 The mucous has a rich blood supply and is relatively permeable
 The mucoadhesive drug delivery system includes the following:
1. Buccal drug delivery systems 2. Sublingual drug delivery systems
3. Rectal drug delivery systems 4. Vaginal drug delivery systems
5. Ocular drug delivery systems 6. Nasal drug delivery systems
Chitosan is one of the natural polymers, which is being widely used for making buccal
adhesive tab and patches
Chitosan is composed of glucosamine and N acetyl glucosamine which are also
constituent of mammalian tissue. It is non toxic, biocompatible and biodegradable
polymer. This polymer is considered for its film as well as matrix forming abilities.
Chitosan is also used as enzyme inhibitor as well as permeation enhancer properties[5].
DHAVALKUMAR RATHOD
5
WHAT IS BDDS
 the administration of drug via the buccal
mucosa(the lining of the cheek)to the systemic
circulation is called buccal drug delivery.
 Buccal mucosa lines the inner region of the check
 In biological terms, the drug/product is placed
between upper gums and check to treat local and
systematic condition.
DHAVALKUMAR RATHOD
6
PRINCIPLE OF
MUCOADHESION
 Before we start about mucoadhesion we should
know about the micosa, so lets get started
 The inner membrane into the mouth cavity
called mucosa, the inner cell lining is covered
with viscoelastic fluid, secreted by globet cells.
 This fluid composed of water and mucin (an
anionic polyelectrolyte). Other component may
be present like protein, lipid and
mucopolysaccharide.
 Mucosa’s thickness varies from 40-50 to 300
micro meter.
 Main role is protection and lubrication.
DHAVALKUMAR RATHOD
7
BIOADHESION / MUCOADHESION [3,4]
 ‘Bioadhesive’ is defined as a substance that is capable of interacting with
biological material and being retained on them or holding them together for
extended period of time.
 Bioadhesive are classified into three types.
 Bioadhesion between biological layers without involvement of artificial
materials. Cell diffusion and cell aggregation are good examples.
 Bioadhesion can be represented by cell adhesion into culture dishes or
adhesion to a variety of substances including metals, woods and other
synthetic materials.
 Adhesion of artificial substances to biological substrate such as adhesion of
polymer to skin or other soft tissue.
DHAVALKUMAR RATHOD
8
Mechanism of bioadhesion [4,5,6]:
For bioadhesion to occur, three stages are involved:
1. An intimate contact between a bioadhesive and a membrane either from a
good wetting of the bioadhesive and a membrane or from the swelling of
bioadhesive.
2. Penetration of the bio-adhesive into the tissue takes place.
3. Inter penetration of the chains of the
bioadhesive with mucous takes place.
Low chemical bonds can then settle.
The bonding between the mucus
and the biological substance occurs
chiefly through both physical and
chemical interactions results from
enlargement of the adhesive material and chemical bonds due to electrostatic
interaction, hydrophobic interactions, hydrogen bonding and dispersion forces.
DHAVALKUMAR RATHOD
9
Theories of Bioadhesion or Mucoadhesion [1,3,5,7,8]: Several
theories have been proposed to explain the fundamental mechanism of adhesion.
a) Wetting Theory: Wetting theory is predominantly applicable to liquid
bioadhesive systems and analyzes adhesive and contact behaviour in terms of a
liquid or a paste to spread over a biological system.
b) Diffusion Theory: According to this theory, the polymer chains and the mucus
mix to a sufficient depth to create a semi-permanent adhesive bond. The exact
depth to which the polymer chains penetrate the mucus depends on the diffusion
coefficient and the time of contact.
c) Electronic Theory: According to this theory, electronic transfer occurs upon
contact of an adhesive polymer and the mucus glycoprotein network because of
differences in their electronic structure. This result in the formulation of an
electronic double layer at the interface adhesion occurs due to attractive forces
across the double layer.
DHAVALKUMAR RATHOD
10
d) Fracture Theory: According to Fracture theory of adhesion is related to
separation of two surfaces after adhesion.
e) Adsorption Theory: According to this theory, after an initial contact between
two surfaces, the materials adhere because of surface forces acting between the
atoms in the two surfaces. Two types of chemical bonds such as primary covalent
(permanent) and secondary chemical bonds (including electrostatic forces,
vander-waals forces and hydrogen and hydrophobic bonds) are involved in the
adsorption process.
DHAVALKUMAR RATHOD
11
ADVANTAGES OF BDDS [9]
Drug administration via the buccoadhesive drug delivery offers several advantages such
as:
1. Drug is easily administered and extinction of therapy in emergency can be facilitated.
2. Drug release for prolonged period of time.
3. In unconscious and trauma patient’s drug can be administered.
4. Drugs bypass first pass metabolism so increases bioavailability.
5. Some drugs that are unstable in acidic environment of stomach can be administered
by buccal delivery.
6. Drug absorption by the passive diffusion.
7. Flexibility in physical state, shape, size and surface.
8. Maximized absorption rate due to close contact with the absorbing membrane
(mucosa).
9. Rapid onset of action.
DHAVALKUMAR RATHOD
12
10. Drug can easily removed in case of toxicity and reduction in dose can be achieved in
case of discomfort.
11. Administration of drug witch have short half life
12. Improved patient compliance due to the elimination of associated pain with
injection; administration of drugs in unconscious or incapacitate patient; covinience of
administration of drug in compare to injection or oral route.
DHAVALKUMAR RATHOD
13
LIMITATION OF BDDS [10]
There are some limitations of buccal drug delivery system such as
1. Drugs which are unstable at buccal pH cannot be administered.
2. Drugs which have a bitter taste or unpleasant taste or an obnoxious odor or irritate the
mucosa cannot be administered by this route.
3. Drug required with small dose can only be administered.
4. Those drugs which are absorbed by passive diffusion can only be administered by this
route.
5. Eating and drinking may become restricted.
6. Continuous secretion of saliva 0.5-2 l/day leads to subsequent dilution of the drug.
7. Over hydration
8. By mistake tablet can be swallowed.
9. Low permeability of the buccal membrane; specifically when compared to the
sublingual membrane.
DHAVALKUMAR RATHOD
14
10. Smaller surface area. The total surface area of membranes of the oral cavity available
for drug absorption is 170 cm2 of which 50 cm2 represents non-keratinized tissues,
including the buccal membrane.
11. Swallowing of saliva can also potentially leads to the lose of dissolved or suspended
drug, and ultimatimately, the involuntarily removal of dosage form.
DHAVALKUMAR RATHOD
15
FORMULATIONS IN BDDS [11]
Novel buccal dosage forms: The novel type buccal dosage forms include buccal
adhesive tablets, patches, films, semisolids (ointments and gels) and powders.
A. Solid buccal adhesive dosage form
 Buccal mucoadhesive tablets: Buccal mucoadhesive tablets are dry dosage
forms that have to be moistened prior to placing in contact with buccal mucosa.
Example: a double layer tablet, consisting of adhesive matrix layer of HPC and
polyacrylic acid with an inner core of cocoa butter containing insulin and a
penetration enhancer (sodium glycocholate).
 Powders: HPC and beclomethasone in powder form when sprayed on to the oral
mucosa of rats, a significant increase in the residence time relative to an oral
solution is seen, and 2.5% of beclomethasone is retained on buccal mucosa for
over 4 hrs.
DHAVALKUMAR RATHOD
16
 Bioadhesive lozenges: a slow release Bioadhesive lozenges offer the potential for
prolonged drug release with improved patient compliance.
B. Semisolid dosage form
 Patches and Films: Buccal patches consists of two laminates, with an aqueous
solution of the adhesive polymer being cast onto an impermeable backing sheet,
which is then cut into the required oval shape. A novel mucosal adhesive film
called “Zilactin” - consisting of an alcoholic solution of HPC and three organic
acids. The film which is applied to the oral mucosal can be retained in place for
at least 12 hrs even when it is challenged with fluids.
 Ointments and Gels: Bioadhesive gels or ointments have less patient
acceptability than solid bioadhesive dosage forms, and most of the dosage forms
are used only for localized drug therapy within the oral cavity. One of the original
oral mucoadhesive delivery systems -“orabase”- consists of finely ground pectin,
gelatin and NaCMC dispersed in a poly (ethylene) and a mineral oil gel base,
which can be maintained at its site of application for 15-150 mins.
DHAVALKUMAR RATHOD
17
 Medicated chewing gum: although medicated chewing gum pose difficulties in
regulation of administration of dose, they still have some advantages as drug
delivery devices, particularly in the treatment of disease of the oral cavity and in
nicotine replacement therapy. Some commercial product are available in market.
 Adhesive gel: various adhesive gel may be used to deliver drug via the buccal
mucosa and allow sustained release.
C. liquid dosage form: they are solutions or suspensions of drugs in suitable
aqueous vehicle.
 Such types of dosage forms are usually employed to exert local action into the
oral cavity and several antibacterial mouthwashes and mouthfreheners are
commercially available for this purpose.
 The limitation of the product is they deliver uncontrolled amount of the drug
into oral cavity.
DHAVALKUMAR RATHOD
18
EVALUATIONS OF BDDS [12,13]
 Thickness: the thickness of the buccal tablet was determine by using digital
micrometer.
 Ten individual tablet from each batch were used and the results averaged.
 Weight variation: 20 tablets were weight by electronic balance and average
value were calculated.
 Hardness: conducted for 3 tab from each batch using Monsanto hardness tester
and average value is calculated.
 Disintegration test (USP NF 2004): only use for buccal drug which does not
having backing effect.
 Six tablets were taken randomly from each batch and placed in USP
disintegration apparatus.
 Apparatus was run for 4 hrs., and basket was lift from fluid, observe whether all
of the tablets have disintegrate.
DHAVALKUMAR RATHOD
19
 Swelling index: the extent of swelling can be measured by in terms of %weight
gain by the dosage form.
 The swelling index is calculated by using following formula,
S.I=Wt-Wo
Wo
where, S.I= swelling index
Wt= weight of tablet at time t
Wo= weight of tablet before placing into beaker
 viscosity: the viscosity of the solution used for buccal films were determined by
Brookfield viscometer.
 Moisture absorbance studies for buccal patches: this test give an indication
about the relative moisture absorption capacity of polymers and an idea wether
the buccal patches maintain their integrity after absorption of moisture.
 %moisture absorbed= final weight - initial weight
initial weight 100
DHAVALKUMAR RATHOD
20
REFERENCES
1. Jain NK. Controlled and Novel Drug Delivery, 1st edition, published by CBS Publishers and
Distributors, New Delhi. 1997; 52-81.
2. Patel KV, Patel ND, Dodiya HD, Shelat PK. Buccal bioadhesive drug delivery system: an
overview. Ind. J. of Pharma. & Bio. Arch. 2011; 2(2): 600-609.
3. Nazila SM, Montakarn C, Thomas PJ. The use of mucoadhesive polymers in buccal drug
delivery. Advanced Drug Delivery Reviews. 2005; 57:1666– 1691.
4. Boddupalli BM, Mohammad ZNK, Nath RA, Banji D. mucoadhesive drug delivery system an
overview. J. Adv. Pharm. Tech. Res. 2010; 1(4): 381-387.
5. Gandhi SD, Priyanka RP, Rahul U, Tambawala T, Shah MA. Mucoadhesive drug delivery
systems-An unusual maneuver for site specific drug delivery system. An Int. J .Pharm. Sci. ISSN:
0976- 7908: 851-871.
6. Pharmaceutics the science of dosage form Design 2nd edition edited by M. E. Aulton. Published
by Harcourt publishers Limited. 2002; 198-200.
DHAVALKUMAR RATHOD
21
7. Nazila SM, Montakarn C, Thomas PJ. The use of mucoadhesive polymers in buccal drug delivery.
Advanced Drug Delivery Reviews. 2005; 57:1666– 1691.
8. Satheesh Madhav NV, Ashok KS, Pragati S, Kuldeep S. Orotransmucosal drug delivery systems: A
review. Journal of Controlled Release. 2009; 140: 2–11
9. Satyabrata B, Ellaiah P, Choudhury R, Murthy KVR, Bibhutibhusan P and Kumar MS, Design and
evaluation of Methotrexate buccal mucoadhesive patches, Inter. J. Pharm. Biomed.Sci., 2010, 1(2), 31-
36.
10. Patil BS, Tate SS, Kulkarni U, Hariprasanna RC and Wadageri GV. Development and In-vitro evaluation
of mucoadhesive buccal tablets of Tizanidine hydrochloride using natural polymer Xanthan gum, Inter.
J. Pharm. Sci. Rev. and Res., 2011, 8(2), 140-146.
11. Shojaei Amir H, Buccal Mucosa As A Route For Systemic Drug Delivery: A Review;J Pharm Pharmaceut
Sci (www.ualberta.ca/~csps) 1998;1 (1):15-30
12. Evaluation of buccal drug delivery system (slideshare.net)
13. Buccal drug delivery system (slideshare.net)
DHAVALKUMAR RATHOD
THANK YOU....
DHAVALKUMAR RATHOD 22

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2103313001_dhavalkumar H rathod_MPH102T.pptx

  • 1. BUCCALDRUG DELIVERY SYSTEM 1 Seminar/Assignment-I For the Subject Drug Delivery System (MPH102T) Submitted to Drs. Kiran & Pallavi Patel Global University (KPGU) Guided by: Dr. Meenaxi Patel Professor M Pharm. PhD. KSP Presented by: Dhavalkumar Rathod M. Pharm Sem-I Pharmaceutics Branch En. No. 2103313001 Krishna School of Pharmacy & Research (KSP) Krishna Edu Campus ,Vadodara Mumbai NH#8, Varnama, Vadodara DHAVALKUMAR RATHOD
  • 2. 2 CONTENT Introduction What Is BDDS (buccal drug delivery system) Principle Of Mucoadhesion / bioadhesion Mechanism of Mucoadhesion Theory of Mucoadhesion Advantages of BDDS Limitation of BDDS Formulations in BDDS Evaluations of BDDS Reference DHAVALKUMAR RATHOD
  • 3. 3 INTRODUCTION  Amogst the varios roures of the drug delivery, oral rute is most preferred to the patient and clinical alike  However Certain drugs have lack of efficacy due to decreased bioavailability, GI intolerance, unpredictable and erratic absorption, first pass metabolism or pre-systemic elimination of other potential route for administration.  So other absorptive mucosa are considered as potential sites for the drug administration  Bioadhesive drug delivery formulations were introduced in 1947 when gum tragacanth was mixed with dental adhesive powder to apply penicillin to the oral mucosa.  The recent development in the drug delivery has intensified the investigation of mucosal drug delivery. Such route includes oral, buccal, ocular, nasal and pulmonary routes etc[1,2]. DHAVALKUMAR RATHOD
  • 4. 4  The mucous has a rich blood supply and is relatively permeable  The mucoadhesive drug delivery system includes the following: 1. Buccal drug delivery systems 2. Sublingual drug delivery systems 3. Rectal drug delivery systems 4. Vaginal drug delivery systems 5. Ocular drug delivery systems 6. Nasal drug delivery systems Chitosan is one of the natural polymers, which is being widely used for making buccal adhesive tab and patches Chitosan is composed of glucosamine and N acetyl glucosamine which are also constituent of mammalian tissue. It is non toxic, biocompatible and biodegradable polymer. This polymer is considered for its film as well as matrix forming abilities. Chitosan is also used as enzyme inhibitor as well as permeation enhancer properties[5]. DHAVALKUMAR RATHOD
  • 5. 5 WHAT IS BDDS  the administration of drug via the buccal mucosa(the lining of the cheek)to the systemic circulation is called buccal drug delivery.  Buccal mucosa lines the inner region of the check  In biological terms, the drug/product is placed between upper gums and check to treat local and systematic condition. DHAVALKUMAR RATHOD
  • 6. 6 PRINCIPLE OF MUCOADHESION  Before we start about mucoadhesion we should know about the micosa, so lets get started  The inner membrane into the mouth cavity called mucosa, the inner cell lining is covered with viscoelastic fluid, secreted by globet cells.  This fluid composed of water and mucin (an anionic polyelectrolyte). Other component may be present like protein, lipid and mucopolysaccharide.  Mucosa’s thickness varies from 40-50 to 300 micro meter.  Main role is protection and lubrication. DHAVALKUMAR RATHOD
  • 7. 7 BIOADHESION / MUCOADHESION [3,4]  ‘Bioadhesive’ is defined as a substance that is capable of interacting with biological material and being retained on them or holding them together for extended period of time.  Bioadhesive are classified into three types.  Bioadhesion between biological layers without involvement of artificial materials. Cell diffusion and cell aggregation are good examples.  Bioadhesion can be represented by cell adhesion into culture dishes or adhesion to a variety of substances including metals, woods and other synthetic materials.  Adhesion of artificial substances to biological substrate such as adhesion of polymer to skin or other soft tissue. DHAVALKUMAR RATHOD
  • 8. 8 Mechanism of bioadhesion [4,5,6]: For bioadhesion to occur, three stages are involved: 1. An intimate contact between a bioadhesive and a membrane either from a good wetting of the bioadhesive and a membrane or from the swelling of bioadhesive. 2. Penetration of the bio-adhesive into the tissue takes place. 3. Inter penetration of the chains of the bioadhesive with mucous takes place. Low chemical bonds can then settle. The bonding between the mucus and the biological substance occurs chiefly through both physical and chemical interactions results from enlargement of the adhesive material and chemical bonds due to electrostatic interaction, hydrophobic interactions, hydrogen bonding and dispersion forces. DHAVALKUMAR RATHOD
  • 9. 9 Theories of Bioadhesion or Mucoadhesion [1,3,5,7,8]: Several theories have been proposed to explain the fundamental mechanism of adhesion. a) Wetting Theory: Wetting theory is predominantly applicable to liquid bioadhesive systems and analyzes adhesive and contact behaviour in terms of a liquid or a paste to spread over a biological system. b) Diffusion Theory: According to this theory, the polymer chains and the mucus mix to a sufficient depth to create a semi-permanent adhesive bond. The exact depth to which the polymer chains penetrate the mucus depends on the diffusion coefficient and the time of contact. c) Electronic Theory: According to this theory, electronic transfer occurs upon contact of an adhesive polymer and the mucus glycoprotein network because of differences in their electronic structure. This result in the formulation of an electronic double layer at the interface adhesion occurs due to attractive forces across the double layer. DHAVALKUMAR RATHOD
  • 10. 10 d) Fracture Theory: According to Fracture theory of adhesion is related to separation of two surfaces after adhesion. e) Adsorption Theory: According to this theory, after an initial contact between two surfaces, the materials adhere because of surface forces acting between the atoms in the two surfaces. Two types of chemical bonds such as primary covalent (permanent) and secondary chemical bonds (including electrostatic forces, vander-waals forces and hydrogen and hydrophobic bonds) are involved in the adsorption process. DHAVALKUMAR RATHOD
  • 11. 11 ADVANTAGES OF BDDS [9] Drug administration via the buccoadhesive drug delivery offers several advantages such as: 1. Drug is easily administered and extinction of therapy in emergency can be facilitated. 2. Drug release for prolonged period of time. 3. In unconscious and trauma patient’s drug can be administered. 4. Drugs bypass first pass metabolism so increases bioavailability. 5. Some drugs that are unstable in acidic environment of stomach can be administered by buccal delivery. 6. Drug absorption by the passive diffusion. 7. Flexibility in physical state, shape, size and surface. 8. Maximized absorption rate due to close contact with the absorbing membrane (mucosa). 9. Rapid onset of action. DHAVALKUMAR RATHOD
  • 12. 12 10. Drug can easily removed in case of toxicity and reduction in dose can be achieved in case of discomfort. 11. Administration of drug witch have short half life 12. Improved patient compliance due to the elimination of associated pain with injection; administration of drugs in unconscious or incapacitate patient; covinience of administration of drug in compare to injection or oral route. DHAVALKUMAR RATHOD
  • 13. 13 LIMITATION OF BDDS [10] There are some limitations of buccal drug delivery system such as 1. Drugs which are unstable at buccal pH cannot be administered. 2. Drugs which have a bitter taste or unpleasant taste or an obnoxious odor or irritate the mucosa cannot be administered by this route. 3. Drug required with small dose can only be administered. 4. Those drugs which are absorbed by passive diffusion can only be administered by this route. 5. Eating and drinking may become restricted. 6. Continuous secretion of saliva 0.5-2 l/day leads to subsequent dilution of the drug. 7. Over hydration 8. By mistake tablet can be swallowed. 9. Low permeability of the buccal membrane; specifically when compared to the sublingual membrane. DHAVALKUMAR RATHOD
  • 14. 14 10. Smaller surface area. The total surface area of membranes of the oral cavity available for drug absorption is 170 cm2 of which 50 cm2 represents non-keratinized tissues, including the buccal membrane. 11. Swallowing of saliva can also potentially leads to the lose of dissolved or suspended drug, and ultimatimately, the involuntarily removal of dosage form. DHAVALKUMAR RATHOD
  • 15. 15 FORMULATIONS IN BDDS [11] Novel buccal dosage forms: The novel type buccal dosage forms include buccal adhesive tablets, patches, films, semisolids (ointments and gels) and powders. A. Solid buccal adhesive dosage form  Buccal mucoadhesive tablets: Buccal mucoadhesive tablets are dry dosage forms that have to be moistened prior to placing in contact with buccal mucosa. Example: a double layer tablet, consisting of adhesive matrix layer of HPC and polyacrylic acid with an inner core of cocoa butter containing insulin and a penetration enhancer (sodium glycocholate).  Powders: HPC and beclomethasone in powder form when sprayed on to the oral mucosa of rats, a significant increase in the residence time relative to an oral solution is seen, and 2.5% of beclomethasone is retained on buccal mucosa for over 4 hrs. DHAVALKUMAR RATHOD
  • 16. 16  Bioadhesive lozenges: a slow release Bioadhesive lozenges offer the potential for prolonged drug release with improved patient compliance. B. Semisolid dosage form  Patches and Films: Buccal patches consists of two laminates, with an aqueous solution of the adhesive polymer being cast onto an impermeable backing sheet, which is then cut into the required oval shape. A novel mucosal adhesive film called “Zilactin” - consisting of an alcoholic solution of HPC and three organic acids. The film which is applied to the oral mucosal can be retained in place for at least 12 hrs even when it is challenged with fluids.  Ointments and Gels: Bioadhesive gels or ointments have less patient acceptability than solid bioadhesive dosage forms, and most of the dosage forms are used only for localized drug therapy within the oral cavity. One of the original oral mucoadhesive delivery systems -“orabase”- consists of finely ground pectin, gelatin and NaCMC dispersed in a poly (ethylene) and a mineral oil gel base, which can be maintained at its site of application for 15-150 mins. DHAVALKUMAR RATHOD
  • 17. 17  Medicated chewing gum: although medicated chewing gum pose difficulties in regulation of administration of dose, they still have some advantages as drug delivery devices, particularly in the treatment of disease of the oral cavity and in nicotine replacement therapy. Some commercial product are available in market.  Adhesive gel: various adhesive gel may be used to deliver drug via the buccal mucosa and allow sustained release. C. liquid dosage form: they are solutions or suspensions of drugs in suitable aqueous vehicle.  Such types of dosage forms are usually employed to exert local action into the oral cavity and several antibacterial mouthwashes and mouthfreheners are commercially available for this purpose.  The limitation of the product is they deliver uncontrolled amount of the drug into oral cavity. DHAVALKUMAR RATHOD
  • 18. 18 EVALUATIONS OF BDDS [12,13]  Thickness: the thickness of the buccal tablet was determine by using digital micrometer.  Ten individual tablet from each batch were used and the results averaged.  Weight variation: 20 tablets were weight by electronic balance and average value were calculated.  Hardness: conducted for 3 tab from each batch using Monsanto hardness tester and average value is calculated.  Disintegration test (USP NF 2004): only use for buccal drug which does not having backing effect.  Six tablets were taken randomly from each batch and placed in USP disintegration apparatus.  Apparatus was run for 4 hrs., and basket was lift from fluid, observe whether all of the tablets have disintegrate. DHAVALKUMAR RATHOD
  • 19. 19  Swelling index: the extent of swelling can be measured by in terms of %weight gain by the dosage form.  The swelling index is calculated by using following formula, S.I=Wt-Wo Wo where, S.I= swelling index Wt= weight of tablet at time t Wo= weight of tablet before placing into beaker  viscosity: the viscosity of the solution used for buccal films were determined by Brookfield viscometer.  Moisture absorbance studies for buccal patches: this test give an indication about the relative moisture absorption capacity of polymers and an idea wether the buccal patches maintain their integrity after absorption of moisture.  %moisture absorbed= final weight - initial weight initial weight 100 DHAVALKUMAR RATHOD
  • 20. 20 REFERENCES 1. Jain NK. Controlled and Novel Drug Delivery, 1st edition, published by CBS Publishers and Distributors, New Delhi. 1997; 52-81. 2. Patel KV, Patel ND, Dodiya HD, Shelat PK. Buccal bioadhesive drug delivery system: an overview. Ind. J. of Pharma. & Bio. Arch. 2011; 2(2): 600-609. 3. Nazila SM, Montakarn C, Thomas PJ. The use of mucoadhesive polymers in buccal drug delivery. Advanced Drug Delivery Reviews. 2005; 57:1666– 1691. 4. Boddupalli BM, Mohammad ZNK, Nath RA, Banji D. mucoadhesive drug delivery system an overview. J. Adv. Pharm. Tech. Res. 2010; 1(4): 381-387. 5. Gandhi SD, Priyanka RP, Rahul U, Tambawala T, Shah MA. Mucoadhesive drug delivery systems-An unusual maneuver for site specific drug delivery system. An Int. J .Pharm. Sci. ISSN: 0976- 7908: 851-871. 6. Pharmaceutics the science of dosage form Design 2nd edition edited by M. E. Aulton. Published by Harcourt publishers Limited. 2002; 198-200. DHAVALKUMAR RATHOD
  • 21. 21 7. Nazila SM, Montakarn C, Thomas PJ. The use of mucoadhesive polymers in buccal drug delivery. Advanced Drug Delivery Reviews. 2005; 57:1666– 1691. 8. Satheesh Madhav NV, Ashok KS, Pragati S, Kuldeep S. Orotransmucosal drug delivery systems: A review. Journal of Controlled Release. 2009; 140: 2–11 9. Satyabrata B, Ellaiah P, Choudhury R, Murthy KVR, Bibhutibhusan P and Kumar MS, Design and evaluation of Methotrexate buccal mucoadhesive patches, Inter. J. Pharm. Biomed.Sci., 2010, 1(2), 31- 36. 10. Patil BS, Tate SS, Kulkarni U, Hariprasanna RC and Wadageri GV. Development and In-vitro evaluation of mucoadhesive buccal tablets of Tizanidine hydrochloride using natural polymer Xanthan gum, Inter. J. Pharm. Sci. Rev. and Res., 2011, 8(2), 140-146. 11. Shojaei Amir H, Buccal Mucosa As A Route For Systemic Drug Delivery: A Review;J Pharm Pharmaceut Sci (www.ualberta.ca/~csps) 1998;1 (1):15-30 12. Evaluation of buccal drug delivery system (slideshare.net) 13. Buccal drug delivery system (slideshare.net) DHAVALKUMAR RATHOD