Int J App Pharm, Vol 13, Issue 6, 2021, 66-74Review Article

AN ASSESSMENT ON BUCCAL MUCOADHESIVE DRUG DELIVERY SYSTEM

LEELA LAKSHMI V.¹, UMASHANKAR M. S.^2*, ALAGUSUNDARAM M.¹

¹Department of Pharmaceutics, Jagan’s College of Pharmacy, Nellore, Andhra Pradesh, India, ²Department of Pharmaceutics, SRM College of Pharmacy, Chennai, India
Email: umashans@srmist.edu.in

Received: 27 Jul 2021, Revised and Accepted: 14 Sep 2021

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ABSTRACT

Buccal drug delivery system (BDDS) has won a variety of exposure and traction as it possesses plenty of advantages and benefits as evaluate to different mucosal drug delivery systems. Buccal path for systemic drug delivery, the use of mucoadhesive polymers twill significantly increase the efficacy of many tablets, has been of outstanding interest over the previous couple of decades. This article affords a precise of BDDS mechanisms, consisting of a composition of the oral mucosa, delivery mechanism, numerous forms of BDDS, formulation, assessment and application of BDDS. Additionally, this text affords a precis over the patents, advertised products and destiny factors of BDDS. In this evaluation article, we've got tried to assemble the maximum significant reports (1988 to 2021) of formulation, assessment, application, patents of BDDS. This review will help pharmaceutical researchers to clarify the potential of BDDS to overcome the various existing drug delivery dispute like the efficiency of absorption, permeability and bioavailability of drugs.

Keywords: Buccal drug delivery, mucoadhesive polymer, Formulation, Evaluation, Application, Patents

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© 2021 The Authors. Published by Innovare Academic Sciences Pvt Ltd. This is an open access article under the CC BY license (https://creativecommons.org/licenses/by/4.0/)
DOI: https://dx.doi.org/10.22159/ijap.2021v13i6.42760. Journal homepage: https://innovareacademics.in/journals/index.php/ijap

INTRODUCTION

Advancement and the progress made by the pharmaceutical industry that greatly contributed to treat the diseases, thus improving the quality of life [1]. With the passage of time researchers who are involved in the drug development industries focus on the alternative routes of administration of potentially capable pharmaceutical products and as well as to overcome defects that are associated with the oral route of administration. Though oral route is the most preferred route for the administration of major drugs, but it possesses certain drawbacks such as, the first pass metabolism in the liver, the local GI and enzymatic degradation inside the GI tracts [2].

In order to overcome the above mention drawbacks, one such strategy was used that is to deliver the drug through the alternative route such as intranasal, sublingual, Buccal, pulmonary or transdermal drug delivery systems [3]. Transmucosal method of drug transmission comprise of the mucosal lining of mouth, eye, vagina, rectum and nasal cavity which provides potential benefits over oral systemic drug delivery system. These features include the ability to bypass the first-pass metabolism, avoid the pre-elimination of the drug in the GI tack and dependence on the drug characters, it shows better enzymatic flora for the drug absorption [4].

Among the different mucosal pathways, the buccal mucosa has excellent accessibility, stretching of smooth muscle and relatively immobile mucosa; thus, this route of administration is suitable for controlled release of drugs from the dosage forms. By eliminating first-pass metabolism and enzymatic degradation owing to GI microbial flora, the oral mucosal drug delivery method is extensively applicable as a unique site for drug administration for immediate and controlled release action. Local and systemic action is provided through the oral mucosal medication delivery system. In addition, it exhibit great patient compliance as compare to other non-oral mucosal methods of drug administration. The Buccal drug delivery avoids acidolysis of the drug in GI system and bypasses the first-pass hepatic metabolism, which results the high bioavailability of the drug [5].

This article summarizes the advantage and disadvantages, application, evaluation, mechanism of the drug penetration, patents and marketed available pelletized drug delivery system. And also it will highlight the important terms and descriptions in the advantages, disadvantages, application, evaluation, mechanism of the drug penetration, patents and marketed available pelletized drug delivery system.

This review was conducted using Google search terms such as buccal mucoadhesive drug delivery system and articles relating to its formulation, evaluation, application and patents, which were collected from standard journals such as science direct, pubmed and scopus indexed journals.

Physiological, anatomical features of the oral cavity

The lips, hard palate (the bony front portion of the roof of the mouth), soft palate (the muscular back portion of the roof of the mouth), retromolar trigone (the area behind the wisdom teeth), front two-thirds of the tongue, gingiva (gums), buccal mucosa (the inner lining of the lips and cheeks), and floor of the mouth under the tongue are all parts of the oral cavity. In the following fig. 1 and table 1, it show the composition of the oral cavity and its respective role in drug penetration.

Fig. 1: (A) Anatomy of oral mucosa; (B) Transverse section of oral mucosa [2]

Table 1: Composition of the oral cavity and mechanism of permeation enhancers

S. No.	Composition of the oral cavity and its role	Thickness	Drug permeation enhancement mechanism	Reference
1.	Epithelium Layer as shown in fig. 1 possesses two type Non keratinized epithelium It covers the soft palate, ventral surface of the tongue, inner lip, floor of the mount and inner cheeks Keratinized epithelium It covers the gingiva, dorsal surface of the tongue and hard palate. Role: Protective layer	500-800 µm	The pores of the protective layer can be enhanced by the addition of surfactant (Anionic: Sodium lauryl sulfate Cationic: Cetyl pyridinium chloride Nonionic: Poloxamer, Brij, Span, Myrj, Tween) by the agitation of intercellular Lipids and its protein (keratin) domain structure	[2, 3]
2.	Basement Membrane It forms a distinct layer between the epithelium and connective layer Role: Provides the adherence between the epithelium and connective tissue and provide mechanical support to the epithelium layer	1-2 µm	Addition of positively charged polymers like Chitosan, Cationic compounds like Poly-L-arginine, L-lysine will show an Ionic interaction with the negative charge on the mucosal surface will paves the way to the enhancement of drug through the mucosa	[4, 5]
3.	Connective Tissue It consists of lamina propria and submucosa layer. The lamina propria consists of collagen fibers, supporting layers, blood vessels and smooth muscles. Role: Responsible for the blood supply to the oral cavity. The Buccal artery like facial artery and infraorbital artery are the predominant source of blood supply to cheek lining in the Buccal cavity. Which will be responsible for enhancement of drug penetration due to the predominant source of blood supply	150-500 µm	By adding a surfactant, Cyclodextrins, Chelators, anionic and cationic polymers may interfere with Ca+ions, negative charge on the mucosal surface will leads to enhancement of drug permeability.	[6, 7]
4.	Mucus Gel like secretion which was translucent and continuous; Composition Water insoluble glycoprotein(Mucin): 1-5% Water: 95-99% Proteins, enzymes, electrolytes and nucleic acids. Role: It is a visco-elastic hydrogel which act as a protective layer to the cell below.	Buccal (Nonkeratinized)-500-600 µm with 2.40 ml/min/cm2 Sublingual (Nonkeratinized)-100-200 µm with 0.97 ml/min/cm2 Gingival (keratinized)-200 µm with 1.47 ml/min/cm2 Palatal (Keratinized)-250 µm with 0.89 ml/min/cm2	By adding anionic and cationic surfactant, bile salts (Sodium glycocholate, Sodium tauro deoxycholate, Sodium tauro cholate), Fatty acids (Oleic acid, Caprylic acid, Lauric acid), Cyclodextrin, Chelator (EDTA, Citric acid, Sodium salicylate, Methoxy salicylates) will either increase the fluidity of phospholipid domains or agitate the intercellular Lipids and its protein(keratin) domain structure	[8, 9]
5	Saliva Role: Protective fluid, Source of mineralization for the tooth enamel, Hydrate the oral drug delivery system	viscosity-1.05 cP and 1.29 cP, respectively	Drug Permeation enhancement mechanism: will either increase the fluidity of phospholipid domains by adding bile salt, fatty acids to the BDDS	[10, 11]

Fig. 2: (a) Buccal mucoadhesive tablet [5]; (b) Administration sites of buccal mucoadhesive tablets [6]; (C) Schematic representation of bioadhesion mechanism [8]; Buccal mucoadhesive films [9]; (D) Contact of Bdds to buccal mucosa [8]; (E) Buccal patch [9]; (F) Scheme of route of permeation from BDDS through buccal mucosa [3]

Transport mechanism

Drug transport mechanism through the Buccal drug delivery is carried out by two mechanisms i.e. transcellular (intracellular) and paracellular (intercellular) as shown in fig. 2 (F). Paracellular route of permeation of the drug across the buccal epithelium is carried out through the passive diffusion. It is the most common route of transportation of various drug especially for the hydrophilic drugs i.e. protein or peptide which undergoes rapid dissolution in the aqueous fluid present in the intercellular spaces. For example caffeine is the drug which undergoes absorption via paracellular route and more often used as a marker for the paracellular absorption [9]. Whereas in case of trancellular pathway drug is penetrated through the cells i.e. by transferring the drug through the lipodial barrier i.e. cell membrane followed by the hydrophilic content of the series cell in order to reach the cytoplasmic content of the next cell. Example of the drug that penetrates via transcellular route of permeation is fentanyl [10]. Certain drugs may penetrate by using both the pathways which is possible only when the drug exhibit proper hydrophilic and lipophilic balance with a slight predominance of hydrophilic property. These drugs undergoes faster penetration, apart from these pathways alternative pathway like carrier mediated transport also play an major role for the penetration of the certain drugs across the membrane [11]. The major factors that influencing the penetration and bioavailability of the drug through the Buccal drug delivery includes permeability and thickness of the epithelium, blood supply, metabolic activity, saliva and mucous, species difference and route of mechanism [12].

Novel buccal dosage formulations

Table 2: Novel buccal dosage formulations

S. No.	Dosage form	Description	Example	Reference
1.	Buccal mucoadhesive tablets as shown in fig. 2(A,B)	Dry dosage form Must be moistened before use prior coming in contact with the Buccal mucosa	Double layer tablet	[13, 14]
2.	Buccal patches as shown in fig. 2(E) It is of two types Reservoir type Matrix type	Consists of two laminates with adhesive polymer(aqueous form) which is glued over the backing sheet When it comes in contact with the mucosal membrane results in the formation of the mucoadhesive bond between the adhesive polymer and the mucosal polymer which is known as bioadhesion. Mechanism of bioadhesion can be explained by theories of bioadhesion which include electronic, adsorption, wetting, diffusion and fracture theory. Formation of mucoadhesive bond is carried out by three major steps as shown in fig. 2 Wetting and swelling of polymer (contact stage). Interpenetration between the adhesive polymer and mucosal membrane (mucin). Chemical bond formation (consolidation stage).	Zilactin	[15, 16]
3.	Semisolid dosage form(ointments and gel)	Less patient compliance Exhibit localized action which is limited to oral cavity	Orabase	[17]
4.	Powders	It increase the residence time of the drug in oral mucosa	Hydroxypropyl cellulose and beclomethasone combination	[18, 19]
5.	Sprays	It is made up of Mucoadhesive suspension, especially used through nasal route	-	[17-19]

Advantages and disadvantages of Buccal drug delivery system

Table 3: advantages and disadvantages of the buccal drug delivery system

Advantages	Disadvantages	Reference
In contrast to the other mucosal tissues, the buccal mucosa is relatively permeable and has a good blood supply. Bypass first pass metabolism Exhibits localized therapy Many medications would work better because they have a longer contact time with the mucosa. Patient acceptance is high as compared to other non-oral drug delivery methods. Lower administration frequency may result from increased residence time combined with controlled API release. API localization at the disease site can also result in substantial cost savings and a reduction in dose-related side effects. The formulation stays longer at the delivery site as a result of adhesion and personal touch, improving API bioavailability while using lower API concentrations for disease care. Buccal drug delivery removes the harsh environmental conditions that occur in oral drug delivery. It is a passive drug absorption mechanism that does not need any activation. In comparison to rectal or transdermal pathways, the presence of saliva guarantees a comparatively large volume of water for drug dissolution. Provides a various different ways to administer hormones, narcotic analgesics, steroids, enzymes, cardiovascular agents, and other medications. It allows for localized tissue permeability alteration, protease inhibition, and immunogenic response reduction. As a result, therapeutic agents such as peptides, proteins, and ionized species can be easily administered.	The total surface area of the oral cavity membranes usable for drug absorption is 170 cm2, with non-keratinized tissues, such as the buccal membrane, accounting for 50 cm2. The mucosa's barrier properties. The medication is diluted as a result of the continuous secretion of saliva (0.5-2 l/day). The risk of choking if the delivery system is swallowed involuntarily is a concern. Swallowing saliva may result in the loss of dissolved or suspended drugs, as well as the inadvertent removal of the dosage type.	[ 16-20]

Formulation of buccal drug delivery

Table 4: Types of excipients and their role in the buccal drug delivery system

S. No.	Excipient	Role	Example	Reference
1.	Mucoadhesive polymer	Mucoadhesives are synthetic or natural polymers that bind with the mucus layer that coats the mucosal epithelial surface and the major molecules that make up mucus. It is the main excipients for adhesion by attracting water, swells and adheres to the mucous through forming a channel by linking to mucin polymer They bind with mucin with help of H-bonding group, hydrophilic group	Semi synthetic/natural polymer: Agarose, gelatin, Hyaluronic acid, pectin and cellulose derivatives. Synthetic polymer: Poly(acrylic acid)-based polymers i.e. poly(acrylic acid-co-thylhexylacrylate), poly(methacrylate) Water soluble polymer: PAA,sodium CMC,sodiumalginate Water insoluble polymer: Chitosan (soluble in dilute aqueous acids), EC, PC Cationic polymer: chitosan, dimethylaminoethyl (DEAE)-dextran, trimethylated chitosan Non ionic polymer: poly(ethylene oxide), PVA, PVP, scleroglucan Anionic polymer: Chitosan-EDTA, CP, CMC, pectin, PAA, PC, sodium alginate, sodium CMC, xanthan gum	[21-23]
2.	Permeation enhancer	Permeation enhancer (<1%) enhances the permeation ability of the drug through the epithelium membrane. The permeation enhancer mechanism depends upon the fick’s first law of diffusion. Its mechanism is as follows: Increasing fluidity and integrity of cell membranes Extracting inter and intracellular lipids Altering cellular proteins Varying mucus rheology Enhancing thermodynamic activity of drugs Decreasing surface tension	Surfactant: Ionic: Dioctyl Sodium sulfosuccinate, Polyoxyethylene-20-cetyl ether Nonionic: Nonylphenoxypolyoxyethylene(NP-POE)(nonionic), Polyoxyethylene-9-lauryl ether (PLE) (nonionic) Fatty acids and derivatives: Acylcarnitine, Oleic acid, Caprylic acid, Mono(di)glycerides and Lauric acid Chelating agents: EDTA,Citric acid and Salicylates Polyols: Propylene glycol and Polyethylene glycol Bile salts and derivatives: Sodium deoxycholate), Sodium glycodihydrofusidate and Sodium deoxycholate Sulfoxides: Dimethyl sulfoxide(DMSO) Others (non-surfactants): Urea and derivative Azone(1-dodecylazacycloheptan-2-one) (laurocapram) and cholines	[24-26]
3.	Enzyme inhibitor	Enzyme inhibitors are used in the formulation of BDDS in order to enchance the drug absorption by decrease the affect of the enzyme over the drug by altering the structural configuration of enzyme and in order to make the drug less susceptible towards the enzyme degradation.	Aprotinin, bestatin, puromycin, bile salts stabilize and polyacrylic acid.	[27-29]

Manufacturing methods of the buccal tablets [6, 10, 26]

Evaluation parameters of buccal drug delivery system

Table 5: Evaluation parameters of BDDS

S. No.	Evaluation parameter	Type of buccal dosage form	Method used	Instrument	Reference
1.	Surface pH	Patch, Tablets Films	Visual colour change	pH meter	[32-35]
2.	Morphology	Tablets, Patches Films	Microscopy	Scanning Electron Microscopy (SEM)	[36-39]
3.	Swelling index	Patches, Films Tablets, Wafers	Swelling of patch and tablet in pH 6.4 phosphate buffer	Agar gel plates	[39-43]
4.	Folding endurance	Patches, Films	Repeated folding in same point	Manually folded	[43-45]
5.	Drug compatibility	Patches, Films Tablets Wafers	Thermal analysis, Spectral analysis	FTIR, DSC, XRD	[46-48]
6.	Thickness	Patches, Films Tablets, Wafers	Standard deviation	Vernier calipers, Screw guaze, Electronic digital micrometer	[49-51]
7.	Mucoadhesive strength	Patches, Films Tablets	Tensile strength	texture analyzer	[42, 58, 62]
8.	Water absorption capacity test	Patches Films	Agar plate technique	Desiccators	[52-54]
9.	Invitro drug release	Tablets, Patches, Films Microspheres	Beaker method; Dissolution method; Rotating paddle method	Kesary chein cell; Franz diffusion cell	[55-58]
10.	Mechanical properties	Patches, Films Buccal hydrogels	Wilhelmy plate technique	Microprocessor Modified tensile strength tester	[59-62]
11.	Residence time	Patches Films	Disintegration	Modified disintegrator	[63, 64]
12.	Palatability test	Patches Films	Grading of taste	E-taste meter	[65-68]
13.	Flatness	Patches Films	Percent constriction	Vernier calipers	[69, 70]
14.	Drug content	Tablets, Patches Films	Titration	RP-HPLC method, UV spectrophotometer	[71-74]
15.	Hardness	Tablets Wafers	Crushing force	Monsanto hardness tester	[75-78]
16.	Friability	Tablets	Weighing	Roche friabilator	[79-83]
17.	Contact angle	Films	Wetting	Optical tensiometer	[72, 84-86]
18.	Transparency	Films	Transmittance	UV spectrophotometer	[87-89]
19.	Water vapour transmission rate	Patches Films	Dressing method	Ovens	[90, 91]
20.	Drug entrapment	Patches, Films, Microspheres	Assay	UV spectrophotometer	[82, 91,]
21.	Bio-adhesion	Patches Films	Colloidal gold staining method Florescence probe method	Dissolution cells	[92, 93]
22.	Percentage moisture loss	Patches Films	Gravimetry method	Desicator	[94, 95]
23.	ex vivo residence time (RT)	Patches Films Tablets	Modified disintegration test apparatus	disintegration tester	[96-98]

Manufacturing methods of the buccal patches/films

Solvent casting

This method is widely used for the manufacturing of the controlled release matrix and liquid reservoir type buccal film, oral disintegrating films, pellets and granules [35, 39].

Direct milling

This method is widely used for the manufacturing of the oral buccal films and buccal wafers [54, 69].

Hot melt extrusion of films

This method is widely used for the manufacturing of the controlled release matrix tablets, oral disintegrating films, pellets and granules. The procedure of hot melts extrusion as follows [80, 97]:

Application of buccal drug delivery

Table 6: applications of bdds

Applications	References
Hypertension. Eg: Atenolol patches. Hormone replacement therapy. Angina pectoris. Eg: Nitroglycerine patches. Cancer. Eg: Opiod analgesics. Smoking cessation therapy. Eg: Nicotine patches. Treatment of microbial infections associated with peridontitis. Local therapy includes oral infections, moth ulcers, dental caries, gingivitis, stomatitis.	[86-102]

Patents of bdds formulations

Table 7: Patents of BDDS formulations

S. No.	Title	Author	Patent number	Year
1.	Buccal and/or sublingual therapeutic formulation	Cumming Alisthair, Kannar david, Sparrow lance	AU2016238901A1	2016
2.	Bioadhesive films for oral and/or systemic delivery	Mcconville Jason Thomas, Morales Javier O, Ross Alistair	US2016128947A1	2016
3.	Buccal delivery system	Rubina Mughal	GB2568554A	2017
4.	Composition and method for Buccal administration of GNRH agonists	De groot Aldemar B, Taneja Rajneesh	WO2017208076A1	2017
5.	Sublingual or Buccal administration of DIM for treatment of skin diseases	Scaife michael	WO2018051183A1	2018
6.	Transmucosal delivery devices with enhanced uptake	Finn Andrew, Vasisht Niraj	US2018133210A1	2018
7.	Chewable composition for rapid Buccal absorption	Purcell Marc	US2019015324A1	2019
8.	Transdermal drug delivery systems for levonorgestrel and ethinyl estradiol	Liao Jun, Nguyen Viet, Patel Prashant	US10231977B2	2019
9.	Buccal swab delivery system	Azimi Nooshin, Cauley Thomas H, Cohen Bruce A, Schnipper Edward F	US2020376241A1	2020
10.	Device and methods for ultrasonic delivery of an agent within an oral cavity	France Marion, Schoellhammmer carl, Sheppard Norman	WO2020018866A1	2020
11.	Enhancing drug activity through accentuated Buccal/sublingual administration	Banerjee Debasish, Banerjee Priyangbada	WO2021019278A1	2021

Marketed products of bdds formulation

Table 8: Marketed products of BDDS formulation

S. No.	Marketed product	Active ingredient	Bioadhesive agent	Dosage form	Company/Manufacturer	Therapeutic class
1.	Buccastem®	Prochlorperazine maleate	Xanthum gum	Buccal tablet	Reckitt Benckiser	Antipsychotics
2.	Corsodyl gel®	Chlorhexidine Digluconate	HPMC	Oral paste	GlaxoSmith Kline	Antimicrobial
3.	Actiq	Fentanyl citrate	Magnesium stearate	Lozenge	Cephalon	Opiod analgesics
4.	Suscard	Glyceryl trinitrate	Hypromellase	Tablet	Forest laboratories	Vasodilator
5.	Corlan pellets	Hydrocortisone sodium succinate	Acacia	Oral mucosal pellets	Celltech	Corticosteroids
6.	Fastum	Ketoprofen	PEG	Gel	A,Menarini industries	NSAIDS
7.	Coreg	Carvedilol	HPMC	Buccal patch	GlaxoSmith Kline	Hypertension
8.	Loramyc	Miconazole	Corn starch	Tablet	BioAliance pharma SA	Antifungal
9.	Bonjela®	Cetalkonium chloride, Choline salicylate	Hypromellose	Gel	Reckitt Benckiser	Antiulcer
10.	Dentipatch®	Lidocaine	Xanthum gum	Patch	Noven	Analgesic

Future outcomes

Buccal drug delivery system offers advantages in accessibility, administration, economy, patient compliance. Novel preparations are focusing on the use of responsive polymeric system using copolymer with desirable hydrophilic/hydrophobic interaction, complexation networks, block or graft polymers from the natural edible sources. At the current global scenario, experts are finding ways to develop Buccal drug delivery with improved bioavailability of orally inefficient drugs by manipulating the formulation with enzyme inhibitors, inclusion of pH, permeation enhancers. At present solid dosage forms, liquids, patches and gels are commercially successful.

CONCLUSION

The Buccal drug delivery system predominantly serves more advantages when compared to controlled drug delivery. It was a promising area for the systemic drug delivery of orally inefficient drugs. It has significant advantages like avoidance of presystemic elimination in GIT and first pass metabolism in liver. Buccal drug delivery can be affected by thickness of mucosal layer, barrier properties of mucosa, area of absorption site and it can be enhanced by penetration enhancers, bio-adhesive agents. In this review we have concluded that with the right dosage form design, mucoadhesive polymers and ideal formulation, the permeability and the local environment of mucosa can be controlled and manipulated in order to enhance drug permeation. This review will help pharmaceutical researchers to clarify the potential of BDDS to overcome the various existing drug delivery dispute like efficiency of absorption, permeability and bioavailability of drugs.

FUNDING

There was no specific funding for this case study from any source

AUTHORS CONTRIBUTIONS

Mrs. V. Leelalakshmi was involved in review of literature and collection of data and preparation of the manuscript. Mr. Umashankar Ms, Mr Alagusundaram M was involved in reviewing, and editing of the manuscript.

CONFLICT OF INTERESTS

there is no conflict of interest for this review.

REFERENCES

1. DiMasi JA, Hansen RW, Grabowski HG. The price of innovation: new estimates of drug development costs. J Health Econ. 2003;22(2):151-85. doi: 10.1016/S0167-6296(02)00126-1, PMID 12606142.

2. Hearnden V, Sankar V, Hull K, Juras DV, Greenberg M, Kerr AR, Lockhart PB, Patton LL, Porter S, Thornhill MH. New developments and opportunities in oral mucosal drug delivery for local and systemic disease. Adv Drug Deliv Rev. 2012;64(1):16-28. doi: 10.1016/j.addr.2011.02.008, PMID 21371513.

3. Hoogstraate JAJ, Wertz PW, Wertz PW. Drug delivery via the buccal mucosa. Pharm Sci Technol Today. 1998;1(7):309-16. doi: 10.1016/S1461-5347(98)00076-5.

4. Mathias NR, Hussain MA. Non-invasive systemic drug delivery: develop ability considerations for alternate routes of administration. J Pharm Sci. 2010;99(1):1-20. doi: 10.1002/jps.21793, PMID 19499570.

5. Shojaei AH. Buccal Mucosa as a route for systemic drug delivery: a review. J Pharm Pharm Sci. 1998;1(1):15-30. PMID 10942969.

6. Lis Fontinele de Sa L, Nogueira NC, Da Silva Filho EC, Figueiras A, Veiga F, Nunes LCC, Lamartine Soares-Sobrinho J. Design of buccal mucoadhesive tablets: understanding and development. J Appl Pharm Sci. 2018;8:150-63.

7. Venkataswamy R, Lavanya Nallaguntla. Review article on pulsatile drug delivery system. Asian J Pharm Clin Res. 2021;14:48-59.

8. Carvalho FC, Bruschi ML, Evangelista RC, Gremião MPD. Mucoadhesive drug delivery systems. Braz J Pharm Sci. 2010;46(1):1-17. doi: 10.1590/S1984-82502010000100002.

9. Satishbabu BK, Srinivasan BP. Preparation and evaluation of buccoadhesive films of atenolol. Indian J Pharm Sci. 2008;70(2):175-9. doi: 10.4103/0250-474X.41451, PMID 20046708.

10. Palem CR, Gannu R, Yamsani SK, Yamsani VV, Yamsani MR. Development of bioadhesive buccal tablets for felodipine and pioglitazone in combined dosage form: in vitro, ex vivo, and in vivo characterization. Drug Deliv. 2011;18(5):344-52. doi: 10.3109/10717544.2011.557786, PMID 21351826.

11. Chinna Reddy PKS, Chaitanya KS, Madhusudan Rao Y. A review on bioadhesive Buccal drug delivery systems: current status of formulation and evaluation methods. Daru. 2011;19(6):385-403. PMID 23008684.

12. Harris D, Robinson JR. Drug delivery via the mucous membranes of the oral cavity. J Pharm Sci. 1992;81(1):1-10. doi: 10.1002/jps.2600810102, PMID 1619560.

13. Wertz PW, Squier CA. Cellular and molecular basis of barrier function in oral epithelium. Crit Rev Ther Drug Carrier Syst. 1991;8(3):237-69. PMID 1954652.

14. Thakur G, Wani SUD, Gautam SP. A review on recent advancement in pulsatile drug delivery systems. Int J Curr Pharm Res. 2021;13:6-10.

15. Kamimori GH, Karyekar CS, Otterstetter R, Cox DS, Balkin TJ, Belenky GL, Eddington ND. The rate of absorption and relative bioavailability of caffeine administered in chewing gum versus capsules to normal healthy volunteers. Int J Pharm. 2002;234(1-2):159-67. doi: 10.1016/s0378-5173(01)00958-9, PMID 11839447.

16. Zhang J, Streisand J, Niu S. Estimation of bucccal fentanyl absorption bioavailability by measuring drug depletion from vehicle solutions: validation of the method in dogs. Pharm Res. 1992;9:S177.

17. Chinna Reddy P, Madhusudan Rao Y. Buccal drug delivery systems. Adv Drug Deliv Rev. 2010;1:139-210.

18. Patel KV, Patel ND, Dodiya HD, Shelat PK. Buccal bioadhesive drug delivery system: an overview. Int J Pharm Bio Arch. 2011;2:600-9.

19. Patel VM, Prajapati BG. Design and in vitro characterization of eudragit containing mucoadhesive buccal patches. Int J Pharm Tech Res. 2009;1:783-9.

20. Gandhi Pankil A. A review article on muco-adhesive Buccal drug delivery system. IJPRD. 2011;3:159-73.

21. Wise Donald L. Handbook of Pharmaceutical controlled release technology; 2000. p. 255-65.

22. Khairnar GA, Sayyad FJ. Development of Buccal drug delivery system based on mucoadhesive polymer. Int J PharmTech Res. 2010;2:719-35.

23. Utoguchi N, Watanabe Y, Suzuki T, Maehara J, Matsumoto Y, Matsumoto M. Carrier-mediated transport of monocarboxylic acids in primary cultured epithelial cells from rabbit oral mucosa. Pharm Res. 1997;14(3):320-4. doi: 10.1023/a:1012046021028. PMID 9098874.

24. Shinde AKJ, Patil NS, Jadhav TS, More HN. Design and development of floating pulsatile drug delivery of losartan potassium. Int J Appl Pharm. 2020;12:218-27.

25. Vyas SP, Khar RK. Controlled drug delivery-concepts and advances. Vallabh Prakashan. 1st ed. New Delhi; 2002.

26. Bottenberg P, Cleymaet R, de Muynck C, Remon JP, Coomans D, Michotte Y, Slop D. Development and testing of bioadhesive, fluoride-containing slow-release tablets for oral use. J Pharm Pharmacol. 1991;43(7):457-64. doi: 10.1111/j.2042-7158.1991.tb03514.x, PMID 1682457.

27. Rossi S, Sandri G, Caramella CM. Buccal drug delivery: A challenge already won? Drug Discov Today Technol. 2005;2(1):59-65. doi: 10.1016/j.ddtec.2005.05.018, PMID 24981756.

28. Junginger HE, Hoogstraate JA, Verhoef JC. Recent advances in buccal drug delivery and absorption- in vitro and in vivo studies. J Control Release. 1999;62(1-2):149-59. doi: 10.1016/s0168-3659(99)00032-2, PMID 10518646.

29. Salamat-Miller NS, Chittchang M, Johnston TP. The use of mucoadhesive polymers in buccal drug delivery. Adv Drug Deliv Rev. 2005;57(11):1666-91. doi: 10.1016/j.addr.2005.07.003, PMID 16183164.

30. Wani Manish S. Current status in buccal drug delivery system. Pharmainfo Net. 2007;5:1-15.

31. Kumar. Mechanism of Buccal permeation enhancers. Indian J Pharm Edu. 2002;36:147-51.

32. Trastullo R, Abruzzo A, Saladini B, Gallucci MC, Cerchiara T, Luppi B, Bigucci F. Design and evaluation of buccal films as paediatric dosage form for transmucosal delivery of ondansetron. Eur J Pharm Biopharm. 2016;105:115-21. doi: 10.1016/j.ejpb.2016.05.026, PMID 27267732.

33. Alur HH, Johnston TP, Mitra AK. Encyclopedia of pharmaceutical technology. In: Swarbrick J, Boylan JC, editors, Peptides and protein S: buccal absorption. Vol. 20. New York: Marcel Dekker Inc; 2001. p. 193-218.

34. Hao J, Heng PW. Buccal delivery systems. Drug Dev Ind Pharm. 2003;29(8):821-32. doi: 10.1081/ddc-120024178, PMID 14570303.

35. kaur A, kaur G. Mucoadhesive buccal patches based on interpolymer complexes of chitosan-pectin for delivery of carvedilol. Saudi Pharm J. 2012;20(1):21-7. doi: 10.1016/j.jsps.2011.04.005, PMID 23960773.

36. Veuillez F, Kalia YN, Jacques Y, Deshusses J, Buri P. Factors and strategies for improving Buccal absorption of peptides. Eur J Pharm Biopharm. 2001;51(2):93-109. doi: 10.1016/s0939-6411(00)00144-2, PMID 11226816.

37. Barocas VH, Balachandran RK. Sustained transscleral drug delivery. Expert Opin Drug Deliv. 2008;5(1):1-10. doi: 10.1517/17425247.5.1.1. PMID 18095925.

38. Verma S, Kaul M, Rawat A, Saini S. An overview on Buccal drug delivery system. IJSR. 2011;2:1303-21.

39. Himabindu. Formulation and in vitro evaluation of mucoadhesive buccal patches of cyproheptadine hydrochloride. J App Pharm Sci. 2012;2:196-201. doi: 10.7324/JAPS.2012.2731.

40. Wong CF, Yuen KH, Peh KK. An in vitro method for buccal adhesion studies: importance of instrument variables. Int J Pharm. 1999;180(1):47-57. doi: 10.1016/s0378-5173(98)00402-5, PMID 10089291.

41. Reddy RJ, Anjum M, Hussain MA. A comprehensive review on buccal drug delivery system. AJADD. 2013;1:300-12.

42. semalty M, Semalty A, Kumar G. Formulation and characterization of mucoadhesive buccal films of glipizide. Indian J Pharm Sci. 2008;70(1):43-8. doi: 10.4103/0250-474X.40330, PMID 20390079.

43. Vani C, Srinivas Reddy K. Pulsatile drug delivery system-a technique of delivering drug in accordance with biological clock- a review. Int J Adv Res. 2021;9(4):101-24. doi: 10.21474/IJAR01/12813.

44. Aungst BJ, Rogers NJ. Site dependence of absorption-promoting actions of laureth-9, Na salicylate, Na2EDTA, and aprotinin on rectal, nasal, and buccal insulin delivery. Pharm Res. 1988;5(5):305-8. doi: 10.1023/a:1015930821648, PMID 2469079.

45. Fariya Mozammel F, Irin Dewan SM, Ashraful Islam Ashraful. A comprehensive review on Buccal drug delivery system. World J Pharm Pharm Sci. 2019;8:77-93.

46. Dibyalochan Mohanty, Gurulatha GC, Vasudha Bakshi V, Mavya B. Novel approaches on buccal mucoadhesive drug delivery system. Indo Am J Pharmacol Sci. 2018;5:2131-45.

47. Wadageri GV, Raju SA, Shirsand SB, Reddy VP. Buccal drug delivery system of atenolol. Res J Pharm Technol. 2012;5:1-18.

48. Boateng JS, Areago D. Composite sodium alginate and chitosan based wafers for Buccal delivery on macromolecules. Austin J Anal Pharm Chem. 2014;1:16-24.

49. Raghavendra Rao NG, Shravani B, Mettu Srikanth Reddy M. Overview on buccal drug delivery systems. J Pharm Sci. 2013;5:80-8.

50. Dhanashri Garud P, Kalyani Dalavi K, Sagar Doele. Application of thiolated chitosan in mucoadhesive Buccal drug delivery system. Application of thiolated chitosan in mucoadhesive Buccal drug delivery system. World J Pharm Res. 2020;9:622-36.

51. Gite Shital Shridhar, Shinkar Dattataraya Manohar, Saudagar Ravindra Bhanudas. Mucoadhesive Buccal drug delivery: an overview. Japer. 2013;3:319-32.

52. Patel D, Patel C, Shah P. Formulation and evaluation of bioadhesive Buccal drug delivery of repaglinide tablets. Asian J Pharm. 2012;6(3):171-9. doi: 10.4103/0973-8398.104830.

53. Reddy Jagadeeshwar R Maimuna Anjum, Mohammed Asif Hussain. A comprehensive review on Buccal drug delivery system. Am J Adv Drug Deliv. 2013;1:300-12.

54. Seema, Kapil Kumar, Deepak Teotia. A comprehensive review on buccal patches. GSC Biol Pharm Sci;13(1):130-5. doi: 10.30574/gscbps.2020.13.1.0308.

55. Ghate SK, Sakarkar. DM. Development and evaluation of osmotically controlled oral drug delivery system. Asian J Pharm Technol. 2017;7(4):459-70. doi: 10.5958/2231-5713.2017.00033.2.

56. Yamagar M, Kadam V, Hirlekar R. Design and evaluation of buccoadhesive drug delivery system of metoprolol tartarate. Int J Pharm Tech Res. 2010;2:453-62.

57. Mohammadi Samani Soliman, Bahri Najafi Rahim, Yousefi Golamhosein. Formulation and in vitro evaluation of prednisolone buccoadhesive tablets. Farmaco. 2005;60(4):339-44. doi: 10.1016/j.farmac.2005.01.009, PMID 15848210.

58. Rajaram Dipak Malpure, Laxman Sharada Deore. Buccal mucoadhesive films: a review. Syst Rev Pharm. 2016;8(1):31-8. doi: 10.5530/srp.2017.1.7.

59. Reddy Sunitha M, Surekha, Anusha G, Mallikarjun Reddy S, Manasa K, Soumya G. A review on transbuccal drug delivery system and its commercially available products. Res J Pharm Technol. 2013;6:1-16.

60. Chaudhari SR, Harsulkar AA. Design and in vitro evaluation of mucoadhesive buccal tablets of carvedilol. Int J Pharm Tech Res. 2012;4:1827-33.

61. Singh R, Sharma D, Garg R. Review on mucoadhesive drug delivery sysem with special emphasis on Buccal route: An important tool in designing of novel controlled drug delivery system for the effective delivery of pharmaceuticals. J Dev Drugs. 2017;6:1-12.

62. El-Maghraby Gamal M, Abdelzaher Mona M. Formulation and evaluation of simvastatin Buccal film. J App Pharm Sci. 2015;5:70-7. doi: 10.7324/JAPS.2015.50412.

63. Chin Nala Krishna Mohan, Panigrahy Rabi Narayan, Mesa Rajendra, Deshu Isaac. Formulation and in vitro evaluation of bilayer muco adhesive drug delivery system containing nifedipine. Int J Pharm Educ. 2014;1:1-8.

64. Patel KV, Patel ND, Dodiy HD, Shelat PK. Buccal bioadhesive drug delivery system: an overview. Int J Pharm Biol Sci Arch. 2011;2:600-9.

65. Pranshu Tangri Satheessh Madhav NV. Oral mucoadhesive drug delivery systems: a review. Int J Biopharm. 2011;2:36-46.

66. Roychowdhury Santanu, Guptha Rajesh, Saha Sourav. A review on Buccal mucoadhesive drug delivery systems. Indo Glob J Pharm Sci. 2011;1:223-33.

67. AL-Dhubiab Bandar E, Nair Anroop B, Kumria Rachna, Attimarad Mahesh, harsha Sree. Formulation and evaluation of nanobased drug delivery system for the Buccal delivery of acyclovir. Colloids Surf B Biointerfaces. 2015;136:878-84. doi: 10.1016/j.colsurfb.2015.10.045, PMID: 26547315

68. Wang Y, Lian Z, Chen M, Zhang L, Zhou C, Wei W. Bioadhesive drug delivery system of diltiazem hydrochloride for improved bioavailability in cardiac therapy. Trop J Pharm Res. 2016;15(7):1375-80. doi: 10.4314/tjpr.v15i7.4.

69. Vishnu Y Vamshi, Chandrasekhar K, Ramesh G, Rao Y Madhusudan. Development of mucoadhesive patches for buccal administration of carvedilol. Curr Drug Deliv. 2007;4(1):27-39. doi: 10.2174/156720107779314785, PMID 17269915.

70. Patil SB, Murthy RSR, Mahajan HS, Wagh RD, Gattani SG. Mucoadhesive polymers: means of improving drug delivery. J Pharm Times. 2006;38:25-8.

71. Singh Chhotec Lal, Srivastava Namita, Monga Munish Garg, Singh Amit. A review: buccal buccoadhesive drug delivery system. World J Pharm Res. 2014;2:1803-7.

72. Bhanja SB, Ellaiah P, Martha SK, Kar RK, Panigrahi BB. Buccoadhesive drug delivery system of captopril: formulation and in vitro evaluation. J Pharm Res. 2010;3:335-40.

73. Parodi B, Russo E, Caviglioli G, Cafaggi S, Bignardi G. Development and characterization of a buccoadhesive dosage form of oxycodone hydrochloride. Drug Dev Ind Pharm. 1996;22(5):445-50. doi: 10.3109/03639049609069353.

74. Raju KN, Velmurugan S, Deepika B, Sundar V. Formulation and in vitro Evaluation of buccal tablets of metoprolol tartrate. Int J Pharm Pharm Sci. 2011;3:239-46.

75. Yamagar M, Kadam V, Hirlekar R. Design and evaluation of buccoadhesive drug delivery system of metoprolol tartrate. Int J Pharm Tech Res. 2010;2:453-62.

76. Yamsani Vamshi Vishnu, Gannu Ramesh, Kolli Chandrasekhar, Rao ME Bhanoji EB, Yamsani Madhusudan Rao. Development and in vitro evaluation of buccoadhesive carvedilol tablets. Acta Pharm. 2007;57(2):185-97. doi: 10.2478/v10007-007-0015-7, PMID 17507315.

77. Shinde Anil Kumar J, Patil Nidhi S, Jadhav Trupti S, More Harinath N. Design and development of floating pulsatile drug delivery of losartan potassium. Int J App Pharm. 2020;12:218-27. doi: 10.22159/ijap.2020v12i4.37607.

78. Nafee Noha Adel, Ismail Fatma Ahmed, Boraie Nabila Ahmed, Mortada Lobna Mohamed. Mucoadhesive delivery systems. I. Evaluation of mucoadhesive polymers for buccal tablet formulation. Drug Dev Ind Pharm. 2004;30(9):985-93. doi: 10.1081/ddc-200037245. PMID 15554223.

79. Jain NK. Controlled and novel drug delivery. 1st ed. New Delhi: CBS Publishers; 2004. p. 236-55.

80. Singh TP, Singh RK, Shah JN, Mehta TA. Mucoadhesive bilayer buccal patches of verapamil hydrochloride: formulation development and characterization. Int J Pharm Pharm Sci. 2014;6:234-41.

81. Prasanth VV, Sirisha M, Mathew Sam T, Mathapan Rinku. Buccal tablet as mucoadhesive drug delivery: an over view. J Pharm Res. 2011;4:706-9.

82. Borgaonkar PA, Virsen TG, Hariprasanna RC, Najmuddin M. Formulation and in vitro evaluation of buccal tablets of loratadine for effective treatment of allergy. Int J Res Pharm Chem. 2011;1:551-9.

83. Naga Raju K, Velmurugan S, Deepika B, Vinushitha Sundar. Formulation and in vitro evaluation of buccal tablets of metoprolol tartrate. Int J Pharm Pharm Sci. 2011;13:239-46.

84. Senel Sevda, Hincal AA. Drug permeation enhancement via buccal route: possibilities and limitations. J Control Release. 2001;72(1-3):133-44. doi: 10.1016/s0168-3659(01)00269-3, PMID 11389992.

85. Shojaei AH. Buccal mucosa as a route for systemic drug delivery: a review. J Pharm Pharm Sci. 1998;1(1):15-30. PMID 10942969.

86. Kadam Prasad B, Dias Remeth J, Mali Kailas K, Havaldar Vijay D, Mahajan Niranjan S. Formulation and evaluation of buccoadhesive tablets of atenolol. J Pharm Res. 2008;1:193-9.

87. Satishbabu BK, Srinivasan BP. Preparation and evaluation of buccoadhesive films of atenolol. Indian J Pharm Sci. 2008;70(2):175-9. doi: 10.4103/0250-474X.41451, PMID 20046708.

88. Mohammed Fergany A, Khedr Hussin. Preparation and in vitro/in vivo evaluation of the buccal bioadhesive properties of slow-release tablets containing miconazole nitrate. Drug Dev Ind Pharm. 2003;29(3):321-37. doi: 10.1081/ddc-120018206, PMID 12741613.

89. Tiwari D, Sause R, Madan PL, Goldman D. Evaluation of polyoxyethylene homopolymers for buccal bioadhesive drug delivery device formulations. AAPS PharmSci. 1999;1(3):50-7. doi: 10.1208/ps010313.

90. Sharmin N, Elias-Al-Mamun M, Islam MS, Jalil R. Preparation and characterization of lidocaine double layer buccal tablet using mucoadhesive carbopol® polymers. Dhaka Univ J Pharm Sci. 2011;10(1):29-34. doi: 10.3329/dujps.v10i1.10012.

91. Desai KG, Kumar TM. Preparation and evaluation of a novel buccal adhesive system. AAPS PharmSciTech. 2004;5(3):e35. doi: 10.1208/pt050335, PMID 15760069.

92. Abd-Elbary A, Makky AMA, Tadros MI, AA Alaa-eldin. Development and in vitro evaluation of mucoadhesive bilayer buccal tablets of carvedilol. Int J Pharm Pharm Sci. 2015;7:172-6.

93. Darekar SS, Khadabadi SS, Shahi SR. Formulation and evaluation of bilayer buccal tablet of sumatriptan succinate. Int J Pharm Pharm Sci. 2014;6:469-75.

94. Abouhussein DMN, El-bary AA, Shalaby SH, Nabarawi MAE. Chitosan mucoadhesive buccal films: effect of different casting solvents on their physicochemical properties. Int J Pharm Pharm Sci. 2016;8(9):206-13. doi: 10.22159/ ijpps.2016.v8i9.12999.

95. Mumtaz AM, Ch’ng HS. Design of a dissolution apparatus suitable for in situ release study of triamcinolone acetonide from bioadhesive buccal tablets. Int J Pharm. 1995;121(2):129-39. doi: 10.1016/0378-5173(94)00406-U.

96. Peddapalli H, Chinnala KM, Banala N. Design and in vitro characterization of mucoadhesive buccal patches of duloxetine hydrochloride. Int J Pharm Pharm Sci. 2017;9(2):52-9. doi: 10.22159/ijpps.2017v9i2.13793.

97. Peh KK, Wong CF. Polymeric films as vehicle for buccal delivery: swelling, mechanical, and bioadhesive properties. J Pharm Pharm Sci. 1999;2(2):53-61. PMID 10952770.

98. Singh B, Chakkal SK, Ahuja N. Formulation and optimization of controlled release mucoadhesive tablets of atenolol using response surface methodology. JAAPS Pharm. Sci Technol. 2006;7:1.

99. Hoogstraate JAJ, Wertz PW, Wertz PW. Drug delivery via the buccal mucosa. Pharm Sci Technol Today. 1998;1(7):309-16. doi: 10.1016/S1461-5347(98)00076-5.

100. Han RY, Fang JY, Sung KC, Hu OYP. Mucoadhesive buccal disks for novel nalbuphine prodrug controlled delivery: effect of formulation variables on drug release and mucoadhesive performance. Int J Pharm. 1999;177(2):201-9. doi: 10.1016/s0378-5173(98)00343-3, PMID 10205614.

101. Deasy PB, O’Neill CT. Bioadhesive dosage form for peroral administration of timolol base. Pharm Acta Helv. 1989;64(8):231-5. PMID 2780757.

102. Agaiah Goud B, Kumara Swamy S, Praveen Kumar V. Formulation and evaluation of bioadhesive buccal tablets of simvastatin. Adv Pharmacol Sci. 2011;1:29-38.