Research & Reviews in Pharmacy and Pharmaceutical Sciences
Menue-ISSN:2320-1215 p-ISSN: 2322-0112
e-ISSN:2320-1215 p-ISSN: 2322-0112
Sakshi Saxena and Nikku Yadav*
Centre for Biosciences and Clinical Research, School of Biosciences, Apeejay Stya University, India
Received date: 16-02-2017 Revised date: 30-02-2017 Accepted date: 05-03-2017
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Oral route of drug administration has been the most preferred one due to the seamlessly numerous advantages that it offers. Adding on to the existing benefits, researchers have smartly used the recent technology and advance knowledge to take oral drug delivery system to next level of patient convenience and compliance. Fast dissolving tablets (FDTs) are the output of this ongoing advancement in science. This novel concept addresses many patient needs from enhancing life cycle management to offering super convenient dosing, especially for pediatric, geriatric, and psychiatric patients for whom swallowing the conventional tablets and capsules was a trouble. This present report generates database on development and evaluation of FDTs from 2000-2016. Along with this, it is aimed at providing complete information of superdisintegrants and the techniques employed in preparation of FDTs studies in past 15 years. Sixty studies were taken into consideration. The findings suggest that majority of FDTs are formulated for NSAIDs, analgesics, GI drugs and cardiovascular including antihypertensive drugs and least for antidiabetic and anticancer drugs. Most of the studies (34 out of 42 studies) used crosspovidone at different concentrations (5% to 10% w/w). 36 out of 60 studies used direct compression (DC) technique for formulation of FDTs.
Fast dissolving tablets, Super disintegrants, Crosspovidone, Direct compression, Crosscarmellose, Plantago ovata
Drugs have been saving lives since time immemorial. Although new drug delivery system involves tremendous innovations, oral route still remains most preferred route of drug administration. The advantageous of this route include accurate dosage, low cost therapy, good stability, self-medication, non-invasive method, ease of administration and patient compliance [1-3]. However traditional tablets and capsules administrated with amount of water as large as 8-oz of glass may be impractical for some geriatric patients Nautiyal [4], due to changes in physiological function with advancing age. Furthermore, for other patient groups such as mentally challenged, uncooperative patients and those who are bed ridden or travelling with limited access to water, the versatility of conventional oral drug delivery system gets a halt.
Therefore, to extend the benefits of oral dosage form to the disadvantaged patient groups, advancements in technology and improved knowledge has led to development of alternative concept called fast dissolving tablet (FDT) technology. The Food and Drug Administration defines FDT as ‘‘a solid dosage form containing medicinal substances which disintegrates rapidly, usually within a matter of seconds, when placed upon the tongue’’. Bandari [5] These tablets disintegrate in mouth itself in few seconds to minutes, thereby eliminating the need for swallowing with water. Although these tablets are like the traditional ones, they need to have certain unique properties.
• water not required to swallow, use saliva as the disintegrating solvent in order to disintegrate into smaller particles in few seconds
• no residue in mouth and masked taste [6].
• low cost of manufacturing
• minimum environmental hazards
Advantages offered by FDTs
One of the numerous reasons that are bringing success to these FDTs is that they incorporate in them, the goodness of both solid as well as liquid dosage forms [6]. Following are the key benefits that have made FDTs draw the interest of healthcare and clinicians.
a. FDTs have inherited the benefit of accurate dosing and good physical as well as chemical stability from solid dosage forms [7].
b. In less than a minute, FDTs disintegrate into simpler granules and form paste in oral cavity itself. This in turn begins absorption right in the mouth, thereby increasing bioavailability [8] along with imparting rapid therapeutic action [9].
c. FDTs are easy to administer, dissolve in mouth and thus do not need water to be swallowed, they have simply turned up to be no less than a boon to geriatric, pediatric, mentally disabled and bed ridden patients [10] for whom swallowing hard tablets and capsules was troublesome.
d. Enhanced palatability and patient compliance due to good taste and obstruction free swallowing respectively, gives FDTs an edge over the traditional solid dosage forms which raise the risk of obstruction in airways while swallowing [9].
e. On manufacturer’s part, these FDTs are cost effective and bring in business avenue through product differentiation, line extension uniqueness and conventional processing and packaging equipments used in production process [10].
These benefits are good enough for the health care industry to recognize the significance of FDTs and the need for their development. The key idea behind the success of FDTs is the use of superdisintegrants [10]. These are the substances that provide FDTs, the characteristic fast dissolving property. A lot many synthetic as well as natural superdisintegrants such as Sodium Lauryl Sulphate (SLS), Crosscarmellose Sodium (CCS), Sodium starch glycolate (SSG), Crosspovidone (CP), isaphghula mucilage, banana powder, pectin, fenugreek gum, Plantago ovata husk and agar and so on have been widely used. Not just this, even the techniques used in the formulation process shows diversity. Right from conventional direct compression technique to improved drying, granulation, effervescence and sublimation processes, preparation of FDTs have employed them all smartly.
Surprisingly, it hasn’t been more than two decades and the concept of FDT technology has conquered almost all the therapeutic classes of drugs. From analgesics, antipyretics, and antimicrobials to those treating disorders of critical organs like liver, heart, brain, and kidney, FDTs have been formulated for each of these classes of drugs.
This paper aims to provide complete database for the status of FDT, whose preparation involves use of different superdisintegrants including natural as well as synthetic ones at different composition and, wide ranging techniques.
English language journals published between 2000-2016 were manually searched. PubMed, Google Scholar and Cochrane database were searched using keywords: Formulation of fast dissolving tablets, mouth dissolving tablets, oral disintegrating tablets and Orodispersible tablets. The studies were selected based on following inclusion and exclusion criteria.
Inclusion criteria:
• Only research studies that involved formulation and evaluation of FDT using different superdisintegrants or different composition of super disintegrants.
• Formulation of FDTs for taste masking.
Exclusion criteria
Studies that met inclusion criteria were selected. Studies with duplicate publication, unbalanced matching or incomplete data were excluded.
Result/findings
All sixty studies under consideration were catalogued and their findings were tabulated in Table 1. Selected studies were categorized in to two groups: Group 1 deals with formulation and evaluation of FDT using different superdisintegrants or different composition of superdisintegrants, Group 2 included formulation of FDTs for taste masking.
| FDT Formulation | Technique | Super Disintegrant | Best Concentration |
|---|---|---|---|
| Oxcarbazepine | DC | Crospovidone, Sodium lauryl Sulphate |
10% Crospovidone+6% Sodium lauryl Sulphate |
| Ofloxacin | DC | Sodium starch Glycolate, Crospovidone, Crosscarmellose | Sodium starch Glycolate-6.8%, +Crospovidone-6.8% +crosscarmellose 6.8% |
| Lornoxicam | DC | Sodium Starch Glycolate, Crospovidone and Crosscarmellose Sodium | 4.8% Croscarmellose Sodium |
| Etoricoxib | S | Crosspovidone | 4% crospovidone |
| Diclofenac | WG | Cucurbita Maxima and Sodium Starch Glycolate | Cucurbita Maxima=2.5% as well as 5% Starch Sodium Glycolate=2.5% |
| Meloxicam | WG | Crospovidone | 10% |
| Tolvaptan | WG | Crospovidone | 6% |
| Meloxicam | SD | Croscarmellose | 4% |
| Promethazine theoclate | DC | Crosspovidone | 2.61% |
| Silymarin | DG | Croscarmellose Sodium, Colloidal Silicon Dioxide Crospovidone, Sodium Starch Glycolate | 1.9% colloidal silicon dioxide+8.3%Crospovidone+11.1% Microcrystalline Cellulose +11.4% Sodium Starch Glycolate |
| Haloperidol | S | Sodium Starch Glycolate with Crosscarmellose Sodium | 10% Crosscarmellose Sodium |
| Naproxen sodium | S | Sodium Starch Glycolate and Crosscarmellose Sodium | 6% each (separately) |
| Nimesulide | VD | Crosspovidone | 4% |
| Ondansetron hydrochloride | S | Camphor (no superdisintegrant used) | 15% |
| Metoclopramide hydrochloride | DC | Sodium Starch Glycolate, Croscarmellose Sodium and Crospovidone |
4.6% Crospovidone |
| Ciprofloxacin | DC | Sodium Starch glycolate, Crosscarmellose sodium, crosspovidone | 4% crospovidone |
| Diltiazem hydrochloride | DC | Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone | 4.5% crospovidone |
| Ornidazole | DC | Microcrystalline Cellulose and Sodium Starch Glycolate | Sodium Starch Glycolate: Mircocrystalline Cellulose=1.5:0 |
| Clonazepam | DC | Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone, Microcrystalline Cellulose | 10% w/w of Crospovidone and 35% w/w of Microcrystalline Cellulose |
| Metoprolol tartrate | DC | Natural-Treated Agar, Agar Synthetic-Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone |
6% treated Agar |
| Glipizide | DC | The husk of Plantago ovata and pregelatinized husk of P. ovata. | 20% pregelatinized husk of P. ovata |
| Cinnarizine | S | Sodium Starch Glycolate, Crosscarmellose Sodium | 8% Sodium Starch Glycolate+8% Crosscarmellose Sodium |
| Loratadine | DC | Crosscarmellose Codium | 8.8% |
| Candesartan cilexetil | SD | Ac Di sol | 4% |
| Valdecoxib | SD | Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone | 15% Crosspovidone |
| Valsartan | DC | Crosspovidone | 8% |
| Rainstorm hydrochloride | VD | Plantago ovata Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone |
Crosscarmellose Sodium=10% Plantago ovata=10% |
| Diclofenac and aspirin | DC | Sodium Starch Glycolate, Crosspovidone Plantago ovata, Ac Di sol | 6% to 10% each |
| Levodopa-Carbidopa | DC | Sodium Starch Glycolate, Crosspovidone, microcrystalline Cellulose | Crosspovidone 10% to 20% |
| Ondansetron | SD | Croscarmellose Sodium, crospovidone, Sodium Starch Glycolate, and low substituted hydroxy propyl Cellulose. | Drug: crospovidone=1:3 |
| Amlexanox | MDG | Sodium Laurl Sulphate (SLS), microcrystalline cellulose(MCC), Crosscarmellose sodium (CCS), Crosspovidone (CP) | 1% SLS+70.9% MCC+4% CCS+4% CP |
| Levocetrizine hydrochloride | DC | Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone | 5% SSG+5% CP |
| Levocetirizine dihydrochloride | S | Crosspovidone | 2.6% to 5.3% |
| Stavudine | DC | Crosspovidone, Sodium Starch Glycolate | 20% each |
| Diclofenac | DC | Crosscarmellose Sodium | Cross Carmellose Sodium, PVP in ratio 1:2 (4%w/w) |
| Roxithromycin | SE | Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone | Crosscarmesllose sodium 4.8% |
| Diclofenac | DC | Sodium Starch Glycolate, Crosscarmellose sodium, Crosspovidone | 3% crospovidone |
| Flutamide | DC | Sodium Starch Glycolate | 6.6% |
| Pheniramine maleate | E | Pregelatinized starch, Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone | 4% w/w CP |
| Lorazepam | E | Crosspovidone | 8% w/w CP |
| Caffeine | E | Sodium Bicarbonate and Sorbitol | 1:3 |
| Prochlorperazine maleate | E | Crosscarmellose Sodium, Crosspovidone | 10% CP |
| Amlodipine | DC | Crosspovidone, Sodium Starch Glycolate | 5% crosspovidine+3% SSG |
| Hydrochlorothizide | DC | Isapghula Mucilage and Banana Powder | 8% Isapghula mucilage |
| Salbutamol sulphate | DC | Sodium Starch Glycolate | 4% SSG |
| Enalapril maleate | DC | Crosspovidone, Sodium Starch Glycolate | CP: SSG=1:1 |
| Bisoprolol hemi fumarate | SD | Hydroxypropyl methyl cellulose, Ethyl cellulose | 1:1 of hydroxypropyl methyl cellulose (HPMC): Ethyl cellulose (EC) |
| Ondansetron hydrochloride | DC | Polyplasdone XL-10 (crospovidone)), Ac Di sol, Primogel (SSG) | 7% polyplasdone |
| Montelukast sodium | DC | Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone | CCS: CP 1:3 |
| Ondansetron | DC | Crosscarmellose Sodium, Crosspovidone, Microcrystalline Cellulose | 5% CP and 20% MCC |
| Albendazole | DC | Microcrystalline Cellulose, Crosscarmellose Sodium, Sodium Starch Glycolate Natural-Isapghula |
6% SSG |
| Diclofenac sodium | DC | Fenugreek gum | 6% |
| Atropine sulfate | DC | Low-substituted hydroxypropyl cellulose | 8.3% to 9.9% |
| Alfuzosin hydrochloride | DC and S | Sodium Starch Glycolate, Crosscarmellose sodium, Crosspovidone | 10% w/w CP |
| Oxcarbazepine | DC | Microcrystalline Cellulose, Crosscarmellose sodium, Crosspovidone | Crosspovidone 10% |
| Lamotrigine | DC | Solutab (CCS), Explotab (SSG) and Polyplasdone XL (CP) | 20% Solutab and 20% explotab |
| Simvastatin | DC | Sodium Starch Glycolate, Crosscarmellose Sodium, Crosspovidone | 5% CP |
| Zolmitriptan | DC | Ispaghula husk powder, Gellan gum, Sodium alginate | 4% of Gellan gum |
| Atenolol and Atorvastatin | DC, E, S | Croscarmellose Sodium and Kyron-T134 (ion exchange resin) | Kyron-T134 (6%) and croscarmellose sodium (2%) |
| Tramadol hydrochloride | DC | Microcrystalline Cellulose, Sodium Starch Glycolate, Crosscarmellose sodium, Crosspovidone | CCS with CP 5% each |
Note: DC=Direct compression, WG=wet granulation, DG=Dry granulation, S= Sublimation, SD=Solid Dispersion, VD=Vacuum Drying, MDG=Molecular Dispersion Granule, SE=Solvent Evaporation, E=Effervescence
Table 1. List of various existing studies on fast dissolving tablets, super disintegrants used and their mechanism of action.
Formulation of FDTs Drug
The characteristics of a drug intended for disintegration in mouth and pre-gastric absorption from solid dosage form include, free from bitter taste, 20 mg dose or less, small weight and good solubility in saliva. There are no specific limitations for the formulation of FDTs and this becomes a major reason for the wide range of FDT formulations that have turned to be promising candidates of advanced pharmaceutical industry. Formulated FDTs belong to different categories of drugs: analgesics, anti-inflammatory, gastrointestinal (GI) and antiemetic’s, antipsychotic, antimicrobials, antidiabetic, cardiovascular and antihypertensive, antiallergic, antiviral, anticancer, anti-respiratory and Central Nervous System drugs. Data from Table 1 shows majority of FDTs are formulated for NSAIDs, analgesics, GI drugs and cardiovascular drugs including antihypertensive drugs and least for antidiabetic and anticancer drugs as depicted in Figure 1. The enormous work in drug classes-analgesics and anti-inflammatory may be because of their wide application and low bioavailability through digestive tract and inconvenient route of administration of currently available dosage forms. FDTs resolve these issues aptly.
Figure 1. Shows number of studies reported from 2001-2016, for FDTs formulation in dfferent category of drugs.
Use of Superdisintegrants
Superdisintegrants affect the rate of disintegration and high concentration of this causes change in taste, hardness, and friability of the tablets. Therefore, various instructions need to be followed while selecting superdisintegrants for formulation of a particular drug.
These instructions include rapid disintegration in mouth, compactness of tablet, good mouth feel and patient compliance. Superdisintegrants can be of natural origin or synthetic ones. Some of the commonly used super disintegrates are listed in Table 2.
| Sr no | Synthetic | Natural |
|---|---|---|
| 1 | Sodium Starch Glycolate (SG) | Gellan gum from Pseudomonas elodea |
| 2 | Crospovidone(CP) | Xanthan gum from Xanthomonas Campetris |
| 3 | Croscarmellose sodium(CS) | Husk of Plantago ovata |
| 3 | Mannitol Sodium Lauryl Sulphate (SLS) | Agar |
| 4 | Ion exchange resins | Pectin |
| 5 | Soy Polysaccharide | Mangifera Indica gum |
| 6 | Cross linked alginic acid | Hibiscus rosa sinensis mucilage |
| 7 | Microcrystalline cellulose(MC) | Isapghula husk and mucilage |
Table 2. List of commonly used Super disintegrants for FDTs formulations.
Selection of Super Disintegrants
Disintegrants are substances or mixture of substances added to the drug formulation so as to facilitate the breakup or disintegration of tablet or capsule content into smaller particles that dissolve more rapidly than in the absence of disintegrants. Superdisintegrants are generally used at a low concentration in solid dosage form, typically 1% to 10% by weight relative to the total weight of the dosage unit. Rapid disintegration of the FDTs is due to the penetration of saliva into the pores of the tablet, which lead to the swelling of super disintegrates to create enough hydrodynamic pressure for quick and complete disintegration of the tablet. Table 1 shows composition of different FDTs with varying super disintegrants. Majority of the studies (34 out of 42) as shown in Figure 2, used crosspovidone in different combinations. The most suitable concentration of crosspovidone used for the formulation of FDTs varies from 5% to 10% w/w.
Figure 2. Shows that Use of different superdisintegrants in formulation of FDTs in published studies from 2001-2016.
Table 1 shows that natural super disintegrants are also used widely for the formulation of FDTs. In sixty selected studies, 8 studies used natural super disintegrates viz Gellan gum, Xanthan gum, Husk, Agar Pectin. Out of these studies, five studies used husk of Plantago ovata as Super disintegrants. This showed that Planta ovata can be considered best superdisintegrants among all natural superdisintegrants. Similar finding reported earlier by Yadav et al. concluded that natural super disintegrants like husk of Plantago ovata showed better disintegrating property than the most widely used synthetic super disintegrants like AC-di-Sol, CP and SG in the formulations of FDTs (Figure 2).
Conventional Used Technique for FDTs
Various techniques used in preparation of fast dissolving tablets include; direct compression, wet granulation, dry granulation, sublimation, solid dispersion, vacuum drying, molecular dispersion granule, solvent evaporation, and effervescence.
In the sixty published reports, 36 studies used direct compression (DC) method for formulation of FDTs. DC is the simplest and most cost-effective tablet manufacturing technique for MDTs as they can be formulated using conventional tablet making machine and easily available tableting excipients. Data from present study showed that molecular dispersion granule (MDG), dry granulation (DG), solvent evaporation (SE) are least used techniques for formulation of FDTs (Figure 3).
The FDTs have potential advantages over conventional dosage forms. With their improved patient compliance, convenience, bioavailability, and rapid onset of action, they have drawn the attention of many pharmaceutical industries over a decade. The present study, for the first time provides complete database for fast dissolving tablet and their formulations. This study shows that majority of FDTs have been successfully formulated by direct compression method and evaluated for most of the classes of drugs with varying concentration of superdisintegrants. Most widely used superdisintegrants among synthetic and natural ones are crosspovidone and Plantago ovata respectively. A wide range of drugs (analgesics, anti cancer, GIT drugs, antimicrobial, antiviral, respiratory drugs, CNS drugs, anti allergic drugs, antidiabetic drugs etc) can be considered for this dosage form. The highest number hits NSAID, analgesics and cardiovascular drugs including antihypertensive drugs.
There is no conflict of interest and authors have nothing to disclose
Ms Sakshi Saxena generated data and helped write the paper. Dr Nikku Yadav conceived the idea and designed work and write paper.
We gratefully acknowledge Apeejay Education Society for providing facilities.