AUCTORES
Research Article | DOI: https://doi.org/10.31579/2693-7247/005
Hospital Universitario Central de Asturias (HUCA)Avda. de Roma, Oviedo. Asturias, Spain.
*Corresponding Author: Prasad Garrepally – Jangaon Institute of Pharmaceutical Sciences, Depot. Of Pharmaceutics, Jangaon, India.
Citation: Prasad Garepally. (2018) Design, Development and Characterizations of Acyclovir Osmotic Tablets. J. Pharmaceutics and Pharmacology Research. 1(1) DOI: 10.31579/2693-7247/005
Copyright: © 2018 Prasad Garrepally. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
Received: 18 September 2018 | Accepted: 06 October 2018 | Published: 08 October 2018
Keywords: Keywords
Oral drug delivery is the most widely utilized route of administration, among all the routes of administration. That has been explored for the systemic delivery drug through different pharmaceutical dosage forms. It can be said that at least 90%of all drugs used to produce systemic effect is by oral route.
Conventional oral drug delivery systems are known to provide an immediate release of drug, in which one cannot control the release of the drug and effective concentration at the target site.
Oral drug delivery is the most widely utilized route of administration, among all the routes of administration. That has been explored for the systemic delivery drug through different pharmaceutical dosage forms. It can be said that at least 90%of all drugs used to produce systemic effect is by oral route.
Conventional oral drug delivery systems are known to provide an immediate release of drug, in which one cannot control the release of the drug and effective concentration at the target site. The bioavailability of drug from these formulations may vary significantly, depending on factors such as physico-chemical properties of the drug, presence of excipients, various physiological factors such as the presence or absence of food, pH of the GI tract, GI motility, etc. so overcome this limitation of oral route is replied by parenteral route. This route offers the advantage of reduced dose, targeting of site and avoiding GI stability, hepatic by-pass of drug molecule. (Leon, L., et al., 1986)
In the recent years, pharmaceutical research has led to the development of several novel drug delivery systems. The role of drug development is to take a therapeutically effective molecule with sub-optimal physicochemical and/or physiological properties and develop an optimized product that will still be therapeutically effective but with additional benefits such as:
Based on the mechanism of the drug release can be classified as:
The most of novel drug delivery systems are prepared using matrix, reservoir or osmotic principle. In matrix systems, the drug is embedded in a polymer matrix and the release takes place by partitioning of drug into the polymer matrix and the surrounding medium. In contrast, reservoir systems have a drug core surrounded by a rate controlling membrane. The osmotic systems utilize the principles of osmotic pressure for the delivery of drugs in both the routes oral as well as Parenteral.
Controlled release (CR) technology has rapidly emerged over the past few decades as a new field offering approaches to the delivery of drugs into systemic circulation at predetermined rate. CR formulations can achieve optional therapeutic responses, prolonged efficacy as well as decrease toxicity duo to achieving predictable and reproducibility release rate of drugs for extended period of time.
Among all the routes of administration that have been explored for the development of controlled release (CR) systems, the reasons the oral route has attained the apex, because of obvious reasons. The reasons that the oral route achieved such popularity may be in fact attributed to its ease of administration as well as the traditional belief that by oral route of administration the drug is well absorbed as the food stuffs that are ingested regularly.
CR delivery systems provide desired concentration of drug at the absorption site permitting maintenance of plasma concentration within the therapeutic range and reducing dosing frequency. CR products provide significant benefits over immediate release formulations including greater effectiveness in the treatment of chronic conditions, reduced side effects, and greater patient convenience due to a simplified dosing schedule.
In recent years, much attention has focused on novel drug delivery systems (NDDS). This is mainly due to low developmental cost and time required for creating a NDDS is also low. In contrast to conventional drug delivery systems, these systems will have number of advantages like increasing the market value, competitiveness and patients compliance.
There are many Novel drug delivery systems are in the market, per oral controlled release (CR) systems hold the major part in market share due to its obvious advantages like ease of administration and better patient compliance.(Verma., et al., 2001).
There are many designing options available to control or modify the drug release from a dosage form. Numerous technologies have been used to control the systemic delivery of drugs. One of the most interesting one is that employs osmotic pressure as an energy source for release of drugs.
Principles of osmosis
The first report of an osmotic effect dates to Abbe Nollet (1748), but pfeffer obtained the first quantitative measurements in 1877. In Pfeffer’s experiment, a membrane permeable to water but impermeable to sugar was used to separate a sugar solution from pure water .A flow of water then takes place into the sugar solution that cannot be halted until a pressure π is applied to the sugar solution. Pfeffer showed that this pressure, the osmotic pressure π of the sugar solution, is directly proportional to the solution concentration and the absolute temperature.
The phenomenon of confining a solution to a membrane, permeable only to the solvent molecules, is known as osmosis and the membrane that allows only the solvent molecules to pass throught it is known as semipermeable membrane (SPM). Therefore osmosis can be defined as the passage of solvent molecules into a solution (containing both solute and solvent molecules) thought SPM or passage of solvent molecules usually water takes place from the SPM from a region of lower concentration to higher concentration. This principle equalizes the escaping tendency of the solvent molecules, which is due to the difference in chemical potential across the SPM. It should be evident that osmosis can also take place when a concentrated solution is separated from a less concentrated solution by a semipermeable membrane. Thus passage of solvent (water) molecules continues until the osmosis pressure of the system i.e., inside and outside compartment becomes equal.
The principle of osmosis can be better understood by the application of the Van’t Hoff equation, which suggests proportionality between osmosis pressure, concentration and temperature. According to Van’t Hoff’s equation, the osmosis pressure of a dilute solution will be equal to the pressure that solute would exert if it were a gas, occupying the same volume.
π V= nRT (1)
Where π stands for osmosis pressure in atm, V stands for volume of solution in liters, n stands for the number of moles of solute, R stands for gas constant(0.082 liter atm/mole deg), and T stands for absolute temperature.
π = nRT/V (2)
Osmosis pressure, like vapour pressure and boiling point is a colligative property of solution in which a non-volatile solute is dissolute in a volatile solvent.
Osmosis pressure can be defined as the pressure exerted as a result of osmosis or the pressure with which the solvent molecules cross from the semipermeable membrane or the required to stop the flow of solvent molecules from crossing the SPM is known as osmosis pressure.
The flow of solvent depends on SPM characteristics and different osmosis pressures between two sides of regions.
Osmosis pressure for concentrated solution of soluble solutes commonly used in controlled release formulation are extremely high, ranging from 30 atm for sodium phosphate up to 500 atm for a lactose-fructose mixture (US patent number 4077407). These osmosis pressures can produce high water flows across semipermeable membrane. The osmotic water influx into osmosis pump across the SPM is given by the equation |
dv / dt = A / h Lp (σ∆π-∆ρ) C (3)
where dv/dt is water influx, A and h are the membrane area and membrane thickness, respectively, Lρ is mechanical permeability, σ is the reflection coefficient and ∆π and ∆ρ are the osmosis and hydrostatic pressure difference respectively, between the inside and outside of the system, C is the concentration of compound in the dispensed fluid. As the size of the delivery orifice increases, hydrostatic pressure inside the system is minimized (∆π > ∆ρ). Also, when the osmotic pressure of the formulation is large compared to the osmotic pressure of the environment, p can be substituted for Dp. Equation 1 then reduces to a much simpler expression in which constant K replaces the product Lp. After simplification, the following equation is obtained:
dM/dt= (A/h)Kp × C (4)
The release rate defined by Eq. 4 remains zero order as long as the terms in the equation remain constant. The first three terms on the right-hand side of Eq. 4 can be maintained constant through proper selection and optimization of the SPM. Therefore, a constant release of drug from the device is maintained as long as excess solid agent is present inside the device to maintain both p and C in Eq. 4 at constant levels. (Santus, G., et al., 1995)
Historical aspects of osmotic pumps
About 75 years after discovery of the osmosis principle, it was first used in the design of drug delivery systems. Rose and Nelson, the Australian scientists, were initiators of osmotic drug delivery. (Rose.,Nelson, J.F., 1955)
In 1955, they developed an implantable pump, which consisted of three chambers: a drug chamber, a salt chamber contains excess solid salt, and a water chamber. The drug and water chambers are separated by rigid semipermeable membrane. The difference in osmotic pressure across the membrane moves water from the water chamber into the salt chamber. The volume of the salt chamber increases because of this water flow, which distends the latex diaphragm separating the salt and drug chambers, thereby pumping drug out of the device.
Fig 1: Schematic diagram of Rose and Nelson pump
Higuchi-Leeper pump
The design of Higuchi-Leeper pump represents the first simplified version of Rose-Nelson osmosis pump made by the Alza Corporation beginning in the early 1970s. An example of the one the pump is shown in Fig 2.
The Higuchi-Leeper pump has no water chamber, and device is activated by water imbibed from the surrounding environment. This means the pump can be prepared loaded with drug and then stored for weeks or months prior to use. The pump is activated when it is swallowed or implanted in the body. Higuchi- Leeper pumps contain a rigid housing and the semipermeable membrane is supported on a perforated frame. This type of pump usually has a salt chamber containing a fluid solution with excess solid salt.
Fig 2: Schematic diagram of Higuchi-Leeper pump
Higuchi-Theeuwes Pump
In the early 1970s, Higuchi and Theeuwes developed another, even simpler variant of the Rose-Nelson pump. In the Higuchi-Theeuwes device, however, the rigid housing is dispensed with and the membrane acts as the outer casing of the dump. This membrane is quite sturdy and is strong enough to withstand the pumping pressure developed inside the device. The device is loaded with the desire drug prior to use. When the device is placed in an aqueous environment, release of the drug follows a time course set by the salt used in the salt chamber and the permeability of the outer membrane casing. Most of the Higuchi-Theeuwes pumps use a dispersion of solid in suitable carrier for the salt chamber of the device.
Fig 3: Schematic diagram of Higuchi-Theeuwes Pump
Elementary osmotic pump
In 1975, the major leap in osmotic delivery occurred as the elementary osmotic pump for oral delivery of drugs was introduced. The pump consists of an osmotic core containing the drug, surrounded by a semipermeable membrane with a delivery orifice. When this pump is exposed to water, the core imbibes water osmotically at a controlled rate, determined by the membrane permeability to water and by the osmotic pressure of the core formulation. As the membrane is non-expandable, the increase in volume caused by the imbibition of water leads to the development of hydrostatic pressure inside the tablet. This pressure is relieved by the flow of saturated solution out of the device through the delivery orifice. This process continues at a constant rate until the entire solid agent inside the tablet has been dissolved and only a solution filled coating membrane is left. This residual dissolved agent continues to be delivered at a declining rate until the osmotic pressure inside and outside the tablet are equal. Normally, the Elementary osmotic pump delivers 60-80% of its contents at a constant rate, and there is a short lag time of 30-60 min as the system hydrates before zero order delivery from the Elementary osmotic pump is obtained. (Theeuwes, F., 1975)
Fig 4: Schematic diagram of Elementary osmotic pump
Push pull Osmotic Pump
Push-pull osmotic pimp (PPOP) can be used for delivery of drugs having extremes of water solubility. As shown below fig 5. It is bilayer tablet coated with a SPM.
Drug along with osmagents is present in the upper compartment whereas lower compartment consists of polymeric osmotic agents.The drug compartment is connected to the
outside environment via a delivery orifice. After coming in contact with the aqueous environment, polymeric osmotic layer swells and pushes the drug as fine dispersion via the orifice.
A number of modifications are available for this type of system such as delayed push-pull system (as used in covera HS, extended release for verapamil), multi-layer push-pull system (for pulsatile or delayed drug delivery), and push-stick system (for delivery of insoluble drugs requiring high loading, with an optional delayed, patterned or pulsatile release profile ). (Wrong., et al., 1986)
Fig 5: Schematic diagram of Push pull Osmotic Pump
Controlled porosity Osmotic Pumps (CPOP)
Controlled porosity osmotic pumps (CPOP) are similar to elementary osmotic pump, the only difference being that the delivery orifice from which the drug release takes place is formed by incorporation of a water-soluble additive in the coating. Once the tablet comes in contact with the aqueous media in the gastrointestinal tract (GIT), the water-soluble component dissolves and an osmotic pumping system results as shown below in Fig 6(Zentner, G.S., et al., 1985
Nevertheless, the solubility of the agents to be delivered can be modulated, and these systems can be designed to deliver drugs having extremes of water solubility (Verma, R.K., et al., 1999).
The modification required depends mainly upon the dose intrinsic water solubility and osmotic pressure, and desired release rate of the drug.
Fig 6: Schematic diagram of Controlled porosity Osmotic Pumps (CPOP)
OROS CT System
The OROS-CT TM system was designed for colon-targeted drug delivery. The system either comprises a single osmotic unit or it might contain as many as push-pull units enclosed within a hard gelatin capsule, immediately after ingestion the hard gelatin capsule shell dissolves. However, the push pull unit is prevented from absorbing water in the acidic environment of the stomach by the enteric coating. The osmotic pumping action results when the coating dissolves in the higher pH environment (pH>7) of the small intestine and the drug is delivered out of the orifice at a rate controlled by the rate of water transport across the membrane.
A class of osmotic pump is also designed to deliver liquid formulation. In the liquid OROSR or L-OROSR SOFTCAP TM, the liquid drug formulation is present in a soft gelatin capsule, which is surrounded with the barrier layer, the osmotic layer, and the release rate –controlling membrane.
The L-OROSR HARDCAPTM is similar to the L-OROSR SOFTCAPTM comprising a drug suspension in a self-emulsifying formulation (SEF) to enhance the oral bioavailability of hydrophobic drugs. (Dong, L., et al., 2001)
Swellable core technology (SCT) is a new emerging field in osmotic drug delivery that can deliver drugs with moderate or poor aqueous solubility per and extended period of time. The SCT formulation consists of a core tablet that contains a drug composition and a water swellable composition. The drug composition contains the drug, an entraining polymer like polyethylene oxide, and osmotic agents. Whereas the swellable portion contains a non-ionic polymer (PEO) or and ionic polymer (croscamellose sodium or sodium starch glycolate) which swells and expands in volume after absorption of water. The drug composition may also contain solubilizers for example buffering agent which solubilize the drug by maintaining a pH environment that helps in drug dissolution and absorption. Furthermore, the drug and water swellable composition may contain other ingredients to improve the flow and compression characteristics of the blends, aiding in the preparation of tablets. In general, the components used in SCT formulation are safe commonly used in pharmaceutical products and available in pharmaceutical grades.
The drugs and water swellable composition in SCT formulation can be designed in various configurations. For example, they can be mixed together resulting in a uniform homogeneous core, or they can be physically separated from each other resulting in a layered configuration. The tablets cores are coated with a film coat of cellulose acetate of proper acetyl content and polyethylene glycol from an acetone – water solvent system. The film coating is them drilling either using a laser or a mechanical drill or slits are made to produce one or more exit ports for the release of drug.
The sandwich osmotic tablet system (SOTS) is composed of a sandwich osmotic tablet core (made of a middle push layer and two attached drug layers) surrounded by an SPM with two orifices on both side surface. After coming contact with the aqueous environment, the middle push layer containing swelling agents’ swells and the drug is released from the delivery orifices. Because the system delivers from two opposite orifices, rather from the single orifices of the PPOP, it may decrease the potential local irritation of the drug (Liu, L., et al., 2000).
Asymmetric membrane capsules were developed in which the drug delivery device consists of a drug-containing core surrounded a membrane which has an asymmetric structure. i.e., it has a relatively thin, dense region supported on a thicker porous region. The capsule wall is made from a water insoluble polymer such as cellulose acetate. Unlike a conventional gelatin capsule the asymmetric membrane capsule does not dissolve immediately after ingestion. But it provides prolonged release of the active ingredient incorporated in the capsule.
(Cardinal, J.R., et al.,1997)
Fig 7: Schematic diagram of OROS CT System
FACTORS AFFECTING DRUG RELEASE RATE
Before discussing the formulation variables that affect the release of oral osmotic systems, it will be prudent to deal with some of the theoretical aspects. The delivery of agent from oral osmotic systems is controlled by the influx of solvent across the SPM, which in turn carries the agent to the outside environment. (Martin, A.,1993)
Solubility:
It can be seen from Eq. 4 that the delivery rate of a drug from an osmotic pump depends to a large extent on the solubility of drug at saturation. Candidate drugs for osmotic delivery have water solubility in the range 50–300 mg/ml. However, by modulating the solubility of these drugs within the core, effective release patterns may be obtained for the drugs, which might otherwise appear to be poor candidates for an OCODDS.
Use of swellable polymers
Vinyl acetate copolymer, polyethylene oxide have uniform swelling rate which causes drug release at constant rate.
Use of wicking agents
These agents may enhance the surface area of drug with the incoming aqueous fluids. E.g. colloidal silicon dioxide, sodium Lauryl sulfate, etc. Ensotrol technology uses the same principle to deliver drugs via osmotic mechanism.
Use of effervescent mixtures
Mixture of citric acid and sodium bicarbonate which creates pressures in the osmotic system and ultimately controls the release rate.
Resin Modulation approach
Ion-exchange resin methods are commonly used to modify the solubility of APIs. Some of the resins used in osmotic systems are Poly (4-vinyl pyridine), Pentaerythritol, citric and adipic acids.
Use of crystal habit modifiers
Different crystal form of the drug may have different solubility, so the excipients which may change crystal habit of the drug can be used to modulate solubility.
Co-compression of drug with excipients
Different excipients can be used to modulate the solubility of APIs with different mechanisms like saturation solubility, pH dependent solubility. Examples of such excipients are organic acids, buffering agent, etc.
OSMOTIC PRESSURE
Osmotic pressure is of a solution depending on number of discrete entities of solute presents in the solution. The release rate of a drug from a osmotic system is directly proportional to the osmotic pressure of the sore formulation in EOP design or in the drug reservoir of agent reservoir-osmotic engine- SPM design (e.g., AlzetR osmotic pump). For controlling drug release from these systems, it is important to optimize the osmotic pressure gradient between the inside compartment and the external environment. It is possible to achieve maintain a constant osmotic pressure by maintaining solution of osmotic agent in the core compartment. If a drug does not possess sufficient osmotic pressure, an osmotically active agent can be added to the formulation.
Water-soluble salts of organic acids (sodium potassium acetate, magnesium succinate, sodium benzoate, sodium citrate, sodium ascrobate etc.), water-soluble amino acids (glycine, leucine, alanine, methionine) and organic polymeric osmogens (sodium carboxy methylcellulose, HPMC, hydroxyethy1, methy1 cellulose, cross-linked PVP, polyethylene oxide (PEO), carbopols, polyacry1 amides) can be used as osmogens. (Srinath, P., et al., 1998)
TABLE 1: LIST OF COMPOUND THAT CAN BE USED AS OSMOGENS
Category |
Compound or Mixture |
Osmotic pressure (atm) |
Water-soluble salt of inorganic acids | Potassium chloride | 245 |
Potassium sulfate | 39 | |
Potassium hydrogen phosphate | 105 | |
Sodium hydrogen phosphate | 28 | |
Sodium chloride | 356 | |
Carbohydrates | Mannitol | 38 |
Sucrose | 150 | |
Lactose-fructose | 500 | |
Dextrose-fructose | 450 | |
Sucrose-fructose | 430 | |
Fructose | 23 | |
Lactose | 82 | |
Dextrose | 415 | |
Mannitol-fructose | 130 | |
Mannitol-lactose | 170 | |
Mannitol-sucrose | 225 | |
Mannitol-dextrose | 225 | |
Lactose-dextrose | 225 | |
Inorganic sodium salts | Sodium phosphate tribasic, 12 H2o | 36 |
Sodium phosphate dibasic 7H2o | 31 | |
Sodium phosphate monobasic, H2o | 28 | |
Sodium phosphate dibasic, 12H2o | 31 | |
Sodium phosphate dibasic anhydrous | 29 | |
Othermiscellaneous substances | Citric acid | 69 |
Trataric acid | 67 | |
Fumaric acid | 10 | |
Adipic acid | 8 | |
Sorbitol | 84 | |
Xylitol | 104 | |
Maleic acid | 117 |
Osmotic System Pressures are:
LASER DRILLING
Laser drilling is one of the most commonly used techniques to create deliver orifice in the osmotic tablets. In simple words, the tablets in which holes are to be formed are changed in the hopper. The tablets drop by gravity into the slots of the rotation feed wheel are carried at a predetermined velocity to the passageway forming station. The walls of the tablets absorb the energy of the beam and gets heated ultimately causing piercing of the wall and, thus forming passageway. After completion, the tracking mirror oscillation counterclockwise back to its starting position to track the next tablet. It is possible to control the size of the passageway by varying the laser power, firming duration (pulse time), thickness of the wall, and the dimension of the beam at the wall.
Systems with passageway formed in situ
Oral osmotic systems in which delivery passageway is formed in situ are described in US patent No. 5,736,159 (Chen et al,. 1982)
The system described consists of a tablet core of the drug along with the water swellable polymers and osmotic agents, which surrounded by a rate-controlled membrane. In contact with the aqueous environment, water is imbibed osmotically at a controlled rate and water swellable polymer expands as the osmotic agents dissolves and increases the osmotic pressure inside the tablets. This results in a rate-controlled slight expansion of the partially hydrates core. The expansion of core cause a small opening to form at the edge of the tablets (weakest point in the membrane) from where the contents of the formulation are released. In the working examples, core tablets of nifedipine were prepared using polyethylene oxide as a water swellable agent and coated with a rate controlling membrane. The osmotic systems were able to maintain plasma concentration of the drug within the therapeutic range for 24 hrs.
Use of modified punches
Use of modified punches for producing a delivery orifice in osmotic dosage forms has also been described in the literature.
The dosage form is pierced using a piercing and unsheathed upon application of compression force. The coating powder top be compressed in charged to the die mold and unpierced tablet core is placed upon it. Additional quotation of coating powder is added to the die mod, subsequent to which both compression and piercing are done simultaneously. (A.D.Ayer et al., 1991)
Use of pore formers
CPOP are extension of EOPs and are essentially similar, expect that there is no need to create a delivery orifice, drug release from these types of system takes place through controlled porosity pores formed in situ. In corporation of water-soluble additive in the membrane wall is the most widely reported method for the formation of pores in CPOP (G.M Zentner et al., 1990; J.L.Haslam et al., 1989).
These water soluble additives dissolve on coming in contact with water, leaving behind pores in the membrane through which drug release takes place. Drug release from these types of system is independent of pH and has been shown to follow zero-order kinetics (Zentner et al., 1985).
These erodible or leachable materials produce one or more passageways with difference geometrical shapes. The pores may also be formed in the wall prior to the operation of the systems by has formation within curing polymer solution, resulting in voids and pores in the final form of the membrane. The pores may also be formed in the walls by the volatilization of components in the polymer solution or by chemical reaction in the polymer solution leading to evaluation of gases prior to application or drugging application of the solution to the core tablets resulting in the creation of the polymer foams serving as the porous wall from where the drug release can take place (Zentner et al., 1990).
Membrane type and characteristics
The choice of a rate-controlling membrane is an important aspect in the formulation development of oral osmotic systems. Recalling Eq.4, which describes the volume flow, one can easily recognize the importance of the SPM in controlling release of the drug. The membrane must possess certain performance criteria (Theeuwes.F., 1975)
Type and nature of polymer
Since the membrane in osmotic systems is semipermeable in nature, any polymer that is permeable to water but impermeable to solute can be selected. Some of the polymers that can be used for above purpose include cellulose esters such as cellulose acetate, cellulose diaceate, cellulose triacetate, cellulose propionate, cellulose acetate butyrate, etc. Cellulose ethers like ethyl cellulose and eudragits.
Table 2: List of semipermeable polymers with their water
Polymer membrane | Water vapour transmission rates |
Polyvinyl alcohol | 100 |
Polyurethene | 30-150 |
Ethylcellulose | 75 |
Methylcellulose | 70 |
Cellulose acetate | 40-75 |
Cellulose acetate butyrate | 50 |
Polyvinylchloride(cast) | 10-20 |
Polyvinylchloride(extruded) | 6-15 |
Polycarbonate | 8 |
Ethylene vinyl acetate | 1-3 |
Poly vinyl chloride | 1 |
Polypropylene | 0.7 |
Ethyl cellulose is also widely used in the formulation of membranes for oral osmotic systems. However, the water permeability of pure ethyl cellulose membrane is very low that may result in slow release in slow release of the drugs. Nevertheless, drug release from osmotic systems coated with ethyl cellulose membrane can be enhance by the incorporation of water-soluble additives addition of HPMC in the coating composition improves the permeability of ethyl cellulose membranes. Tablets core of potassium chloride coated with a mixture of ethyl cellulose and up to 24% of HPMC were shown to release the contents mainly through osmotic mechanism. (B. Lindstedt et al., 1989)
Effect of type of plasticizer on release profile
Plasticizers can change viscoelastic behavior of polymers significantly. In particular, plasticizers can turn a hard and brittle polymer into a softer, more pliable material, and possibly make it more resistant to mechanical stress. These changes also affect the permeability of polymer films. The effect of different types of plasticizers (TA and polyethylene glycols) on the water permeation and mechanical properties were studied. The water permeability of CA films was found to decrease with increasing plasticizer concentration to a minimum and then increases with higher concentration of plasticizer.( J. Guo.1993)
Thickness of the membrane has a profound effect on the drug release from osmotic systems. It can be seen Eq. 4, that release rate from osmotic systems is inversely proportional to membrane thickness. Pellets of phenylpropanolamine coated with aqueous ethyl cellulose based films were found to release drugs mainly through the mechanism of osmotic pumping and diffusion. (Ozturk,A.G. et al., 1990).
On studying the release as function of coating thickness, it was found that as the coating thickness increased from 9 to 50 µm, the drug release decreased in an inversely proportional manner. In case of monolithic osmotic tablets of nifedipine, release rates were found to decrease with increase in membrane thickness from 85 to 340µm (L. Liu et al., 2000).
An increased resistance of the membrane to water diffusion resulted in this effect.
On the other hand, thickness of the membrane in case of asymmetric coating was found to have insignificant effect on drug release. Release rates were found to be virtually unaffected by the overall membrane thickness in the range of 95-150 µm. (Herbig S.M. et al., 1995)
Evaluation of Osmotically controlled drug delivery systems
Over the past few years there is increase in the development and commercialization of controlled-release dosage forms has necessitated changes in evaluation aspects of them. This is to provide in-house quality control tests and to furnish regulatory agencies with the experimental evidence that the dosage forms delivers the drug in a controlled and reproducible manner. There is a need for establishing in-vitro-in-vivo correlations to simulate the drug evaluation in the in-vivo system. [Hanlon J C et al., 2008]
ADVANTAGES
A part from the general advantages shared by conventional CR systems. OCODDSs have several other unique advantages. Osmotic delivery is a versatile technology that can be used as a powerful research tool to determine various pharmacokinetic parameters and pharmacodynamic response of drugs in animals and humans.
1. Delivery of drug from osmotic pumps can be designed to follow true Zero-order Kinetics. Constant delivery rate is an important specification for chronic treatment. In addition, based upon the requirements, drug delivery can be modulated to achieve pulsatile or delayed zero-order delivery.
2. Drug release from osmotic pumps is minimally affected by the gastric pH and hydrodynamic condition of the body. This is mainly because of the special properties of this semi-permeable membrane employed in the coating of osmotic formulations. The delivery rate is independent of the variation in pH throughout the GIT and GI motility.
3. Higher release rates can be obtained from osmotic systems than with conventional diffusion based drug delivery systems.
4. The delivery of drug takes place in solution form, which is ready for absorption. Thus it is an in situ prepared liquid dosage form.
5. It is possible design an osmotic pump for drug with wide range of water solubility.
6. The delivery rate of drug(s) from these systems is highly predicable and programmable. The in vitro rate can be accurately predicated since the system well described by the equation.
7. A high degree of in vitro/in-vivo correlation can be obtained from osmotic pumps. The Significant in vitro and in vivo correlation for a verapamil oral osmotic system was studied. (Gupta et al. 1996)
8. Drug release from the osmotic systems is minimally affected by the presence of food.
EXCIPIENT PROFILE
CELLULOSE ACETATE
1. Nonproprietary Names
• BP: Cellulose acetate
• PhEur: Cellulosi acetas
• USPNF: Cellulose acetate
2. Synonyms
Acetyl cellulose; cellulose diacetate; cellulose triacetate.
3. Chemical Name
Cellulose acetate
Cellulose diacetate
Cellulose triacetate
coatings on tablets or granules for taste masking.
5. Description
Cellulose acetate occurs as a white to off-white powder, free-flowing pellets, or flakes. It is tasteless and odorless, or may have a slight odor of acetic acid.
6. Stability and Storage Conditions
Cellulose acetate is stable if stored in a well-closed container in a cool, dry place. Cellulose
acetate hydrolyzes slowly under prolonged adverse conditions such as high temperature and
humidity, with a resultant increase in free acid content and odor of acetic acid.
7. Incompatibilities
Cellulose acetate is incompatible with strongly acidic or alkaline substances. Cellulose
acetate is compatible with the following plasticizers: diethyl phthalate, polyethylene glycol,triacetin, and triethyl citrate.(handbook of excipients)
POTASSIUM CHLORIDE
5. Applications in Pharmaceutical Formulation or Technology:
• Potassium chloride is widely used in a variety of parenteral and nonparenteral pharmaceutical formulations. Its primary use, in parenteral and ophthalmic preparations, is to produce isotonic solutions.
• Potassium chloride is also used therapeutically in the treatment of hypokalemia Many solid-dosage forms of potassium chloride exist including: tablets prepared by direct compression1–4 and granulation;5,6 effervescent tablets; coated, sustained-release tablets;7–10 sustained-release wax matrix tablets;11 microcapsules;12 pellets; and osmotic pump formulations.13,14
• Experimentally, potassium chloride is frequently used as a model drug in the development of new solid-dosage forms, particularly for sustained-release or modified-release products. Potassium chloride is also used widely in the food industry as a dietary supplement, pH control agent, stabilizer, thickener, and gelling agent. It can also be used in infant formulations.
6. Description
Potassium chloride occurs as odorless, colorless crystals or a white crystalline powder, with an unpleasant, saline taste. The crystal lattice is a face-centered cubic structure.
7. Solubility:
Table 3: Solubility of KCl
Solvent | Solubility at 20°C unless otherwise stated |
Acetone | Practically insoluble |
Ethanol (95%) | 1 in 250 |
Ether | Practically insoluble |
Glycerin | 1 in 14 |
Water | 1 in 2.8 1 in 1.8 at 100°C |
8. Stability and Storage Conditions
Potassium chloride tablets become increasingly hard on storage at low humidities. However, tablets stored at 76% relative humidity showed no increase or only a slight increase in hardness and hardness on aging.2 Aqueous potassium chloride solutions may be sterilized by autoclaving or by filtration. Potassium chloride is stable and should be stored in a well-closed container in a cool, dry place. (Parikh, M.,)
9. Incompatibilities
Potassium chloride reacts violently with bromine trifluoride and with a mixture of sulfuric acid and potassium permanganate. The presence of hydrochloric acid, sodium chloride, and magnesium chloride decreases the solubility of potassium chloride in water. Aqueous solutions of potassium chloride form precipitates with lead and silver salts. Intravenous aqueous potassium chloride solutions are incompatible with protein hydrolysate.
10.Method of Manufacture
Potassium chloride occurs naturally as the mineral sylvite or sylvine; it also occurs in other minerals such as sylvinite, carnallite, and kainite. Commercially, potassium chloride is obtained by the solar evaporation of brine or by the mining of mineral deposits.
Mannitol
Functional Category
Confectionery base; coating agent; granulation aid; suspending agent; sweetening agent; tablet binder; tablet and capsule diluent; tablet filler; therapeutic agent; viscosity-increasing agent.
Applications in Pharmaceutical Formulation or Technology
Sucrose is widely used in oral pharmaceutical formulations. Sucrose syrup, containing 50–67% w/w sucrose, is used in tableting as a binding agent for wet granulation. In the powdered form, sucrose serves as a dry binder (2–20% w/w) or as a bulking agent and sweetener in chewable tablets and lozenges. That contain large amounts of sucrose may harden to give poor disintegration.
Sucrose syrups are used as tablet-coating agents at concentra-tions between 50% and 67% w/w. With higher concentrations, partial inversion of sucrose occurs, which makes sugar coating difficult. Sucrose syrups are also widely used as vehicles in oral liquid-dosage forms to enhance palatability or to increase viscosity. Sucrose has been used as a diluent in freeze-dried protein products. Sucrose is also widely used in foods and confectionery, and therapeutically in sugar pastes that are used to promote wound healing.
Sucrose
Description
Sucrose is a sugar obtained from sugar cane (Saccharum officinarum Linne ´ (Fam. Gramineae)), sugar beet (Beta vulgaris Linne ´ (Fam. Chenopodiaceae)), and other sources. It contains no added substances. Sucrose occurs as colorless crystals, as crystalline masses or blocks, or as a white crystalline powder; it is odorless and has a sweet taste.
MICROCRYSTALLINE CELLULOSE:
Use | Concentration (%) |
---|---|
Adsorbent | 20–90 |
Antiadherent | 5–20 |
Capsule binder/diluents | 20–90 |
Tablet disintegrant | 5–15 |
Tablet binder/diluents | 20–90 |
Description
Microcrystalline cellulose is purified, partially depolymerized cellulose that occurs as a white, odorless, tasteless, crystalline powder composed of porous particles. It is commercially available in different particle sizes and moisture grades that have different properties and applications.
Solubility
slightly soluble in 5% w/v sodium hydroxide solution; practically insoluble in water, dilute acids, and most organic solvents.
Stability and Storage Conditions
Microcrystalline cellulose is a stable though hygroscopic material. The bulk material should be stored in a well-closed container in a cool, dry place.
Incompatibilities
Microcrystalline cellulose is incompatible with strong oxidizing agent. (Owen S.et al.)
POVIDONE (PVP)
Applications in Pharmaceutical Formulation or Technology
Although povidone is used in a variety of pharmaceutical formulations, it is primarily used in solid-dosage forms. In tableting, povidone solutions are used as binders in wet-granulation processes. Povidone is also added to powder blends in the dry form and granulated in situ by the addition of water, alcohol, or hydroalcoholic solutions. Povidone is used as a solubilizer in oral and parenteral formulations and has been shown to enhance dissolution of poorly soluble drugs from solid-dosage forms Povidone solutions may also be used as coating agents. Povidone is additionally used as a suspending, stabilizing, or viscosity-increasing agent in a number of topical and oral suspensions and solutions. The solubility of a number of poorly soluble active drugs may be increased by mixing with povidone. [Parikh, M.]
Uses
Table 5: Uses of povidone in percentage concentration
Use | Concentration (%) |
Carrier for drugs | Carrier for drugs |
Dispersing agent | Up to 5 |
Eye drops | 2–10 |
Suspending agent | Up to 5 |
Tablet binder, tablet diluent, or coating agent | 0.5–5 |
Description
Povidone occurs as a fine, white to creamy-white colored, odorless or almost odorless, hygroscopic powder. Povidone with K-values equal to or lower than 30 are manufactured
by spray-drying and occur as spheres. Povidone K-90 and higher K-value povidone are manufactured by drum drying and occur as plates.
MAGNESIUM STEARATE
Applications in Pharmaceutical Formulation or Technology
Magnesium stearate is widely used in cosmetics, foods, and pharmaceutical formulations. It is primarily used as a lubricant in capsule and tablet manufacture at concentrations between 0.25% and 5.0% w/w. It is also used in barrier creams.
Description
Magnesium stearate is a very fine, light white, precipitated or milled, impalpable powder of low bulk density, having a faint odor of stearic acid and a characteristic taste. The powder is greasy to the touch and readily adheres to the skin.
TRIETHYL CITRATE
Functional Category: Plasticizer.
Applications in Pharmaceutical Formulation or Technology
Triethyl citrate and the related esters acetyltriethyl citrate, tributyl citrate, and acetyltributyl are used to plasticize polymers in formulated pharmaceutical coatings.
The coatingapplications include capsules, tablets, beads, and granules for taste masking , immediaterelease, sustained-release, and enteric formulations.
Triethyl citrate is also used as a direct food additive for flavoring, for solvency, and as a surface active agent.
Description
Triethyl citrate is a clear, odorless, practically colorless, oily liquid.
Solubility: soluble 1 in 125 of peanut oil, 1 in 15 of water. Miscible with ethanol (95%), acetone, and propan-2-ol.
Viscosity (dynamic): 35.2 mPa s (35.2 cP) at 25°C
Fructose
Functional Category
Dissolution enhancer; flavoring agent; sweetening agent; tablet diluent.
Applications in Pharmaceutical Formulation or Technology
Fructose is used in tablets, syrups, and solutions as a flavoring and sweetening agent. The sweetness-response profile of fructose is perceived in the mouth more rapidly than that of sucrose and dextrose, which may account for the ability of fructose to enhance syrup or tablet fruit flavors andmask certain unpleasant vitamin ormineral ‘off-flavors’. The increased solubility of fructose in comparison to sucrose is advantageous in syrup or solution formulations that must be refrigerated, since settling or crystallization of ingredients is retarded. Similarly, the greater solubility and hygroscopicity of fructose over sucrose and dextrose helps to avoid ‘cap-locking’ (sugar crystallization around the bottle cap) in elixir preparations. Fructose also has greater solubility in ethanol (95%) and is therefore used to sweeten alcoholic formulations. The water activity of a sweetener influences product microbial stability and freshness. Fructose has a lower water activity and a higher osmotic pressure than sucrose. Syrup formulations may be made at lower dry-substance levels than sugar syrups without compromising shelf-life stability. It may be necessary to include a thickener or gelling agent to match the texture or viscosity of the sugar-equivalent formulation. Fructose is sweeter than the sugar alcohols mannitol and sorbitol, which are commonly used as tableting excipients. Although fructose is effective at masking unpleasant flavors in tablet formulations, tablets of satisfactory hardness and friability can only be produced by direct compression if tablet presses are operated at relatively slow speeds. However, by the combination of crystalline fructose with tablet-grade sorbitol in a 3 : 1 ratio, satisfactory direct-compression characteristics can be achieved. A directly compressible grade of fructose, containing a small amount of starch (Advantose FS 95, SPI Pharma) is also commercially available. Pregranulation of fructose with 3.5% povidone also produces a satisfactory tablet excipient.
The added sweetness of fructose may also be used to advantage by coating the surface of chewable tablets, lozenges, or medicinal gums with powdered fructose. The coprecipitation of fructose with hydrophobic drugs such as digoxin has been shown to enhance the dissolution carrier upon coprecipitation, thereby allowing hydrophobic drugs to be more readily wetted.
Description
Fructose occurs as odorless, colorless crystals or a white crystalline powder with a very sweet taste.
profile of such drugs. Fructose apparently acts as a water-soluble
Table 6 : List of Materials used in the present work are as follows.
S NO | Materials | Name of the supplier |
1 | Acyclovir(mg) | Chandra labs, hyd |
2 | Potassium chloride | MYL CHEM Mumbai |
3 | Sodium chloride | MYL CHEM Mumbai |
4 | Mannitol | MYL CHEM Mumbai |
5 | Sucrose | MYL CHEM Mumbai |
6 | Fructose | S.D Fine chem. LTD Mumbai |
7 | PVP K-30 | S.D Fine chem. LTD Mumbai |
8 | MCC | MYL CHEM Mumbai |
9 | Magnesium Stearate | MYL CHEM Mumbai |
10 | Cellulose acetate | S.D Fine chem. LTD Mumbai |
Table 7: List of Equipments used in the present work are as follows
S.No | Instruments | Source |
1 | Electronic balance | Shimadzu |
2 | UV/Visible Spectrophotometer | Corporation-BL-220H |
3 | FTIR spectrophotometer | Corporation japan |
4 | Magnetic stirrer | Remi motor equipments |
5 | Dissolution apparatus | Shimadzu |
6 | Oven | Biotech india. |
7 | pH meter | Shital scientific industries |
8 | Compression machine | Cadmach machinery |
METHODOLOGY
PREFORMULATION STUDIES
Construction of Standard Graph of Acyclovir in 0.1N Hcl
Preparation of 0.1N Hcl
Take 8.5ml of Hcl in distilled water and make up to 1000ml with distilled Water to get 0.1N Hcl
Construction of Standard Graph of Acyclovir in 0.1N Hcl
Preparation of stock solution:
Accurately weighed amount of 25 mg was transferred into a 25ml volumetric flask. And the volume was made up to 25 mL with 0.1N Hcl. The resulted solution had the concentration of 1mg/ml which was labeled as ‘stock’.
Preparation of working standard solution:
From this stock solution 10ml was taken and diluted to 100 mL with 0.1N Hcl which has given the solution having the concentration of 100 mcg/mL.
Drug – Excipient Compatibility Study:
Infrared spectroscopy is a useful analytical technique utilized to check the chemical interaction between the drug and excipients used in the formulation.1-2 mg of solid fine powder of drug and 200-300 mg of dry powder of KBr(IR grade) were taken in a mortar and mixed well with the help of a spatula. Spectrum measurement was carried out using KBr disk method in the wavelength region of 4000-400cm-1 by FTIR spectrophotometer. The IR spectrum of the physical mixture was compared with that of the pure drug to check any possible drug-excipient interaction.
FORMULATION OF OSMOTIC TABLET
Table 8: Various formulations of ODDS were made as given table
Ingredients (%) | F1 | F2 | F3 | F4 | F5 | F6 | F7 | F8 | ||||||
Acyclovir(mg) | 200 | 200 | 200 | 200 | 200 | 200 | 200 | 200 | ||||||
Potassium chloride | 0.5 | - | - | - | - | - | - | - | ||||||
Sodium chloride | - | 0.5 | - | - | - | 0.75 | 1.0 | 1.25 | ||||||
Mannitol | - | - | 0.5 | - | - | - | - | - | ||||||
Sucrose | - | - | - | 0.5 | - | - | - | - | ||||||
Fructose | - | - | - | - | 0.5 | - | - | - | ||||||
PVP K-30 | 5 | 5 | 5 | 5 | 5 | 5 | 5 | 5 | ||||||
MCC | qs | qs | qs | qs | qs | qs | qs | qs | ||||||
Magnesium Stearate | 2.5 | 2.5 | 2.5 | 2.5 | 2.5 | 2.5 | 2.5 | 2.5 | ||||||
Total wt | 400 | 400 | 400 | 400 | 400 | 400 | 400 | 400 |
Coating with semi-permeable polymer:
Core tablets were coated by using a coating machine with a perforated pan. A solution of cellulose acetate in acetone at a concentration of (4%w/v), containing TEC at concentration of 10% of w/w of cellulose acetate, level of plasticizer (TEC) was used as the coating solution. To the acetone, slowly cellulose acetate added with proper mixing. In between, plasticizer was added drop wise and through mixing was done to dissolve the cellulose acetate. Addition of plasticizer in the coating solution improves film properties like film flexibility. The final coating solution was filtered through # 80 sieve. The composition solution used is mentioned in table below:
Table 9 : Coating solution composition
INGREDIENTS | Weight | CONCENTRATION (%) |
Cellulose acetate | 40gms | 4% |
Triethyl citrate | 4 gms | 0.4 |
Acetone | 1000ml | Quantity sufficient |
PREFORMULATION STUDY
Pre-compression parameters
a) Angle of repose.
b) Bulk density & Tapped density.
c) Hausner ratio.
d) Compressibility index (%)
Angle of repose |
Flow property |
<25> 25-30 30-40 >40 | Excellent Good Passable Very poor |
b) Bulk density and tapped density:
Both loose bulk density (LBD) and Tapped bulk density (TBD) were determined .A quantity of 15gm of granules from each formula, previously shaken to break any agglomerates formed, was introduced in to 50ml measuring cylinder. After that the initial volume was noted and the cylinder was allowed to fall under its own weight on to a hard surface from the height of 2.5 cm at sec intervals. Tapping was continued until no further change in volume was noted. LBD and TBD were calculated using the following equations.
LBD = Weight of the powdered blend /bulk volume
TBD = Weight of the powdered blend /true volume
c) Hausner’s factor
Hausner ratio is an indirect index of ease of powder flow. It is calculated by the following formula
Hausner’s factor = Tapped density/Bulk density d) Carr’s compressibility index28, 53:
The compressibility index of the granules was determined by Carr‟s compressibility index. (%) Carr‟s Index can be calculated by using the following formula
Compressibility % = [(TD - BD)/ TD] ×100
Compressibility index |
Flow property |
5 – 15 12 – 16 18 – 21 23 – 35 33 – 38 >40 | Excellent Good Fair to passable Poor Very poor Very very poor |
Kinetic Analysis of Dissolution Data
To analyze the in vitro release data various kinetic models were used to describe the release kinetics. The zero order rate Eq. (1) describes the systems where the drug release rate is independent of its concentration. The first order Eq. (2) describes the release from system where release rate is concentration dependent , Higuchi (1963) described the release of drugs from insoluble matrix as a square root of time dependent process based on Fickian diffusion Eq. (3). The Hixson-Crowell cube root law Eq. (4) describes the release from systems where there is a change in surface area and diameter of particles or tablets (Hixson and Crowell, 1931).
C = K0 t (1)
where, K0 is zero-order rate constant expressed in units of concentration/time and t is the time.
LogC = LogC0 - K1 t / 2.303 (2)
where, C0 is the initial concentration of drug and K1 is first order constant.
Q = KHt1/2 (3)
where, KH is the constant reflecting the design variables of the system.
Q01/3 – Qt1/3 = KHC t (4)
where, Qt is the amount of drug remained in time t, Q0 is the initial amount of the drug in tablet and KHC is the rate constant for Hixson-Crowell rate equation.
The following plots were made using the in-vitro drug release data
Cumulative % drug release vs. time (Zero order kinetic model);
Log cumulative of % drug remaining vs. time (First order kinetic model);
Cumulative % drug release vs. square root of time (Higuchi model);
And cube root of initial concentration minus the cube root of percentage of drug remaining in the matrix vs. time (Hixson-Crowell cube root law).
viii) Mechanism of drug release
Korsmeyer et al (1983) derived a simple relationship which described drug release from a polymeric system Eq. (5). To find out the mechanism of drug release, first 60% drug release data was fitted in Korsmeyer–Peppas model.
Mt / M∞ = Ktn (5)
where Mt / M∞ is fraction of drug released at time t, K is the release rate constant incorporating structural and geometric characteristics of the tablet, and n is the release exponent. The n value is used to characterize different release mechanisms.
A plot of log cumulative % drug release vs. log time was made. Slope of the line was n. The n value is used to characterize different release mechanisms as given in Table, for the cylindrical shaped matrices. Case-II generally refers to the erosion of the polymeric chain and anomalous transport (Non-Fickian) refers to a combination of both diffusion and erosion controlled-drug release
Table 12: Diffusion Exponent and Solute Release Mechanism for Cylindrical Shape
Diffusion exponent (n) | Overall solute diffusion mechanism |
0.45 | Fickian diffusion |
0.45 < n> | Anomalous (non-Fickian) diffusion |
0.89 | Case-II transport |
n > 0.89 | Super case-II transport |
RESULTS AND DISCUSSION
Preparation of standard calibration curve of Acyclovir:
Table No 13 : Concentration and absorbances of Acyclovir in 0.1N Hcl
S.No | Concentration | Absorbance at 254nm |
1 | 0 | 0 |
2 | 2 | 0.121 |
3 | 4 | 0.238 |
4 | 6 | 0.354 |
5 | 8 | 0.475 |
6 | 10 | 0.576 |
7 | 12 | 0.682 |
Graph 1 - calibration curve of Acyclovir
Standard Graph of Acyclovir in 6.8pH phosphate buffer:
Table No 14: concentration and absorbances of Acyclovir in 6.8pH phosphate buffer
Concentration | Absorbance |
0 | 0 |
2 | 0.124 |
4 | 0.244 |
6 | 0.363 |
8 | 0.485 |
10 | 0.61 |
12 | 0.71 |
Graph No 2 - calibration curve of Acyclovir
DRUG AND EXCIPIENT COMPATIBITLITY
Graph 3 : FTIR Spectra of Acyclovir pure drug
Graph 4: FTIR Spectra of Acyclovir optimized
Table 15: Preformulation parameters of Acyclovir tablets Prepared by direct compression method.
S.no | Formulations | Bulk Density (gm/ml) | Tapped Density (gm/ml) | Compressibility index (%) | Angle of repose (0) | Haunser ratio |
1 | F1 | 0.45 | 0.52 | 24.6 | 13.4 | 1.15 |
2 | F2 | 0.44 | 0.52 | 26.9 | 15.3 | 1.18 |
3 | F3 | 0.45 | 0.51 | 24.2 | 11.7 | 1.13 |
4 | F4 | 0.44 | 0.50 | 29.5 | 12.0 | 1.13 |
5 | F5 | 0.45 | 0.52 | 20.6 | 13.6 | 1.15 |
6 | F6 | 0.43 | 0.50 | 22.6 | 14.0 | 1.16 |
7 | F7 | 0.66 | 0.8 | 25.6 | 16.66 | 1.2 |
8 | F8 | 0.33 | 0.4 | 25.1 | 16.66 | 1.2 |
a.Bulk density and tapped density
Bulk density and tapped density of powder blend was evaluated. The results were shown in the Table No..
b. Angle of Repose
The angle of repose for the entire formulations blend was evaluated. The results were shown in the Table No. range from 11-16.
c. Compressibility Index
Compressibility index for the entire formulations blend was evaluated. The results were shown in the Table No., range from 20-27.
d. Hausner`s Ratio
The Hausner`s ratio for the entire formulations blend was evaluated. The results were shown in the Table No. , range from 1.15-1.20. All these are within the limit.
EVALUATION OF TABLETS
HARDNESS
The prepared tablets in all the formulations possessed good mechanical strength with sufficient hardness in the range of 6.8 to 7.4 kg/sq cm. Shown in table no 16..
FRIABILITY
Friability values below 1% were an indication of good mechanical resistance of the tablets.
WEIGHT VARIATION
All the tablets from each formulation passed weight variation test, as the % weight variation was within the pharmacopoeial limits of ±5% of the weight. The weight variation in all the Eight formulations was found to be 398 to 402 mg, which was in pharmacopoeial limits of ±5% of the average weight. Shown in table no 16.
Table 16 : Post formulation parameters of tablets
Formula code | Hardness (Kg/cm2) | Weight variation (mg) | Friability (%) | Drug content (%) |
F1 | 7.2 | 398 | 0.26 | 99.6 |
F2 | 7.4 | 399 | 0.35 | 99.0 |
F3 | 7.0 | 400 | 0.28 | 99.4 |
F4 | 6.9 | 402 | 0.33 | 99.3 |
F5 | 6.8 | 398 | 0.28 | 99.2 |
F6 | 7.0 | 400 | 0.5 | 99.5 |
F7 | 7.2 | 401 | 0.45 | 99.8 |
F8 | 7.1 | 399 | 0.35 | 99.1 |
DRUG CONTENT
The percentage drug content of all the tablets was found to be around 99 % of acyclovir which was within the acceptable limits. Shown in table no 16.
Table No 17 : DISSOLUTION DATA FOR CORE TABLET
Time in min | F1 | F2 | F3 | F4 | F5 | F6 | F7 | F8 |
0 | 0 | 0 | 0 | 0 | 0 | 0 | 0 | 0 |
5 | 2.5 | 1.8 | 6.3 | 5.8 | 9.4 | 1.2 | 1.6 | 1.4 |
10 | 10 | 6.9 | 11.4 | 10.9 | 16.8 | 6.8 | 5.2 | 6.4 |
15 | 16 | 12 | 19.8 | 18.3 | 22 | 12.3 | 11.8 | 12.4 |
30 | 20 | 19 | 26.3 | 24.8 | 29.8 | 19.9 | 16.3 | 14.9 |
45 | 28 | 24 | 32.8 | 32.4 | 36.9 | 24.8 | 22 | 19 |
60 | 35 | 30 | 40 | 38 | 42 | 36 | 24 | 20 |
Graph No 5: Dissolution graph for core tablets
Table No 18: DISSOLUTION STUDIES FOR OSMOTIC TABLETS
Time in hrs | F1 | F2 | F3 | F4 | F5 | F6 | F7 | F8 |
30min | 10.6 | 11.6 | 7.2 | 30.6 | 29.7 | 6.3 | 5.7 | 5.0 |
1 | 39.8 | 40.7 | 17.1 | 60.2 | 70.8 | 15.4 | 11.9 | 10.6 |
2 | 70.3 | 68.2 | 29.2 | 100.1 | 100.3 | 26.1 | 20.2 | 21.4 |
4 | 100.1 | 99.1 | 50.8 | 40.6 | 30.5 | 29.7 | ||
6 | 73.7 | 61.1 | 48.9 | 50.2 | ||||
8 | 99.26 | 89.9 | 62.1 | 64.8 | ||||
10 | 99.5 | 88.2 | 86.1 | |||||
12 | 100.1 | 90.9 |
Graph No 6: Dissolution graph for osmotic tablets
It is evident that after coating with semipermeable membrane of Cellulose acetate, the increase in concentration of osmogen NaCl leads to increase in drug release from the tablet due to the osmotic effect. Among all formulations F7 was optimized based on maximum drug release.
KINETIC STUDIES FOR OPTIMIZED FORMULATION (F7)
Table no 19: Release kinetics for the optimized formulation F7
ZERO | FIRST | HIGUCHI | PEPPAS | |
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We are grateful for this opportunity to provide a glowing recommendation to the Journal of Psychiatry and Psychotherapy. We found that the editorial team were very supportive, helpful, kept us abreast of timelines and over all very professional in nature. The peer review process was rigorous, efficient and constructive that really enhanced our article submission. The experience with this journal remains one of our best ever and we look forward to providing future submissions in the near future.
I am very pleased to serve as EBM of the journal, I hope many years of my experience in stem cells can help the journal from one way or another. As we know, stem cells hold great potential for regenerative medicine, which are mostly used to promote the repair response of diseased, dysfunctional or injured tissue using stem cells or their derivatives. I think Stem Cell Research and Therapeutics International is a great platform to publish and share the understanding towards the biology and translational or clinical application of stem cells.
I would like to give my testimony in the support I have got by the peer review process and to support the editorial office where they were of asset to support young author like me to be encouraged to publish their work in your respected journal and globalize and share knowledge across the globe. I really give my great gratitude to your journal and the peer review including the editorial office.
I am delighted to publish our manuscript entitled "A Perspective on Cocaine Induced Stroke - Its Mechanisms and Management" in the Journal of Neuroscience and Neurological Surgery. The peer review process, support from the editorial office, and quality of the journal are excellent. The manuscripts published are of high quality and of excellent scientific value. I recommend this journal very much to colleagues.
Dr.Tania Muñoz, My experience as researcher and author of a review article in The Journal Clinical Cardiology and Interventions has been very enriching and stimulating. The editorial team is excellent, performs its work with absolute responsibility and delivery. They are proactive, dynamic and receptive to all proposals. Supporting at all times the vast universe of authors who choose them as an option for publication. The team of review specialists, members of the editorial board, are brilliant professionals, with remarkable performance in medical research and scientific methodology. Together they form a frontline team that consolidates the JCCI as a magnificent option for the publication and review of high-level medical articles and broad collective interest. I am honored to be able to share my review article and open to receive all your comments.
“The peer review process of JPMHC is quick and effective. Authors are benefited by good and professional reviewers with huge experience in the field of psychology and mental health. The support from the editorial office is very professional. People to contact to are friendly and happy to help and assist any query authors might have. Quality of the Journal is scientific and publishes ground-breaking research on mental health that is useful for other professionals in the field”.
Dear editorial department: On behalf of our team, I hereby certify the reliability and superiority of the International Journal of Clinical Case Reports and Reviews in the peer review process, editorial support, and journal quality. Firstly, the peer review process of the International Journal of Clinical Case Reports and Reviews is rigorous, fair, transparent, fast, and of high quality. The editorial department invites experts from relevant fields as anonymous reviewers to review all submitted manuscripts. These experts have rich academic backgrounds and experience, and can accurately evaluate the academic quality, originality, and suitability of manuscripts. The editorial department is committed to ensuring the rigor of the peer review process, while also making every effort to ensure a fast review cycle to meet the needs of authors and the academic community. Secondly, the editorial team of the International Journal of Clinical Case Reports and Reviews is composed of a group of senior scholars and professionals with rich experience and professional knowledge in related fields. The editorial department is committed to assisting authors in improving their manuscripts, ensuring their academic accuracy, clarity, and completeness. Editors actively collaborate with authors, providing useful suggestions and feedback to promote the improvement and development of the manuscript. We believe that the support of the editorial department is one of the key factors in ensuring the quality of the journal. Finally, the International Journal of Clinical Case Reports and Reviews is renowned for its high- quality articles and strict academic standards. The editorial department is committed to publishing innovative and academically valuable research results to promote the development and progress of related fields. The International Journal of Clinical Case Reports and Reviews is reasonably priced and ensures excellent service and quality ratio, allowing authors to obtain high-level academic publishing opportunities in an affordable manner. I hereby solemnly declare that the International Journal of Clinical Case Reports and Reviews has a high level of credibility and superiority in terms of peer review process, editorial support, reasonable fees, and journal quality. Sincerely, Rui Tao.
Clinical Cardiology and Cardiovascular Interventions I testity the covering of the peer review process, support from the editorial office, and quality of the journal.
Clinical Cardiology and Cardiovascular Interventions, we deeply appreciate the interest shown in our work and its publication. It has been a true pleasure to collaborate with you. The peer review process, as well as the support provided by the editorial office, have been exceptional, and the quality of the journal is very high, which was a determining factor in our decision to publish with you.
The peer reviewers process is quick and effective, the supports from editorial office is excellent, the quality of journal is high. I would like to collabroate with Internatioanl journal of Clinical Case Reports and Reviews journal clinically in the future time.
Clinical Cardiology and Cardiovascular Interventions, I would like to express my sincerest gratitude for the trust placed in our team for the publication in your journal. It has been a true pleasure to collaborate with you on this project. I am pleased to inform you that both the peer review process and the attention from the editorial coordination have been excellent. Your team has worked with dedication and professionalism to ensure that your publication meets the highest standards of quality. We are confident that this collaboration will result in mutual success, and we are eager to see the fruits of this shared effort.
Dear Dr. Jessica Magne, Editorial Coordinator 0f Clinical Cardiology and Cardiovascular Interventions, I hope this message finds you well. I want to express my utmost gratitude for your excellent work and for the dedication and speed in the publication process of my article titled "Navigating Innovation: Qualitative Insights on Using Technology for Health Education in Acute Coronary Syndrome Patients." I am very satisfied with the peer review process, the support from the editorial office, and the quality of the journal. I hope we can maintain our scientific relationship in the long term.
Dear Monica Gissare, - Editorial Coordinator of Nutrition and Food Processing. ¨My testimony with you is truly professional, with a positive response regarding the follow-up of the article and its review, you took into account my qualities and the importance of the topic¨.
Dear Dr. Jessica Magne, Editorial Coordinator 0f Clinical Cardiology and Cardiovascular Interventions, The review process for the article “The Handling of Anti-aggregants and Anticoagulants in the Oncologic Heart Patient Submitted to Surgery” was extremely rigorous and detailed. From the initial submission to the final acceptance, the editorial team at the “Journal of Clinical Cardiology and Cardiovascular Interventions” demonstrated a high level of professionalism and dedication. The reviewers provided constructive and detailed feedback, which was essential for improving the quality of our work. Communication was always clear and efficient, ensuring that all our questions were promptly addressed. The quality of the “Journal of Clinical Cardiology and Cardiovascular Interventions” is undeniable. It is a peer-reviewed, open-access publication dedicated exclusively to disseminating high-quality research in the field of clinical cardiology and cardiovascular interventions. The journal's impact factor is currently under evaluation, and it is indexed in reputable databases, which further reinforces its credibility and relevance in the scientific field. I highly recommend this journal to researchers looking for a reputable platform to publish their studies.
Dear Editorial Coordinator of the Journal of Nutrition and Food Processing! "I would like to thank the Journal of Nutrition and Food Processing for including and publishing my article. The peer review process was very quick, movement and precise. The Editorial Board has done an extremely conscientious job with much help, valuable comments and advices. I find the journal very valuable from a professional point of view, thank you very much for allowing me to be part of it and I would like to participate in the future!”
Dealing with The Journal of Neurology and Neurological Surgery was very smooth and comprehensive. The office staff took time to address my needs and the response from editors and the office was prompt and fair. I certainly hope to publish with this journal again.Their professionalism is apparent and more than satisfactory. Susan Weiner
My Testimonial Covering as fellowing: Lin-Show Chin. The peer reviewers process is quick and effective, the supports from editorial office is excellent, the quality of journal is high. I would like to collabroate with Internatioanl journal of Clinical Case Reports and Reviews.
My experience publishing in Psychology and Mental Health Care was exceptional. The peer review process was rigorous and constructive, with reviewers providing valuable insights that helped enhance the quality of our work. The editorial team was highly supportive and responsive, making the submission process smooth and efficient. The journal's commitment to high standards and academic rigor makes it a respected platform for quality research. I am grateful for the opportunity to publish in such a reputable journal.
My experience publishing in International Journal of Clinical Case Reports and Reviews was exceptional. I Come forth to Provide a Testimonial Covering the Peer Review Process and the editorial office for the Professional and Impartial Evaluation of the Manuscript.