Int J Curr Pharm Res, Vol 9, Issue 6, 5-7Review Article


SUBLINGUAL DRUG DELIVERY: AN INDICATION OF POTENTIAL ALTERNATIVE ROUTE

PUJA SAHA1*, SUSHMA VERMA2, PRATIK SWARUP DAS1

1Noida Institute of Engineering and Technology, 2Pharmacy Institute, Noida Institute of Engineering and Technology
Email: pujasahaps070@gmail.com

Received: 20 Aug 2017, Revised and Accepted: 13 Oct 2017

ABSTRACT

Sublingual literally meaning is “under the tongue”, refers to a method of administrating substance via mouth in such a way that the substance is rapidly absorbed via blood vessels under tongue. Sublingual route is useful when a rapid onset of action is desired with better patient compliance than orally ingested tablets. Drugs that are given sublingually reach directly into the systemic circulation through the ventral surface of the tongue and floor of the mouth. The portion of drug absorbed through the sublingual blood vessels bypasses the hepatic first‐pass metabolic processes giving acceptable bioavailability. As nowadays most of the people need effective relief within a short period of time so sublingual is the most suitable form of administration. New sublingual technologies address many pharmaceutical and patient needs, ranging from enhanced life‐cycle management to convenient dosing for paediatric, geriatric, and psychiatric patients with dysphagia.

Keywords: Sublingual route, Patient compliance, Dysphagia, Sublingual technologies

© 2017 The Authors. Published by Innovare Academic Sciences Pvt Ltd. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/)
DOI: http://dx.doi.org/10.22159/ijcpr.2017v9i6.23436

INTRODUCTION

Sublingual administration of the drug means placement of the drug under the tongue and the drug reaches directly into the bloodstream through the ventral surface of the tongue and floor of the mouth. The drug solutes are rapidly absorbed into the reticulated vein which lies underneath the oral mucosa, and transported through the facial veins, internal jugular vein, and brachiocephalic vein and then drained into systemic circulation. The routes of absorption via the highly vascularized buccal mucosa allow the substance a more direct access to the blood circulation, thus providing direct systemic administration [1].

Medically, sublingual drug administration is applied in the field of cardiovascular drugs, steroids, some barbiturates and enzymes. It has been a developing field in the administration of many vitamins and minerals which are found to be readily and thoroughly absorbed by this method [2].

Mechanism of sublingual absorption

The mucosal lining consists of three distinct layers. The outermost layer is the epithelial membrane, which consists of stratified squamous epithelial cells and has a protective barrier function. The innermost layer of the epithelial membrane is called the basement membrane that replenishes the epithelium. Below the epithelium lies the lamina propria followed by the submucosa. The lamina propria is a hydrated and less dense layer of connective tissue containing collagen and elastic fibres [3]. The oral submucosa is also richly supplied with blood vessels [4].

The following absorption through the mucous membrane in the sublingual region, the drug instantly diffuses into venous blood. The venous blood from the sublingual region of the oral cavity drains into a common trunk, which then drains via the internal jugular vein, the subclavian vein, and the brachiocephalic vein directly into the superior vena cava. 8Thus, venous return from these regions enter the systemic circulation, bypassing the pre-systemic drug elimination, unlike in oral administration. Direct drainage into systemic circulation results in the immediate systemic availability of the drug and rapid onset of action. It should be noted that smoking, which causes vasoconstriction, may affect drug absorption [5].

Drugs for sublingual administration

Sublingually absorbed nutrition, which avoids exposure to the gastric system and liver, means direct nutritional benefits, particularly important for sufferers of gastrointestinal difficulties such as ulcers, hyperactive gut, coeliac disease, those with compromised digestion, the elderly and invalids–the nutritional benefit is independent of gastro‐intestinal influences10.

Examples of drugs administered by this route include antianginal like nitrites and nitrates, antihypertensive like nifedipine, analgesics like morphine and bronchodilators like fenoterol. Certain steroids like estradiol and peptides like oxytocin can also be administered e. g. fentanyl citrate, apomorphine, prochlorperazine dimaleate {PRO}, and hydrazine HCl {HYD} [6].

Factors affecting the sublingual absorption [7]

Advantages [8]

• Liver is bypassed and also drug is protected from degradation due to pH and digestive enzymes of the middle gastrointestinal tract.

• Improved patient compliance due to the elimination of associated pain with injections; administration of drugs in unconscious or incapacitated patients; convenience of administration as compared to injections or oral medications.

• Low dosage gives high efficacy as hepatic first-pass metabolism is avoided and also reduces the risk of side effects.

• Due to rapidity in action, these sublingual dosage forms are widely used in emergency conditions e. g. asthma.

• Rapid absorption and higher blood levels due to high vascularization of the region and therefore particularly useful for administration of antianginal drugs.

• They also present the advantage of providing fast dissolution or disintegration in the oral cavity, without the need for water or chewing.

Disadvantages [9]

Formulation aspects of sublingual tablet

The distinct feature in the formulation of sublingual tablets involves the selection of suitable excipients of bland taste that shall ultimately resulting in a rapidly disintegrating tablet their by enhancing the dissolution of active ingredient [10].

There are two different types of the sublingual tablet:

  1. Molded Sublingual Tablets.

  2. Compressed Sublingual Tablets.

Molded sublingual tablets

Molded sublingual tablets are usually prepared from soluble ingredients so that the tablets are completely and rapidly soluble. They contain, in addition to the drug, an excipient or base namely lactose, dextrose, sucrose, mannitol or other rapidly soluble materials or mixtures of these ingredients. Tablets containing insoluble excipients may be prepared from finally divided kaolin, calcium carbonate, calcium phosphate or other insoluble powders. To insure rapid solubility of the soluble tablets, the excipients are usually passed through a fine screen or # 120 mesh bolting cloth. After the excipients are blended with the drug, the powder mix is moistened with the solvent, which is most commonly alcohol and water mixture. Other volatile solvents, such as acetone or hydrocarbons, may also be used. Antioxidants such as sodium bisulphate and buffers or other ingredients may be added to improve the physical and chemical stability of the product. To increase the hardness and reduce the erosion on the edges of the tablets during handling, agents such as glucose, sucrose, acacia or povidone may be added to the solvent mixture [11-12].

Compressed sublingual tablets

Compressed sublingual tablets can be prepared by two different methods:

a) Wet Granulation method

b) Direct compression method

The directly compressible sublingual tablet formulation contains directly compressible soluble excipients, a super disintegrant, and lubricant. It may also contain microcrystalline cellulose, a dry binder, buffers, surface-active agents, sweeteners, and flavors. Sugar-based excipients are widely used as bulking agents because of their high aqueous solubility, sweetness, pleasant feeling in the mouth, and good taste-masking. Nearly all sublingual formulations incorporate some saccharide-based material. The choice of a suitable disintegrant and its amount are critical for achieving a fast disintegration and dissolution rate. Sometimes effervescent agents are used to increasing disintegration and dissolution of sublingual tablets [13].

Several novel approaches of incorporating disintegrants and other soluble and/or insoluble excipients to obtain rapid dissolution and adequate mechanical strength are reported. One example is the Flash tab technology of multiparticulate actives (coated crystals and uncoated or coated microgranules) [14-15]. In these tablets, the simultaneous presence of a disintegrant with a high swelling or disintegrating force, defined as “disintegrating agent,” and a substance with a low swelling force (starch, cellulose, and direct-compression sugar), defined as “swelling agent,” was claimed as the key factor for the rapid disintegration of a tablet. The tablet manufactured by this technology is reported to have adequate mechanical strength [16].

In vitro and in vivo evaluation

Physical evaluation

Disintegration time (DT)

A relatively simple method with rigorous conditions has been developed to evaluate the DT of sublingual tablets. Each individual tablet is dropped into 10‐mL glass test tube (1.5‐cm diameter) containing 2 ml distilled water, and the time required for complete tablet disintegration is observed visually and recorded using a stopwatch. The visual inspection can be enhanced by gently rotating the test tube at a 45 ° angle, without agitation, to distribute any tablet particles that might mask any remaining undisintegrated portion of the tablets.

In the USP disintegration test for sublingual tablets, the disintegration apparatus for oral tablets is used without the covering plastic disks, and 2 min* is specified as the acceptable time limit for tablet disintegration [23].

Wetting time (WT)

Although a wetting test is not a USP standard test, it is useful for quality control and provides a supportive evaluation of these sublingual tablets. Using this test, the time required for moisture to penetrate the tablet completely is measured and possibly represents the time required to release the drug in the presence of minute volumes of saliva [24].

Friability

Twenty tablets are to be weighed and placed in a Roche friabilator and the equipment has to be rotated at 25 rpm for 4 min. The tablets were taken out, dedusted, and reweighed. The percentage friability of the tablets can be calculated by:

In vivo evaluation

Pharmacokinetic data analysis and bioavailability evaluation

Rabbits have been described as one of the few laboratory animals that do not have keratinized mucosa, thus closely resembling human sublingual mucosal tissue 25. The maximal plasma concentration (Cmax) and the time to reach maximum plasma concentration (Tmax) can be directly obtained from the plasma data. The area under the plasma concentration curve (AUC) can also calculate using the trapezoidal rule and then the bioavailability [25].

Permeation studies

Ex vivo permeation studies through porcine oral mucosa can be carried out using the modified Franz diffusion cell of the internal diameter of 2.5 cm. The buccal mucosa has to be excised and trimmed evenly from the sides and then washed in isotonic phosphate buffer of pH 6.6 and used immediately. The membrane needs to be stabilized before mounting to remove the soluble components. The mucosa has to be mounted between the donor and receptor compartments. The receptor compartment has to be filled with 200 ml of isotonic phosphate buffer of pH 7.4 which is maintained at 37±0.2 °C and hydrodynamics has to be maintained by stirring with a magnetic bead at 50 rpm. The donor compartment has to be filled with 1 ml of simulated saliva of pH 6.8. Samples are to be withdrawn at suitable interval replacing the same amount with fresh medium26, 27. The percentage of drug permeated can be determined by measuring the absorbance in a UV‐Visible spectrophotometer [26-27].

Recent developments

Nitroglycerine‐delivering sublingual aerosol formulation (nitro-glycerine in propellants) in a metered‐dose spraying pump, Nitrolingual spray, was developed. It delivers nitroglycerine by spraying onto or under the tongue in the form of spray droplets, which ultimately increase the absorption and hence the bioavailability of nitroglycerine. The rapid onset of action is always required in case of hypertension.

CONCLUSION

In conclusion, this review demonstrates that there are a number of commercially available sublingual formulations manufactured using various technologies. The publically available information on sublingual tablets implies that this dosage form has good potential to enhance drug delivery in treating a number of indications. In most reported cases, it has been shown that the sublingual dosage form not only improves the patient’s compliance, but also reduces the time for the onset of the drug action, and increases the bioavailability of drugs as compared to conventional tablets. Therefore sublingual tablets are an accepted technology for systemic delivery of drugs.

CONFLICT OF INTERESTS

Declared none

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