Orally disintegrating tablet

An orally disintegrating tablet or orodispersible tablet (ODT) is a drug dosage form available for a limited amount of over-the-counter (OTC) and prescription medications. ODTs differ from traditional tablets in that they are designed to be dissolved on the tongue rather than swallowed whole.^{[1][2][3][4][5][6][7][8][9][10][11]} The ODT serves as an alternative dosage form for patients who experience dysphagia (difficulty in swallowing) or for where compliance is a known issue and therefore an easier dosage form to take ensures that medication is taken. Common among all age groups, dysphagia is observed in about 35% of the general population, as well as up to 60% of the elderly institutionalized population ^[12][13] and 18-22% of all patients in long-term care facilities ^[14] During the last decade, ODTs have become available in a variety of therapeutic markets, both OTC and by presciption. An additional reason to use an ODTs is the convenience of a tablet that can be taken without water.

History

Tablets designed to dissolve on the buccal (cheek) mucous membrane were a precursor to the ODT. This dosage form was intended for drugs that yield low bioavailability through the digestive tract but are inconvenient to administer parenterally, such as steroids and narcotic analgesics.^[15] Absorption through the cheek allows the drug to bypass the digestive tract for rapid systemic distribution. Not all ODTs have buccal absorption and many have similar absorption and bioavailability to standard oral dosage forms with the primary route remaining GI absorption. However, a fast disintegration time and a small tablet weight can enhance absorption in the buccal area. The first ODTs disintegrated through effervescence rather than dissolution, and were designed to make taking vitamins more pleasant for children.^[16] This method was adapted to pharmaceutical use with the invention of microparticles containing a drug, which would be released upon effervescence of the tablet and swallowed by the patient.^[17] Dissolution became more effective than effervescence through improved manufacturing processes and ingredients (such as the addition of mannitol to increase binding and decrease dissolution time).^[18] Catalent Pharma Solutions (formerly Scherer DDS) in the U.K., Cima Labs in the U.S. and Takeda Pharmaceutical Company in Japan led the development of ODTs.

The first ODT form of a drug to get approval from the U.S. Food and Drug Administration (FDA) was a Zydis ODT formation of Claritin (loratadine) in December 1996.^[19] It was followed by a Zydis ODT formulation of Klonopin (clonazepam) in December 1997,^[20] and a Zydis ODT formulation of Maxalt (rizatriptan) in June 1998.^[21] The regulatory condition for meeting the definition of an orally disintegrating tablet is USP method 701 for Disintegration. FDA guidance issued in Dec 2008 is that ODT drugs should disintegrate in less than 30 seconds.^[22] This practice is under review by the FDA as the fast disintegration time of ODTs makes the Disintegration test too rigorous for some of the ODT formulations that are commercially available.

Manufacturing/packaging

The processes used to manufacture orally disintegrating tablets include loose compression tabletting, a process which is not very different than the manufacturing method used for traditional tables and lyophilization processes. In loose compression, ODTs are compressed at much lower forces (4 – 20 kN) than traditional tablets. However, since ODTs are compressed at very low forces due to the need to them to be soft enough to disintegrate rapidly in the mouth, issues of material sticking to the die walls can be challenging. Typically, as in most tablet blends, lubricants such as magnesium stearate are added to the blend to reduce the amount of material that may stick to the die wall. Differences may be the use of disintegrating aids, such as crospovidone, and binding agents that aid in mouth feel, such as microcrystalline cellulose. Primarily, ODTs contain some form of sugar such as mannitol, which typically serves as the major diluent of the ODTs, and is also the primary contributor to the smooth and creamy mouth feel of most ODTs. Lyophilized ODT formulations may use proprietary technologies but can produce a tablet that has a faster disintegration rate, the Zydis ODT typically dissolves in the mouth in less than 5 seconds without water.

ODTs are available in HPDE bottles (Parcopa) or individually sealed in blister packs to protect the tablets from damage, moisture, and oxidation. Because ODTs are soft in nature, the ability to successfully package an ODT in a bottle is difficult. However, CIMA Labs markets their Durasolv ODT as being able to be placed into bottle for commercial sale, while CIMA's Orasolv is marketed for blisters only. Zydis ODT tablets manufactured by Catalent Pharma Solutions are delivered in a blisterpack. The differences between the two CIMA products are proprietary, however, the primary difference is expected to be the use of microcrystalline cellulose (MCC), such as Avicel PH101, in the Durasolv product. MCC serves multiple purposes in an ODT but in the case of CIMA's products, it acts as a binder, increasing the internal strength of the tablet and making it more robust for packaging in bottles.

ODTs currently or previously available

ODTs under development

See also

• Phagophobia - fear of swallowing
• Pnigophobia - fear of choking
• Sugar alcohol - a family of chemicals common in ODTs to enhance the mouth feel of the tablet as it disintegrates

References

v t e Routes of administration / Dosage forms
Oral	Digestive tract (enteral) Solids Pill · Tablet · Capsule · Osmotic controlled release capsule (OROS) · Softgel Liquids Solution · Suspension · Emulsion · Syrup · Elixir · Tincture · Hydrogel Buccal / Sublabial / Sublingual Solids Orally Disintegrating Tablet (ODT) · Film · Lollipop · Lozenges · Chewing gum Liquids Mouthwash · Toothpaste · Ointment · Oral spray Respiratory tract Solids Smoking device · Dry Powder Inhaler (DPI) Liquids pressurized Metered Dose Inhaler (pMDI) · Nebulizer · Vaporizer Gas Oxygen mask · Oxygen concentrator · Anaesthetic machine · Relative analgesia machine	58px 58px 58px 58px 58px 52px
Ocular / Otologic / Nasal	Nasal spray · Ear drops · Eye drops · Ointment · Hydrogel · Nanosphere suspension · Mucoadhesive microdisc (microsphere tablet)
Urogenital	Ointment · Pessary (vaginal suppository) · Vaginal ring · Vaginal douche · Intrauterine device (IUD) · Extra-amniotic infusion · Intravesical infusion
Rectal (enteral)	Ointment · Suppository · Enema (Solution · Hydrogel) · Murphy drip · Nutrient enema
Dermal	Ointment · Liniment · Paste · Film · Hydrogel · Liposomes · Transfersome vesicals · Cream · Lotion · Lip balm · Medicated shampoo · Dermal patch · Transdermal patch · Transdermal spray · Jet injector
Injection / Infusion (into tissue/blood)	Skin Intradermal · Subcutaneous · Transdermal implant Organs Intracavernous · Intravitreal · Transscleral Central nervous system Intracerebral · Intrathecal · Epidural Circulatory / Musculoskeletal Intravenous · Intracardiac · Intramuscular · Intraosseous · Intraperitoneal · Nanocell injection
Additional explanation:	Mucous membranes are used by the human body to absorb the dosage for all routes of administration, except for "Dermal" and "Injection/Infusion". Administration routes can also be grouped as Topical (local effect) or Systemic (defined as Enteral = Digestive tract/Rectal, or Parenteral = All other routes).

1. ↑ ^{1.0 1.1 1.2} Allegra Prescribing Information
2. ↑ ^{2.0 2.1 2.2 2.3} Aricept Prescribing Information
3. ↑ ^{3.0 3.1 3.2} Maxalt Prescribing Information
4. ↑ ^{4.0 4.1 4.2 4.3 4.4} Remeron SolTob Prescribing Information
5. ↑ ^{5.0 5.1 5.2 5.3 5.4} Zofran Prescribing Information
6. ↑ ^{6.0 6.1 6.2} Orapred Prescribing Information
7. ↑ ^{7.0 7.1 7.2} Parcopa Prescribing Information
8. ↑ ^{8.0 8.1 8.2 8.3} Prevacid Prescribing Information
9. ↑ ^{9.0 9.1 9.2} Risperdal Prescribing Information
10. ↑ ^{10.0 10.1 10.2 10.3} Zelapar Prescribing Information
11. ↑ ^{11.0 11.1 11.2} Zomig Prescribing Information
12. ↑ Sastry, S. et al., Pharm. Sci. & Tech. Today 3: 138-145, 2000.
13. ↑ Groher ME, Bukatman MS. The prevalence of swallowing disorders in two teaching hospitals. Dysphagia. 1: 3-6, 1986.
14. ↑ Layne KA, Losinski DS, Zenner PM, Ament JA. Using the Fleming index of dysphagia to establish prevalence. Dysphagia. 4: 39-42, 1989.
15. ↑ US 5073374, Mccarty, John A., "Fast dissolving buccal tablet", published 1991 
16. ↑ US 5223264, Wehling, Fred; Steve Schuehle & Navayanarao Madamala, "Pediatric effervescent dosage form", published 1993 
17. ↑ US 5178878, Wehling, Fred; Steve Schuehle & Navayanarao Madamala, "Effervescent dosage form with microparticles", published 1993 
18. ↑ US 4946684, Blank, Robert G.; Dhiraj S. Mody & Richard J. Kenny et al., "Fast dissolving dosage forms", published 1990 
19. ↑ FDA Drug Details for Claritin RediTabs
20. ↑ FDA Drug Details for Klonopin Wafer
21. ↑ FDA Drug Details for Maxalt-MLT
22. ↑ FDA Guidance for Industry Orally Disintegrating Tablets
23. ↑ ^{23.0 23.1 23.2} Abilify Prescribing Information
24. ↑ ^{24.0 24.1} Clonazepam ODT Prescribing Information
25. ↑ ^{25.0 25.1} FazaClo Prescribing Information
26. ↑ ^{26.0 26.1 26.2} Klonopin Prescribing Information
27. ↑ [2]
28. ↑ Unisom Drug Facts
29. ↑ ^{29.0 29.1} Zyprexa Prescribing Information
30. ↑ ^{30.0 30.1 30.2 30.3 30.4 30.5 30.6 30.7} Biovail Product Pipeline
31. ↑ Citalopram Prescribing Information
32. ↑ ^{32.0 32.1 32.2 32.3} Salix Pharmaceuticals Acquires Patent–Protected Metoclopramide–Zydis
33. ↑ ^{33.0 33.1 33.2 33.3} FDA Drug Approval for Reglan ODT
34. ↑ ^{34.0 34.1} Ultracet Prescribing Information
35. ↑ ^{35.0 35.1} Ambien Prescribing Information