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Novel substituted benzimidazole dosage forms and method of using same

a technology of benzimidazole and dosage form, which is applied in the direction of drug composition, dispersed delivery, inorganic non-active ingredients, etc., can solve the problems of ineffective treatment, adverse side effects, and significant upper gastrointestinal bleeding, and achieve enhanced ppi effect and pharmacologic activity

Inactive Publication Date: 2004-03-11
UNIVERSITY OF MISSOURI
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Benefits of technology

[0038] Kits utilizing the inventive dry dosage forms are also disclosed herein to provide for the easy preparation of a liquid composition from the dry forms.
[0088] Additionally, the present invention can be manufactured by utilizing micronized compounds in place of the granules or powder. Micronization is the process by which solid drug particles are reduced in size. Since the dissolution rate is directly proportional to the surface area of the solid, and reducing the particle size increases the surface area, reducing the particle size increases the dissolution rate. Although micronization results in increased surface area possibly causing particle aggregation, which can negate the benefit of micronization and is an expensive manufacturing step, it does have the significant benefit of increasing the dissolution rate of relatively water insoluble drugs, such as omeprazole and other proton pump inhibitors.

Problems solved by technology

These above-listed conditions commonly arise in healthy or critically ill patients, and may be accompanied by significant upper gastrointestinal bleeding.
These drugs have certain disadvantages associated with their use.
Some of these drugs are not completely effective in the treatment of the aforementioned conditions and / or produce adverse side effects, such as mental confusion, constipation, diarrhea, and thrombocytopenia.
H2-antagonists, such as ranitidine and cimetidine, are relatively costly modes of therapy, particularly in NPO patients, which frequently require the use of automated infusion pumps for continuous intravenous infusion of the drug.
Regardless of the risk type, stress-related mucosal damage results in significant morbidity and mortality.
Although these drugs are stable at alkaline pH, they are destroyed rapidly as pH falls (e.g., by gastric acid).
The absence of an intravenous or oral liquid dosage form in the United States has limited the testing and use of omeprazole, lansoprazole and rabeprazole in the critical care patient population.
However, such pellets are not ideal as they can aggregate and occlude such tubes, and they are not suitable for patients who cannot swallow the pellets.
However, in their current form (capsules containing enteric-coated granules or enteric-coated tablets), proton pump inhibitors can be difficult or impossible to administer to patients who are either unwilling or unable to swallow tablets or capsules, such as critically ill patients, children, the elderly, and patients suffering from dysphagia.
This device and method of parenteral infusion of omeprazole does not provide the omeprazole solution as an enteral product, nor is this omeprazole solution directly administered to the diseased or affected areas, namely the stomach and upper gastrointestinal tract, nor does this omeprazole formulation provide the immediate antacid effect of the present formulation.
This formulation of omeprazole does not teach a non-enteric-coated omeprazole dosage form which can be enterally administered to a patient who may be unable and / or unwilling to swallow capsules, tablets or pellets, nor does it teach a convenient form which can be used to make an omeprazole or other proton pump inhibitor solution or suspension.
The administration of large amounts of sodium bicarbonate can produce at least six significant adverse effects, which can dramatically reduce the efficacy of the omeprazole in patients and reduce the overall health of the patients.
First, the fluid volumes of these dosing protocols would not be suitable for sick or critically ill patients who must receive multiple doses of omeprazole.
The large volumes would result in the distention of the stomach and increase the likelihood of complications in critically ill patients such as the aspiration of gastric contents.
Second, because bicarbonate is usually neutralized in the stomach or is absorbed, such that belching results, patients with gastroesophageal reflux may exacerbate or worsen their reflux disease as the belching can cause upward movement of stomach acid (Brunton, Agents for the Control of Gastric Acidity and Treatment of Peptic Ulcers, In, Goodman A G, et al.
The ingestion of large amounts of sodium bicarbonate is inconsistent with this advice.
Fourth, patients with numerous conditions that typically accompany critical illness should avoid the intake of excessive sodium bicarbonate as it can cause metabolic alkalosis that can result in a serious worsening of the patient's condition.
Fifth, excessive antacid intake (such as sodium bicarbonate) can result in drug interactions that produce serious adverse effects.
Sixth, because the buffered omeprazole solutions of the prior art require prolonged administration of sodium bicarbonate, it makes it difficult for patients to comply with the regimens of the prior art.
Not only does this regimen require the ingestion of excessive amounts of bicarbonate and water, which is likely to be dangerous to some patients, it is unlikely that even healthy patients would comply with this regimen.
It is well documented that patients who are required to follow complex schedules for drug administration are non-compliant and, thus, the efficacy of the buffered omeprazole solutions of the prior art would be expected to be reduced due to non-compliance.

Method used

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  • Novel substituted benzimidazole dosage forms and method of using same
  • Novel substituted benzimidazole dosage forms and method of using same
  • Novel substituted benzimidazole dosage forms and method of using same

Examples

Experimental program
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Effect test

example i

[0122] Fast Disintegrating Suspension Tablets of Omeprazole. A fast disintegrating tablet is compounded as follows: Croscarmellose sodium 300 g is added to the vortex of a rapidly stirred beaker containing 3.0 kg of deionized water. This slurry is mixed for 10 minutes. Omeprazole 90 g (powdered) is placed in the bowl of a Hobart mixer. After mixing, the slurry of croscarmellose sodium is added slowly to the omeprazole in the mixer bowl, forming a granulation, which is then placed in trays and dried at 70.degree. C. for three hours. The dry granulation is then placed in a blender, and to it is added 1,500 g of Avicel.RTM. AC-815 (85% microcrystalline cellulose coprocessed with 15% of a calcium, sodium alginate complex) and 1,500 g of Avicel.RTM. PH-302 (microcrystalline cellulose). After this mixture is thoroughly blended, 35 g of magnesium stearate is added and mixed for 5 minutes. The resulting mixture is compressed into tablets on a standard tablet press (Hata HS). These tablets h...

example ii

[0125] Standard Tablet of PPI and Buffering Agent: Ten (10) tablets were prepared using a standard tablet press, each tablet comprising about 20 mg omeprazole and about 975 mg sodium bicarbonate uniformly dispersed throughout the tablet. To test the disintegration rate of the tablets, each was added to 60 ml of water. Using previously prepared liquid omeprazole / sodium bicarbonate solution as a visual comparator, it was observed that each tablet was completely dispersed in under three (3) minutes.

[0126] Another study using the tablets compounded according to this Example evaluated the bioactivity of the tablets in five (5) adult critical care patients. Each subject was administered one tablet via ng with a small amount of water, and the pH of ng aspirate was monitored using paper measure. The pH for each patient was evaluated for 6 hours and remained above 4, thus demonstrating the therapeutic benefit of the tablets in these patients.

[0127] Tablets were also prepared by boring out th...

example iii

[0128] PPI Central Core Tablet: Tablets are prepared in a two-step process. First, about 20 mg of omeprazole is formed into a tablet as is known in the art to be used as a central core. Second, about 975 mg sodium bicarbonate USP is used to uniformly surround the central core to form an outer protective cover of sodium bicarbonate. The central core and outer cover are both prepared using standard binders and other excipients to create a finished, pharmaceutically acceptable tablet. The tablets may be swallowed whole with a glass of water.

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Abstract

Disclosed herein are compositions and methods for treating gastric acid disorders employing pharmaceutical compositions comprising a proton pump inhibitor (PPI) in a pharmaceutically acceptable carrier.

Description

[0001] This application is a continuation of U.S. patent application Ser. No. 09 / 901,942, filed on Jul. 9, 2001, which is a continuation-in-part of U.S. patent application Ser. No. 09 / 481,207 filed Jan. 11, 2000, which is a continuation-in-part of U.S. patent application Ser. No. 09 / 183,422 filed on Oct. 30, 1998, now abandoned, which is a continuation-in-part of U.S. patent application Ser. No. 08 / 680,376 filed on Jul. 15, 1996, now U.S. Pat. No. 5,840,737, which claims priority to U.S. Provisional Application Serial No. 60 / 009,608 filed on Jan. 4, 1996. This application claims priority to all such previous applications, and such applications are hereby incorporated herein by reference to the extent permitted by law.BACKGROUND OF INVENTION[0002] Omeprazole is a substituted benzimidazole, 5-methoxy-2-[(4-methoxy--3,5-dimethyl-2-pyridinyl) methyl]sulfinyl]-1H-benzimidazole, that inhibits gastric acid secretion. Omeprazole belongs to a class of antisecretory compounds called proton pu...

Claims

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Application Information

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Patent Type & Authority Applications(United States)
IPC IPC(8): A61K9/00A61K9/20A61K9/22A61K9/24A61K9/28A61K9/46A61K31/00A61K31/198A61K31/4439A61K31/522A61K33/00A61K33/06A61K36/00A61K36/185A61K36/42A61K36/48A61K36/534A61K36/82A61K36/898A61K45/06A61K47/02A61K47/04A61K47/12A61P1/04C07D401/12
CPCA61K9/0007A61K9/0056A61K47/02A61K45/06A61K36/898A61K36/534A61K36/48A61K36/42A61K36/185A61K33/00A61K31/4439A61K31/00A61K9/2813A61K9/209A61K9/2086A61K9/0095A61K9/2009A61K9/2013A61K9/2054A61K9/2081A61K2300/00A61P1/04
Inventor PHILLIPS, JEFFREY OWEN
Owner UNIVERSITY OF MISSOURI
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