Brand Information

RABEKIND

Brand:
RABEKIND

Manufacturer:
MANKIND

Compositions:
Rabeprazole 20mg ec tablets,

Strength	Rate	Packing Style
20mg	33.00	10s e.c.. tablets

List of Related Indications:

Gastroestrophageal reflux disease (GERD)

List Of Drugs:

Rabeprazole - @Proton pump inhibitors-(FDC- List)- (Aug 1991)

Indication Type Description:

Drug Interaction

Indication

Adverse Reaction

Contra-Indications

Dosages/ Overdosage Etc

Other Information

Patient Information

Pharmacology/ Pharmacokinetics

Drug Interaction:

Proton pump inhibitors include-

Esomeprazole, Lansoprazole, Omeprazole, Pantoprazole, Rabeprazole, Pramiprazole

Refer - Omeprazole

Proton pump inhibitors causes a profound and long lasting inhibition of gastric acid secretion. Therefore esomeprazole, lanzoprazole , omeprazole ,pantoprazole and rabeprazole, may interfere with the absoption of drugs where gastric pH is an important detreminant of bioavailability ( eg.ketoconazole, ampicillin, iron salts, digoxin, cyanocobalamin )

CYP450 system - There have been reports of interaction between omeprazole and certain drugs metabolized via the CYP450 system ( eg. cyclosporine, disulfram, benzodiazepines ).

Esmoprazole , lansoprazole, pantoprazole, and rabeprazole are extensively metabolised by CYP2C19 and CYP34A . in clinical studies antacids were used conomittantly with these agents

Rabeprazole may interact with other medication by increasing gastric pH and altering their absorption.

Elimination half-life of digoxin increases upon the administration rabeprazole Studies have indicated that drug interaction with other drugs metabilised by cytochrome P-450 enzyme system

Indication:

U.S. FDA APPROVED DRUGS FROM 01-01-08 TO 31-12-08

Drug name Indication Date of Approval

110. Rabeprazole sodium 16-04-08

Enteric coated pellets 15.4%w/w

(20mg/129.83)

same as approved

122. Rabeprazole Sodium 28-04-08

(with bicrbonate as buffer) 10mg/20mg

For the treatment of gastric ulcer, duodenal

ulcer, Zollinger Ellison Syndrome and GERD

Proton pump inhibitors include-

Esomeprazole, Lansoprazole, Omeprazole, Pantoprazole, Rabeprazole, Pramiprazole

Refer - Omeprazole

Duodenal and gastric ulcer. Reflux osesophagitis

U.S FDA APPROVED DRUGS DURING 2004

199. Rabeprazole sodium Injection 20mg/vial 12-05-2004

For Gastric and Deudonal Ulcers and GERD

218. FDC of Rabeprazole (20mg) + 27-07-2004

Mosapride SR (15mg) tablet

For GERD

242. FDC of Rabeprazole Sodium (20mg) + 04-10-2004

Domperidone (30mg) SR capsule

For GERD

U.S FDA APPROVED DRUGS DURING 2006

150. Rabeprazole 20mg EC+ 28-11-2006

Itropride SR 150mg For GERD

US.FDA APPROVED DRUGS DURING 2007

28. Rabeprazole sodium 20mg/10mg 26-02-07

with sodium bicarbonate as buffer

For Duodenal ulcer GU,Z.E.S & GERD

New Drugs Approved by (DCI) Drug Controller GENERAL - India For Marketing

(Ref- IDMA Publication)

Name of Drug Indication Date of Approval

1.Rabeprozole Anti-ulcer August 1991

2.Rabeprazole 20mg EC 27-12-2001to

+ Itorpride SR 150mg 28-11-2006

Anti-ulcer, Proton Pump inhibitor for GERD

3.Rabeprazole Sodium 12-05-2004

For Gastric and Deudonal

4.Rabeprazole Sodium (with sodium 28-04-2008

bicarbonate as buffer)

10mg/20mg tablets

For treatment of Gastric ulcer, Zollinger Ellison syndtome and GERD

5.Rabeprazole Sodium 20mg/10mg 26-02-2007

with Sodium Bicarbonate as buffer

For Duodenal ulcer , GU, Z.E.S. and GERD

6.Rabeprazole Sodium enteric Coated tablets 16-04-2008

15.4% w/w ( 20mg /129.83 )

same as approved

FIXED DOSE COMBINATIONS APPROVED BY DCG(I)

FROM JANUARY 1961 TILL NOVEMBER 2014

Name of Drug Indication Date of Approval

1.Rabeprazole 20mg + 10-08-2004

Domperidone 30mg SR Capsule

For the treatment of GERD not responding adequately

to Rabeprazole alone

2. Rabeprazole 20mg + 27-07-2004

Mosapride 15mg tablet

For the treatment of GERD not responding adequately

to Rabeprazole alone

Patent Expiry Date of drugs (Ref - IDMA Publication)

Chemical Category Manufacturer/ US Patent

Ingredient- Marketer Expiration Date

Rabeprazole Gastrointestinal Hoechst AG 03-10-2002

Adverse Reaction:

Rabeprazole is well tolerated in both long-term and short-term clinical trials.

Headaches, diarrhea, rash, infection and flu syndrome are the observed adverse effects

Contra-Indications:

None reported

Special precautions:

Rabeprazole should be used with caution in patients with severe hepatic impairment

Dosages/ Overdosage Etc:

Approved on August 1991

Indications:

Duodenal and gastric ulcer.

Dosage:

Duodenal ulcer- 20mg/day for 4 weeks Zollinger- Elilison syndrome- 60mg/day

Missed dose-

1. If you miss a dose of this medicine, take it as soon as possible

2. However, if it is almost time for next dose, skip the missed dose and go back to your regular dosing schedule.

3. Do not double doses.

Other Information:

GASTRO OSEPHAGEAL REFLUX DISEASE (GORD)

Evidence Based Medicine (MIMS- March 2003)

Beneficial

1. Proton Pump Inhibitors such as omeprazole, Lansoprazole, pantoprazole

2. H-2 Antagonists such as cimetidine, ranitidine, famotidine, (less than proton pump inhibitors)

3. Fundoplication

Likely to be beneficial

1. Medical and surgical tretment of GORD in selected patients with extraoesophageal manifestations.

Unknown effectiveness

1. Medical and surgical treatment of GORD in patients with Barrets oesophagus

2. Surgical treatment for non erosive oesophagitis

Key Points

1. One systemic review of randomised clinical trials has found proton inhibitors to be more effective than H-2 antagonists in both erosive and non-erosive oesophagitis. One trial has found no significant differences in the effectiveness of different proton pump inhibitors

2. Surgical treatment has not been adequately evaluated in controlled clinical trials. Medical and surgical treatments have not been adequately compared

3. It is not clear whether patients with Barretts oesophagitis benefit from medical or surgical treatment of their gastro oesophageal reflux

4. There is limited, conflicting evidence on the basis on the benefits of treating gastro oesophageal reflux in patients with extra oesophageal manifestations (such as asthma)

Patient Information:

Refer - Omeprazole

Pharmacology/ Pharmacokinetics:

Pharmacology:

Rabeprazole is effective in treatment, for the healing and relief of symptoms of duodenal and benign gastric ulcers of GERD and for the maintenance of healed ulcers. H-pylori eradication. It causes dose dependent inhibition of acid secretion and has a more rapid onset of action. Rabeprazole causes dose dependent inhibition of histamine-stimulated acid secretion.

Pharmacokinetics:

Rabeprazole is rapidly absorbed after oral administration. The oral bioavailability of rabeprazole is approximately 52%. The time to reach cmax is about 2.9 to 3.8 hrs. after administration of a single dose of 10 -80mg.

The drug is 96.3% plasma bound. it is rapidly cleared from the body by hepatic metabolism and renal excretion.The drug has a half-life of 1 hour after administration of single or multiple doses of 10-80mg. After administration of radiolabeled rabiprazole,approximately 90% of the dose was excreted in the urine and the remaining was excreted in the faces.The plasma elimination half-life of rabeprazole is 1-2 hrs.

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