Share on Facebook Share on Twitter Email
Answers.com

ritonavir

 
American Heritage Dictionary:

ri·ton·a·vir

Home > Library > Literature & Language > Dictionary
(rĭ-tŏn'ə-vîr) pronunciation
n.
A protease-inhibiting drug usually used in combination with other drugs to suppress the replication of HIV.

[rito-, of unknown origin + -navir, protease inhibitor suff. (from SAQUINAVIR).]


Search unanswered questions...

Enter a question here...
Search: All sources Community Q&A Reference topics

Oxford A-Z of Medicinal Drugs:

ritonavir

Top
Home > Library > Health > Drugs Directory

A protease inhibitor (see antiviral drugs), similar to indinavir, used in combination with other antiretroviral drugs for the treatment of HIV disease. It is available as capsules or a solution on prescription only.

Side effects:
include stomach and bowel upsets, disturbances of taste, tingling around the mouth or in the fingers and toes, and headache.

Precautions:
ritonavir should not be taken by women who are breastfeeding. It should be used with caution in people with liver or kidney disease, diabetes, diarrhoea, and haemophilia and in pregnant women.

Interactions with other drugs:
ritonavir is a potent inhibitor of several enzyme systems in the liver that are involved in metabolizing drugs; it therefore has the potential to interact with many drugs. A doctor should be consulted before ritonavir is taken with any other drug.

Proprietary preparations:
Norvir; Kaletra (combined with lopinavir).

Previous:ritodrine, risperidone, risedronate sodium
Next:rituximab, rivaroxaban, rivastigmine
Wikipedia on Answers.com:

Ritonavir

Top
Home > Library > Miscellaneous > Wikipedia
Ritonavir
Systematic (IUPAC) name
1,3-thiazol-5-ylmethyl N-[(2S,3S,5S)-3-hydroxy-5-[(2S)-3-methyl-2-{[methyl({[2-(propan-2-yl)-1,3-thiazol-4-yl]methyl})carbamoyl]amino}butanamido]-1,6-diphenylhexan-2-yl]carbamate
Clinical data
Trade names Norvir
AHFS/Drugs.com monograph
MedlinePlus a696029
Pregnancy cat. B (U.S.)
Legal status ℞-only (U.S.)
Routes oral
Pharmacokinetic data
Protein binding 98-99%
Half-life 3-5 hours
Excretion mostly fecal
Identifiers
CAS number 155213-67-5 YesY
ATC code J05AE03
PubChem CID 392622
DrugBank APRD00312
ChemSpider 347980 YesY
UNII O3J8G9O825 YesY
KEGG D00427 YesY
ChEMBL CHEMBL163 YesY
NIAID ChemDB AIDSNO:028478
Chemical data
Formula C37H48N6O5S2 
Mol. mass 720.946 g/mol
SMILES eMolecules & PubChem
 N(what is this?)  (verify)

Ritonavir, with trade name Norvir (Abbott Laboratories), is an antiretroviral drug from the protease inhibitor class used to treat HIV infection and AIDS.

Ritonavir is frequently prescribed with HAART, not for its antiviral action, but as it inhibits the same host enzyme that metabolizes other protease inhibitors. This inhibition leads to higher plasma concentrations of these latter drugs, allowing the clinician to lower their dose and frequency and improving their clinical efficacy.

Contents

History

Ritonavir is manufactured as Norvir by Abbott Laboratories. Research that led to the drug's development was financed by a $3,500,000 federal grant through the National Institutes of Health (NIH) and over $200,000,000 by Abbott Labs. Most of the $200,000,000 figure cited by Abbott paid for clinical trials-despite NIH offering to pay for them-because Abbott was concerned about "public interest" responses to the high prices they projected Norvir would command.[1] The Food and Drug Administration (FDA) approved ritonavir on March 1, 1996, making it the seventh approved antiretroviral drug in the United States. In 2003, Abbott raised the price of a Norvir course from USD $1.71 per day to $8.57 per day, leading to claims of price gouging by patients' groups and some members of Congress. Consumer group Essential Inventions petitioned the NIH to override the Norvir patent, but the NIH announced on August 4, 2004 that it lacked the legal right to allow generic production of Norvir.[2]

Method of action

Ritonavir (center) bound to the active site of HIV protease.

Ritonavir was originally developed as an inhibitor of HIV protease. It is one of the most complex inhibitors. It is now rarely used for its own antiviral activity, but remains widely used as a booster of other protease inhibitors. More specifically, ritonavir is used to inhibit a particular liver enzyme that normally metabolizes protease inhibitors, cytochrome P450-3A4 (CYP3A4).[3] The drug's molecular structure inhibits CYP3A4, so a low dose can be used to enhance other protease inhibitors. This discovery, which has drastically reduced the adverse effects and improved the efficacy of PI's and HAART, was first communicated in an article published in the AIDS Journal in 1997 by the University of Liverpool. This effect does come with a price: it also affects the efficacy of numerous other medications, making it difficult to know how to administer them concurrently. In addition it can cause a large number of side-effects on its own.

Drug interactions

Concomitant therapy of ritonavir with a variety of medications may result in serious and sometimes fatal drug interactions.[4] These interactions can occur with strong inhibitors, strong or moderate inducers or substrates of hepatic cytochrome P450 CYP3A4 isoform.

The list of clinically significant interactions of ritonavir includes but is not limited to following drugs:

Side effects

The most common side effects of ritonavir therapy are[5]:

One of ritonavir's side effects is hyperglycemia. It appears that ritonavir directly inhibits the GLUT4 insulin-regulated transporter, keeping glucose from entering fat and muscle cells[citation needed]. This can lead to insulin resistance and cause problems for Type Ⅱ diabetics.

Conformational polymorphism

 This section needs attention from an expert on the subject. See the talk page for details. WikiProject Pharmacology or the Pharmacology Portal may be able to help recruit an expert. (September 2009)

Norvir was originally dispensed as an ordinary capsule, which did not require refrigeration. The API of the original capsule exhibited strong conformational polymorphism. This threatened existing supplies of ritonavir as the lower energy polymorph caused the therapeutically effective polymorph to convert to the lower energy polymorph on contact. This lower energy polymorph, which was not therapeutically effective, entered production lines and effectively halted production processes.[6] After this discovery in the late 1990s, Abbot withdrew the original capsules from the market, and recommended patients switch to Norvir suspension while researchers worked to solve the problem. The capsules have been replaced with refrigerated gelcaps, to solve the crystallization problem of the original capsules. More recently Norvir has been reformulated into a white oblong solid tablet that no longer required refrigeration.

References

  1. ^ James Love (2004-06-03). "How much has the public invested in ritonavir, and how much has Abbott?". Essential Inventions. http://www.essentialinventions.org/drug/ei06032004.html. Retrieved 2008-05-06. .
  2. ^ Ceci Connolly (2004-08-05). "NIH Declines to Enter AIDS Drug Price Battle". Washington Post. http://www.washingtonpost.com/wp-dyn/articles/A40430-2004Aug4.html. Retrieved 2006-01-16. 
  3. ^ Zeldin RK, Petruschke RA (2004). "Pharmacological and therapeutic properties of ritonavir-boosted protease inhibitor therapy in HIV-infected patients". Journal of Antimicrobial Chemotherapy 53 (1): 4–9. doi:10.1093/jac/dkh029. PMID 14657084. http://jac.oxfordjournals.org/cgi/content/full/53/1/4. 
  4. ^ http://www.merck.com/mmpe/lexicomp/ritonavir.html
  5. ^ http://www.rxlist.com/cgi/generic/ritonavirsol_ad.htm
  6. ^ Bauer J, et al. (2004). "Ritonavir: An Extraordinary Example of Conformational Polymorphism". Pharmaceutical Research 18 (6): 859–866. doi:10.1023/A:1011052932607. PMID 11474792. http://www.springerlink.com/content/k655264600tjh122/. 

Further reading

  • Chemburkar, Sanjay R.; Bauer, John; Deming, Kris; Spiwek, Harry; Patel, Ketan; Morris, John; Henry, Rodger; Spanton, Stephen et al. (2000). "Dealing with the Impact of Ritonavir Polymorphs on the Late Stages of Bulk Drug Process Development". Organic Process Research & Development 4 (5): 413. doi:10.1021/op000023y. 

External links

Antiviral drugs: antiretroviral drugs used against HIV (primarily J05)
Entry/fusion inhibitors
(Discovery & development)
Reverse-transcriptase
inhibitors (RTIs)
(1st generation) Efavirenz°# • Nevirapine#  • Loviride • Delavirdine •
 (2nd generation) diarylpyrimidines (Etravirine, Rilpivirine)  • Lersivirine
Integrase inhibitors
Raltegravir • Elvitegravir • Dolutegravir • Globoidnan A (experimental)  • MK-2048  • BI 224436  
Maturation inhibitors
Bevirimat • Vivecon
Protease Inhibitors (PI)
(Discovery and development)
1st generation
Fosamprenavir° • Lopinavir°# • Nelfinavir# • Ritonavir# • Saquinavir# • Amprenavir • Indinavir#
2nd generation
Combined formulations
Experimental agents
TRIM5alpha (gene)
Other
Failed agents
°DHHS preferred first-line agent. Formerly or rarely used agent.

This entry is from Wikipedia, the leading user-contributed encyclopedia. It may not have been reviewed by professional editors (see full disclaimer)

 
 
Related topics:
Ritonavir
Lopinavir; Ritonavir
Ritonavir capsules

Help us answer these:
Ritonavir is suitable for floating drug delivery?
Is ritonavir fast disintegrating tablets are in market?

Post a question - any question - to the WikiAnswers community:

 

Copyrights:

American Heritage Dictionary. The American Heritage® Dictionary of the English Language, Fourth Edition Copyright © 2007, 2000 by Houghton Mifflin Company. Updated in 2009. Published by Houghton Mifflin Company. All rights reserved.  Read more
 Oxford A-Z of Medicinal Drugs. Market University Press. © 2000, 2003, 2010 An A-Z of Medicinal Drugs. All rights reserved.  Read more
Wikipedia on Answers.com. This article is licensed under the Creative Commons Attribution/Share-Alike License. It uses material from the Wikipedia article Ritonavir Read more

Related answers
» More
Answer these
» More
Follow us
Facebook Twitter
YouTube