Английская Википедия:Flumequine

Материал из Онлайн справочника
Перейти к навигацииПерейти к поиску

Шаблон:Short description Шаблон:Drugbox Flumequine[1] is a synthetic fluoroquinolone antibiotic[2][3] used to treat bacterial infections. It is a first-generation fluoroquinolone antibacterial that has been removed from clinical use and is no longer being marketed.[4] The marketing authorization of flumequine has been suspended throughout the EU.[5] It kills bacteria by interfering with the enzymes that cause DNA to unwind and duplicate. Flumequine was used in veterinarian medicine for the treatment of enteric infections (all infections of the intestinal tract),[6] as well as to treat cattle, swine, chickens, and fish, but only in a limited number of countries.[4][7][8] It was occasionally used in France (and a few other European Countries) to treat urinary tract infections under the trade name Apurone.[4][9] However this was a limited indication[10] because only minimal serum levels were achieved.[11]

History

The first quinolone used was nalidixic acid (was marketed in many countries as Negram) followed by the fluoroquinolone flumequine.[4] The first-generation fluoroquinolone agents, such as flumequine, had poor distribution into the body tissues and limited activity. As such they were used mainly for treatment of urinary tract infections. Flumequine (benzo quinolizine) was first patented in 1973, (German Patent) by Rikker Labs.[12] Flumequine is a known antimicrobial compound described and claimed in U.S. Pat. No. 3,896,131 (Example 3), July 22, 1975.[13] Flumequine is the first quinolone compound with a fluorine atom at the C6-position of the related quinolone basic molecular structure.[14] Even though this was the first fluoroquinolone, it is often overlooked when classifying the drugs within this class by generations and excluded from such a list.

Though used frequently to treat farm animals and on occasion household pets, flumequine was also used to treat urinary tract infections in humans. Flumequine, was used transiently treat urinary infections[9] until ocular toxicity was reported.[15][16][17] as well as liver damage[18] and anaphylactic shock.[19][20]

In 2008, the United States Food and Drug Administration (FDA) requested that all quinolone/fluoroquinolone drugs package inserts include a Black Boxed Warning concerning the risk of spontaneous tendon ruptures, which would have included flumequine. The FDA also requested that the manufacturers send out Dear Doctor Letters regarding this new warning. Such tendon problems have also been associated with flumequine.[21]

Drug residue

The use of flumequine in food animals had sparked considerable debate. Significant and harmful residues of quinolones have been found in animals treated with quinolones and later slaughtered and sold as food products. There has been significant concern regarding the amount of flumequine residue found within food animals such as fish, poultry and cattle.[22][23] In 2003 the Joint FAO/WHO Committee on Food Additives (JECFA) withdrew the maximum residue limits (MRLs) for flumequine and carbadox based on evidence showing both are direct acting genotoxic carcinogens, therefore the Committee was unable to establish an Acceptable Daily Intake (ADI) for human exposure to such residues.[24] Subsequently, in 2006, the JEFCA, re-established the ADI having received appropriate evidence and MRLs were re-specified. The role of JECFA is to evaluate toxicology, residue chemistry and related information and make recommendations for acceptable daily intake (ADI) levels and maximum residue limits (MRLs). At its 16th session, held May 2006, the Committee on Residues of Veterinary Drugs in Foods (CCRVDF) requested information on registered uses of flumequine. As the CCRVDF did not receive any information regarding the registered uses of flumequine that they had requested, the committee members agreed to discontinue work on the MRLs for flumequine in shrimp.[25][26]

Licensed uses

Urinary tract infections (veterinary and human)[27]

Availability

Veterinary use:

  • Solution; Oral; 20% (prescription only)
  • Solution; Oral; 10% (prescription only)

Human use:

  • Tablet; Oral; Flumequine 400 mg (discontinued)

Mode of action

Flumequine is a member of the quinolone antibiotics family, which are active against both Gram-positive and Gram-negative bacteria. It functions by inhibiting DNA gyrase, a type II topoisomerase, and topoisomerase IV,[28] enzymes necessary to separate bacterial DNA, thereby inhibiting cell division.

This mechanism can also affect mammalian cell replication. In particular, some congeners of this drug family (for example those that contain the C-8 fluorine),[29] display high activity not only against bacterial topoisomerases, but also against eukaryotic topoisomerases and are toxic to cultured mammalian cells and in vivo tumor models.[30]

Although quinolones are highly toxic to mammalian cells in culture, its mechanism of cytotoxic action is not known. Quinolone induced DNA damage was first reported in 1986 (Hussy et al.).[31]

Recent studies have demonstrated a correlation between mammalian cell cytotoxicity of the quinolones and the induction of micronuclei.[32][33][34][35]

As such, some fluoroquinolones may cause injury to the chromosome of eukaryotic cells.[36][37][38][39][40][41]

There continues to be considerable debate as to whether or not this DNA damage is to be considered one of the mechanisms of action concerning the severe adverse reactions experienced by some patients following fluoroquinolone therapy.[30][42]

Adverse reactions

Flumequine was associated with severe ocular toxicity, which precluded its use in human patients.[15][16][17] Drug-induced calculi (kidney stones) has been associated with such therapy as well.[43][44][45] Anaphylactic shock induced by flumequine therapy has also been associated with its use.[19][20][46] Anaphylactoid reactions such as shock, urticaria, and Quincke’s oedema have been reported to generally appear within two hours after taking the first tablet. There were eighteen reports listed within the WHO file in 1996.[47] As with all drugs within this class, flumequine therapy may result in severe central nervous system (CNS) reactions,[48][49][50] phototoxicity resulting in skin reactions like erythema, pruritus, urticaria and severe rashes,[51][52] gastrointestinal and neurological disorders.[9]

Drug interactions

Flumequine was found to have no effect on theophylline pharmacokinetics.[53]

Chemistry

Flumequine is a 9-fluoro-6,7-dihydro-5-methyl-1-oxo-1H,5H-benzo[ij]quinolizine-2-carboxylic acid. The molecular formula is C14H12FNO3. It is a white powder, odorless, flavorless, insoluble in water but soluble in organic solvent.[54]

Pharmacokinetics

Flumequine is considered to be well absorbed and is excreted in the urine and feces as the glucuronide conjugates of the parent drug and 7-hydroxyflumequine. It is eliminated within 168 hours post-dosing. However, studies concerning the calf liver showed additional unidentified residues, of which a new metabolite, ml, represented the major single metabolite 24 hours after the last dose and at all subsequent time points. The metabolite ml, which exhibited no antimicrobial activity, was present in both free and protein-bound fractions. The major residue found in the edible tissues of sheep, pigs, and chickens was parent drug together with minor amounts of the 7-hydroxy-metabolite. The only detected residue in trout was the parent drug.[55]

See also

References

Шаблон:Reflist

Шаблон:QuinoloneAntiBiotics

Партнерские ресурсы
Криптовалюты
Магазины
Хостинг
Разное

  1. INN: Lomefloxacin Hydrochloride
  2. Шаблон:Cite journal
  3. Шаблон:Cite journal
  4. 4,0 4,1 4,2 4,3 Шаблон:Cite web
  5. Шаблон:Cite web
  6. Шаблон:Cite book
  7. Шаблон:Cite conference Cattle only in Europe and Latin America. (Limited use in Latin America), Poultry only in Europe, Asia and Latin America, Fish only in Asia
  8. Шаблон:Cite web
  9. 9,0 9,1 9,2 Шаблон:Cite journal
  10. The quinolones (Third Edition 2000) By Vincent T. Andriole Chapter I History and overview By Dr. Peter Ball (page 5)
  11. Шаблон:Cite journal
  12. Шаблон:Cite journal
  13. Шаблон:Cite web
  14. Шаблон:Cite journal
  15. 15,0 15,1 Шаблон:Cite journal
  16. 16,0 16,1 Шаблон:Cite journal
  17. 17,0 17,1 Шаблон:Cite journal
  18. Шаблон:Cite journal
  19. 19,0 19,1 Шаблон:Cite journal
  20. 20,0 20,1 Шаблон:Cite journal
  21. Шаблон:Cite web
  22. Шаблон:Cite conference
  23. Шаблон:Cite web
  24. Шаблон:Cite web
  25. Шаблон:Cite web
  26. Шаблон:Cite web
  27. WHO Drug Information Vol. 2, No. 3, 1988
  28. Шаблон:Cite journal
  29. Шаблон:Cite journal
  30. 30,0 30,1 Шаблон:Cite journal
  31. Шаблон:Cite journal
  32. Шаблон:Cite journal
  33. Шаблон:Cite journal
  34. Шаблон:Cite journal
  35. Шаблон:Cite journal
  36. Шаблон:Cite journal
  37. Шаблон:Cite journal
  38. Шаблон:Cite journal
  39. Шаблон:Cite journal
  40. Шаблон:Cite journal
  41. Шаблон:Cite web
  42. Шаблон:Cite journal
  43. Шаблон:Cite journal
  44. Шаблон:Cite journal
  45. Шаблон:Cite journal
  46. Шаблон:Cite journal
  47. Adverse Reaction Newsletter 1996:1 WHO collaborating centre for international drug monitoring
  48. Шаблон:Cite journal
  49. Шаблон:Cite journal
  50. Шаблон:Cite journal
  51. Шаблон:Cite journal
  52. Шаблон:Cite journal
  53. Шаблон:Cite journal
  54. Шаблон:Cite web
  55. Шаблон:Cite web
Источник — http://wikihandbk.com/ruwiki/index.php?title=Английская_Википедия:Flumequine&oldid=14728932