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01-08-2008 | Review Article

A Benefit-Risk Assessment of Benzbromarone in the Treatment of Gout

Was its Withdrawal from the Market in the Best Interest of Patients?

Authors: Ming-Han H. Lee, Garry G. Graham, Kenneth M. Williams, Dr Richard O. Day

Published in: Drug Safety | Issue 8/2008

Abstract

Benzbromarone, a potent uricosuric drug, was introduced in the 1970s and was viewed as having few associated serious adverse reactions. It was registered in about 20 countries throughout Asia, South America and Europe. In 2003, the drug was withdrawn by Sanofi-Synthélabo, after reports of serious hepatotoxicity, although it is still marketed in several countries by other drug companies. The withdrawal has greatly limited its availability around the world, and increased difficulty in accessing it in other countries where it has never been available.

The overall aim of this paper is to determine if the withdrawal of benzbromarone was in the best interests of gouty patients and to present a benefit-risk assessment of benzbromarone. To determine this, we examined (i) the clinical benefits associated with benzbromarone treatment and compared them with the success of alternative therapies such as allopurinol and probenecid, particularly in patients with renal impairment; (ii) the attribution of the reported cases of hepatotoxicity to treatment with benzbromarone; (iii) the incidence of hepatotoxicity possibly due to benzbromarone; (iv) adverse reactions to allopurinol and probenecid. From these analyses, we present recommendations on the use of benzbromarone.

Large reductions in plasma urate concentrations in patients with hyperuricaemia are achieved with benzbromarone and most patients normalize their plasma urate. The half-life of benzbromarone is generally short (about 3 hours); however, a uricosuric metabolite, 6-hydroxybenzbromarone, has a much longer half-life (up to 30 hours) and is the major species responsible for the uricosuric activity of benzbromarone, although its metabolism by cytochrome P450 (CYP) 2C9 in the liver may vary between patients as a result of polymorphisms in this enzyme. It is effective in patients with moderate renal impairment. Standard dosages of benzbromarone (100 mg/day) tend to produce greater hypouricaemic effects than standard doses of allopourinol (300 mg/day) or probenecid (1000 mg/ day).

Adverse effects associated with benzbromarone are relatively infrequent, but potentially severe. Four cases of benzbromarone-induced hepatotoxicity were identified from the literature. Eleven cases have been reported by Sanofi-Synthélabo, but details are not available in the public domain. Only one of the four published cases demonstrated a clear relationship between the drug and liver injury as demonstrated by rechallenge. The other three cases lacked incontrovertible evidence to support a diagnosis of benzbromarone-induced hepatotoxicity. If all the reported cases are assumed to be due to benzbromarone, the estimated risk of hepatotoxicity in Europe was approximately 1 in 17 000 patients but may be higher in Japan.

Benzbromarone is also an inhibitor of CYP2C9 and so may be involved in drug interactions with drugs dependent on this enzyme for clearance, such as warfarin. Alternative drugs to benzbromarone have significant adverse reactions. Allopurinol is associated with rare life-threatening hypersensitivity syndromes; the risk of these reactions is approximately 1 in 56 000. Rash occurs in approximately 2% of patients taking allopurinol and usually leads to cessation of prescription of the drug. Probenecid has also been associated with life-threatening reactions in a very small number of case reports, but it frequently interacts with many renally excreted drugs. Febuxostat is a new xanthine oxidoreductase inhibitor, which is still in clinical trials, but abnormal liver function is the most commonly reported adverse reaction.

Even assuming a causal relationship between benzbromarone and hepatotoxicity in the identified cases, benefit-risk assessment based on total exposure to the drug does not support the decision by the drug company to withdraw benzbromarone from the market given the paucity of alternative options. It is likely that the risks of hepatotoxicity could be ameliorated by employing a graded dosage increase, together with regular monitoring of liver function. Determination of CYP2C9 status and consideration of potential interactions through inhibition of this enzyme should be considered. The case for wider and easier availability of benzbromarone for treating selected cases of gout is compelling, particularly for patients in whom allopurinol produces insufficient response or toxicity.

We conclude that the withdrawal of benzbromarone was not in the best interest of patients with gout.

Sternon J, Kocheleff P, Couturier E, et al. Hypouricemizing effect of benzbromarone: study of 24 cases (preliminary results) [in French]. Acta Clin Belg 1967; 22(5): 285–93PubMed

Nivet M, Marcovici J, Compagnon P, et al. The hypo-uricemic action of oral benziodarone [in French]. Sem Hop 1967 Jan 8; 43(2): 135–8PubMed

Bekaert J, Deltour G, Broekhuysen J. Research on the benzofuran series III: study of the thyroid function in man during the administration of an iodized bensofuran derivative (Benziodarone) [in German]. Arch Int Pharmacodyn Ther 1961 Jul 1; 132: 339–48PubMed

Enomoto A, Kimura H, Chairoungdua A, et al. Molecular identification of a renal urate anion exchanger that regulates blood urate levels. Nature 2002 May 23; 417(6887): 447–52PubMed

Medicinal compositions containing 6-hydroxybenzbromarone or salts thereof. European patent EP1767531 [online]. Available from URL: http://www.freepatentsonline.com/EP1767531.html[Accessed 2008 May 19]

Maurer H, Wollenberg P. Urinary metabolites of benzbromarone in man. Arzneimittelforschung 1990 Apr; 40(4): 460–2PubMed

de Vries JX, Walter-Sack I, Ittensohn A, et al. Benzbromarone hydroxylation in man: defective formation of the 6-hydroxybenzbromarone metabolite. Clin Investig 1993 Nov; 71(11): 947–52PubMedCrossRef

McDonald MG, Rettie AE. Sequential metabolism and bioactivation of the hepatotoxin benzbromarone: formation of glutathione adducts from a catechol intermediate. Chem Res Toxicol 2007 Dec; 20(12): 1833–42PubMedCrossRef

van der Klauw MM, Houtman PM, Stricker BH, et al. Hepatic injury caused by benzbromarone. J Hepatol 1994 Mar; 20(3): 376–9PubMedCrossRef

10.

Wagayama H, Shiraki K, Sugimoto K, et al. Fatal fulminant hepatic failure associated with benzbromarone [letter]. J Hepatol 2000 May; 32(5): 874PubMedCrossRef

11.

Suzuki T, Suzuki T, Kimura M, et al. A case of fulminant hepatitis, possibly caused by benzbromarone [in Japanese]. Nippon Shokakibyo Gakkai Zasshi 2001 Apr; 98(4): 421–5PubMed

12.

Arai M, Yokosuka O, Fujiwara K, et al. Fulminant hepatic failure associated with benzbromarone treatment: a case report. J Gastroenterol Hepatol 2002 May; 17(5): 625–6PubMedCrossRef

13.

Jansen TL, Reinders MK, van Roon EN, et al. Benzbromarone withdrawn from the European market: another case of “absence of evidence is evidence of absence”? [letter]. Clin Exp Rheumatol 2004 Sep–Oct; 22(5): 651PubMed

14.

Thomson Healthcare. Benzbromarone. In: Martindale: the complete drug reference (internet database) [online]. Available from URL: http://www.medicinescomplete.com/mc/ [Accessed 2008 May 5]

15.

Nakamura N. Efficacy of benzbromarone for hyperuricemia [in Japanese]. Rinsho to Kenkyu 1971; 48(11): 2956–60

16.

de Gery A, Auscher C, Saporta L, et al. Treatment of gout and hyperuricaemia by benzbromarone, ethyl 2 (dibromo-3,5 hydroxy-4 benzoyl)-3 benzofuran. Adv Exp Med Biol 1974; 41: 683–9PubMed

17.

Ravera R. Benzbromarone in the treatment of hyperuricemias [in Italian]. Minerva Med 1975 Mar 7; 66(17): 783–800PubMed

18.

Didier M, Olmer M. Hypouricemic effect of benzbromarone especially in kidney failure [in French]. Sem Hop 1978 Apr; 54(9–12): 463–5PubMed

19.

Ferber H, Bader U, Matzkies F. The action of benzbromarone in relation to age, sex and accompanying diseases. Adv Exp Med Biol 1980; 122A: 287–94PubMed

20.

Bluestone R, Klinenberg J, Lee IK. Benzbromarone as a long-term uricosuric agent. Adv Exp Med Biol 1980; 122A: 283–6PubMed

21.

Scott JT. Comparison of allopurinol and probenecid. Ann Rheum Dis 1966 Nov; 25(6): 623–6PubMed

22.

Zurcher RM, Bock HA, Thiel G. Excellent uricosuric efficacy of benzbromarone in cyclosporin-A-treated renal transplant patients: a prospective study. Nephrol Dial Transplant 1994; 9(5): 548–51PubMed

23.

Nakamura N. Efficacy of benzbromarone for hyperuricemia: part 2. Comparison with allopurinol [in Japanese]. Rinsho to Kenkyu 1972; 49(5): 1381–4

24.

Mertz DP. The uric acid-lowering action of benzbromarone effervescent granules and allopurinol: comparative studies (author’s translation) [in German]. MMW Munch Med Wochenschr 1978 Oct 20; 120(42): 1387–90PubMed

25.

Schepers GW. Benzbromarone therapy in hyperuricaemia: comparison with allopurinol and probenecid. J Int Med Res 1981; 9(6): 511–5PubMed

26.

Perez-Ruiz F, Alonso-Ruiz A, Calabozo M, et al. Efficacy of allopurinol and benzbromarone for the control of hyperuricaemia: a pathogenic approach to the treatment of primary chronic gout. Ann Rheum Dis 1998 Sep; 57(9): 545–9PubMedCrossRef

27.

Perez-Ruiz F, Calabozo M, Fernandez-Lopez M, et al. Treatment of chronic gout in patients with renal function impairment. J Clin Rheumatol 1999; 5(2): 49–55PubMedCrossRef

28.

Hanvivadhanakul P, Akkasilpa S, Deesomchok U. Efficacy of benzbromarone compared to allopurinol in lowering serum uric acid level in hyperuricemic patients. J Med Assoc Thai 2002 Jun; 85 Suppl. 1: S40–7PubMed

29.

Liang L, Xu N, Zhang H, et al. A randomized controlled study of benzbromarone and probenecid in the treatment of gout. West China Medical Journal 1994; 9(4): 405–8

30.

Mertz DP. Reducing the risks in the treatment of gout and hyperuricaemia (author’s translation) [in German]. Dtsch Med Wochenschr 1976 Aug 27; 101(35): 1288–92PubMedCrossRef

31.

Frerick H, Schaefer J, Rabinovici K, et al. Longterm treatment of hyperurikemia and gout; randomised study. Therapiewoche 1987; 37(36): 3379–84

32.

Berg H. Effectiveness and tolerance of long-term uricosuric treatment [in German]. Z Gesamte Inn Med 1990 Dec 1; 45(23): 719–20PubMed

33.

Akkasilpa S, Osiri M, Deesomchok U, et al. The efficacy of combined low dose of allopurinol and benzbromarone compared to standard dose of allopurinol in hyperuricemia. J Med Assoc Thai 2004 Sep; 87(9): 1087–91PubMed

34.

Arntz HR, Dreykluft HR, Leonhardt H. Effect of uric acid lowering drugs in low dosage in patients with hyperuricemia and hypertriglyceridemia in a randomized group study [in German]. Fortschritte der Medizin 1979; 97(27): 1212–4PubMed

35.

Adams PF, Hendershot GE, Marano MA. Current estimates from the National Health Interview Survey, 1996. Vital Health Stat 10 1999 Oct; (200): 1–203

36.

Roddy E, Zhang W, Doherty M. The changing epidemiology of gout. Nat Clin Pract Rheumatol 2007 Aug; 3(8): 443–9PubMedCrossRef

37.

Stewart OJ, Silman AJ. Review of UK data on the rheumatic diseases: 4.Gout. Br J Rheumatol1990 Dec; 29(6): 485–8PubMedCrossRef

38.

Arromdee E, Michet CJ, Crowson CS, et al. Epidemiology of gout: is the incidence rising? J Rheumatol 2002 Nov; 29(11): 2403–6PubMed

39.

Kim KY, Ralph Schumacher H, Hunsche E, et al. A literature review of the epidemiology and treatment of acute gout. Clin Ther 2003 Jun; 25(6): 1593–617PubMedCrossRef

40.

Emmerson BT. The management of gout. N Engl J Med 1996 Feb 15; 334(7): 445–51PubMedCrossRef

41.

Gonzalez AA, Puig JG, Mateos FA, et al. Should dietary restrictions always be prescribed in the treatment of gout? Adv Exp Med Biol 1989; 253A: 243–6PubMedCrossRef

42.

Ralston SH, Capell HA, Sturrock RD. Alcohol and response to treatment of gout. BMJ (Clin Res Ed) 1988 Jun 11; 296(6637): 1641–2CrossRef

43.

Sutaria S, Katbamna R, Underwood M. Effectiveness of interventions for the treatment of acute and prevention of recurrent gout: a systematic review. Rheumatology (Oxford) 2006 Nov; 45(11): 1422–31CrossRef

44.

Wortmann RL. Recent advances in the management of gout and hyperuricemia. Curr Opin Rheumatol 2005 May; 17(3): 319–24PubMedCrossRef

45.

Bland JM, Altman DG. Statistics notes: the odds ratio. BMJ 2000 May 27; 320(7247): 1468PubMedCrossRef

46.

Arellano F, Sacristan JA. Allopurinol hypersensitivity syndrome: a review. Ann Pharmacother 1993 Mar; 27(3): 337–43PubMed

47.

Ferraz MB, O’Brien B. A cost effectiveness analysis of urate lowering drugs in nontophaceous recurrent gouty arthritis. J Rheumatol 1995 May; 22(5): 908–14PubMed

48.

Zhang W, Doherty M, Bardin T, et al. EULAR evidence based recommendations for gout. Part II: management. Report of a task force of the EULAR Standing Committee for International Clinical Studies Including Therapeutics (ESCISIT). Ann Rheum Dis 2006 Oct; 65(10): 1312–24PubMedCrossRef

49.

Day RO, Miners JO, Birkett DJ, et al. Allopurinol dosage selection: relationships between dose and plasma oxipurinol and urate concentrations and urinary urate excretion. Br J Clin Pharmacol 1988 Oct; 26(4): 423–8PubMedCrossRef

50.

Emmerson BT, Gordon RB, Cross M, et al. Plasma oxipurinol concentrations during allopurinol therapy. Br J Rheumatol 1987 Dec; 26(6): 445–9PubMedCrossRef

51.

Jordan KM, Cameron JS, Snaith M, et al. British Society for Rheumatology and British Health Professionals in Rheumatology guideline for the management of gout. Rheumatology (Oxford) 2007 Aug; 46(8): 1372–4CrossRef

52.

Dalbeth N, Kumar S, Stamp L, et al. Dose adjustment of allopurinol according to creatinine clearance does not provide adequate control of hyperuricemia in patients with gout. J Rheumatol 2006 Aug; 33(8): 1646–50PubMed

53.

Walter-Sack I, de Vries JX, Ernst B, et al. Uric acid lowering effect of oxipurinol sodium in hyperuricemic patients: therapeutic equivalence to allopurinol. J Rheumatol 1996 Mar; 23(3): 498–501PubMed

54.

Elion GB, Yu TF, Gutman AB, et al. Renal clearance of oxipurinol, the chief metabolite of allopurinol. Am J Med 1968 Jul; 45(1): 69–77PubMedCrossRef

55.

Gibson T, Rodgers V, Potter C, et al. Allopurinol treatment and its effect on renal function in gout: a controlled study. Ann Rheum Dis 1982 Feb; 41(1): 59–65PubMedCrossRef

56.

Tarng DC, Lin HY, Shyong ML, et al. Renal function in gout patients. Am J Nephrol 1995; 15(1): 31–7PubMedCrossRef

57.

Hande KR, Noone RM, Stone WJ. Severe allopurinol toxicity. Description and guidelines for prevention in patients with renal insufficiency. Am J Med 1984 Jan; 76(1): 47–56PubMedCrossRef

58.

Walter-Sack I, de Vries JX, Ittensohn A, et al. Benzbromarone disposition and uricosuric action; evidence for hydroxilation instead of debromination to benzarone. Klin Wochenschr 1988 Feb 15; 66(4): 160–6PubMedCrossRef

59.

Jain AK, Ryan JR, McMahon FG, et al. Effect of single oral doses of benzbromarone on serum and urinary uric acid. Arthritis Rheum 1974 Mar–Apr; 17(2): 149–57PubMedCrossRef

60.

Broekhuysen J, Pacco M, Sion R, et al. Metabolism of benzbromarone in man. Eur J Clin Pharmacol 1972 Mar; 4(2): 125–30PubMedCrossRef

61.

Kunishima C, Inoue I, Oikawa T, et al. The metabolism, toxicity and pharmacological studies of benzbromarone (Urinorm). J Saitama Med School 2003; 30(4): 187–94

62.

Uchida S, Shimada K, Misaka S. Influences of CYP2C9 genotype on pharmacokinetics and pharmacodynamics of benzbromarone [abstract P 13. Clin Pharmacol Ther 2006; 79(2): 13CrossRef

63.

Lee CR, Goldstein JA, Pieper JA. Cytochrome P450 2C9 polymorphisms: a comprehensive review of the in vitro and human data. Pharmacogenetics 2002 Apr; 12(3): 251–63PubMedCrossRef

64.

Walter-Sack I, de Vries JX, von Bubnoff A, et al. Biotransformation and uric acid lowering effect of benzbromarone in patients with liver cirrhosis: evidence for active benzbromarone metabolites? Eur J Med Res 1995 Oct 16; 1(1): 16–20PubMed

65.

Heel RC, Brogden RN, Speight TM, et al. Benzbromarone: a review of its pharmacological properties and therapeutic use in gout and hyperuricaemia. Drugs 1977; 14: 349–66PubMedCrossRef

66.

Rizwan AN, Burckhardt G. Organic anion transporters of the SLC22 family: biopharmaceutical, physiological, and pathological roles. Pharm Res 2007 Mar; 24(3): 450–70PubMedCrossRef

67.

Ichida K, Hosoyamada M, Kimura H, et al. Urate transport via human PAH transporter hOAT1 and its gene structure. Kidney Int 2003 Jan; 63(1): 143–55PubMedCrossRef

68.

Sommers DK, Van Wyk M, Moncrieff J, et al. Renal Secretory mechanisms for ampicillin and uric acid. S Afr Med J 1987; 83: 114–5

69.

Politta G, Berthoud S, Gaudin G, et al. Mechanism of uricosuric action of benzbromaron [in French]. Schweiz Rundsch Med Prax 1973 Oct 30; 62(44): 1345–50PubMed

70.

Kippen I, Nakata N, Honda S, et al. Uptake of uric acid by separated renal tubules of the rabbit. II. Effects of drugs. J Pharmacol Exp Ther 1977 Apr; 201(1): 226–32PubMed

71.

Moriwaki Y, Yamamoto T, Takahashi S, et al. Analysis of uric acid transport in renal tubules using benzbromarone and pyrazinamide. Int J Clin Pharmacol Ther Toxicol 1990 Feb; 28(2): 84–8PubMed

72.

Kumar S, Ng J, Gow P. Benzbromarone therapy in management of refractory gout. NZ Med J 2005 Jun 24; 118(1217): U1528

73.

Perez-Ruiz F, Calabozo M, Pijoan JI, et al. Effect of uratelowering therapy on the velocity of size reduction of tophi in chronic gout. Arthritis Rheum 2002 Aug; 47(4): 356–60PubMedCrossRef

74.

Masbernard A, Giudicelli CP. Ten years’ experience with benzbromarone in the management of gout and hyperuricaemia. S Afr Med J 1981 May 9; 59(20): 701–6PubMed

75.

Boss GR, Seegmiller JE. Hyperuricemia and gout: classification, complications and management. N Engl J Med 1979 Jun 28; 300(26): 1459–68PubMedCrossRef

76.

Mertz DP, Eichhorn R. Does benzbromarone in therapeutic doses raise renal excretion of oxipurinol? Klin Wochenschr 1984 Dec 17; 62(24): 1170–2PubMedCrossRef

77.

Ruffer C, Zorn G, Henkel E, et al. Influence of benzbromarone on the pharmacokinetics and pharmacodynamics of oxipurinol [in German]. Arzneimittelforschung 1982; 32(9): 1149–52PubMed

78.

Loffler W, Grobner W, Zollner N. Uric acid-lowering effect of a combination of benzbromarone and allopurinol: studies under standardized dietary conditions [in German]. Arzneimittelforschung 1983; 33(12): 1687–91PubMed

79.

Yamamoto T, Moriwaki Y, Takahashi S, et al. Effects of pyrazinamide, probenecid, and benzbromarone on renal excretion of oxypurinol. Ann Rheum Dis 1991 Sep; 50(9): 631–3PubMedCrossRef

80.

Bartels EC, Matossian GS. Gout: six-year follow-up on probenecid (benemid) therapy. Arthritis Rheum 1959 Jun; 2(3): 193–202PubMedCrossRef

81.

Thompson GR, Duff IF, Robinson WD, et al. Long term uricosuric therapy in gout. Arthritis Rheum 1962 Aug; 5: 384–96PubMedCrossRef

82.

Yue TF, Gutman AB. Effect of allopurinol (4-hydroxypyrazolo-(3,4-D)pyrimidine) on serum and urinary uric acid in primary and secondary gout. Am J Med 1964 Dec; 37: 885–98PubMedCrossRef

83.

Reinders MK, van Roon EN, Houtman PM, et al. Biochemical effectiveness of allopurinol and allopurinol-probenecid in previously benzbromarone-treated gout patients. Clin Rheumatol 2007; 26(9): 1459–65PubMedCrossRef

84.

Stocker SL, Williams KM, McLachlan AJ, et al. Pharmacokinetic and pharmacodynamic interaction between allopurinol and probenecid in healthy subjects. Clin Pharmacokinet 2008; 47(2): 111–8PubMedCrossRef

85.

Wallis RB. Mechanisms of action of sulphinpyrazone. Thromb Res Suppl 1983; 4: 31–8PubMedCrossRef

86.

Pedersen AK, FitzGerald GA. The human pharmacology of platelet inhibition: pharmacokinetics relevant to drug action. Circulation 1985 Dec; 72(6): 1164–76PubMedCrossRef

87.

Kersley GD. Allopurinol in primary gout with and after the administration of uricosuric agents. Ann Rheum Dis 1966 Nov; 25 (6 Suppl.): 643–4PubMed

88.

Tomlinson B. Febuxostat (Teijin/Ipsen/TAP). Curr Opin Investig Drugs 2005 Nov; 6(11): 1168–78PubMed

89.

Schumacher HR, Becker Jr MA, Wortmann RL, et al. Febuxostat compared with allopurinol in patients with hyperuricemia and gout. N Engl J Med 2005 Dec 8; 353(23): 2450–61PubMedCrossRef

90.

Kaufmann P, Torok M, Hanni A, et al. Mechanisms of benzarone and benzbromarone-induced hepatic toxicity. Hepatology 2005 Apr; 41(4): 925–35PubMedCrossRef

91.

Bichet N, Cahard D, Fabre G, et al. Toxicological studies on a benzofuran derivative: III. Comparison of peroxisome proliferation in rat and human hepatocytes in primary culture. Toxicol Appl Pharmacol 1990 Dec; 106(3): 509–17PubMedCrossRef

92.

Butler EG, Ichida T, Maruyama H, et al. Toxicological studies on a benzofurane derivative. II. Demonstration of peroxisome proliferation in rat liver. Toxicol Appl Pharmacol 1990 Dec; 106(3): 500–8PubMedCrossRef

93.

Parzefall W, Schuppler J, Barthel G, et al. Toxicological studies on a benzofurane derivative. I. A comparative study with phenobarbital on rat liver. Toxicol Appl Pharmacol 1990 Dec; 106(3): 482–99PubMedCrossRef

94.

Enayetallah AE, French RA, Thibodeau MS, et al. Distribution of soluble epoxide hydrolase and of cytochrome P450 2C8 2C9, and 2J2 in human tissues. J Histochem Cytochem 2004; 52(4): 447–54PubMedCrossRef

95.

Takahashi H, Sato T, Shimoyama Y, et al. Potentiation of anticoagulant effect of warfarin caused by enantioselective metabolic inhibition by the uricosuric agent benzbromarone. Clin Pharmacol Ther 1999 Dec; 66(6): 569–81PubMedCrossRef

96.

Sevilla-Mantilla C, Ortega L, Agundez JA, et al. Leflunomide-induced acute hepatitis. Dig Liver Dis 2004 Jan; 36(1): 82–4PubMedCrossRef

97.

Larrey D, Pageaux GP. Genetic predisposition to drug-induced hepatotoxicity. J Hepatol 1997; 26 Suppl. 2: 12–21CrossRef

98.

Lilly MB, Omura GA. Clinical pharmacology of oral intermediate-dose methotrexate with or without probenecid. Cancer Chemother Pharmacol 1985; 15(3): 220–2PubMedCrossRef

99.

Chaibriant H. Stop marketing of proprietary medical product DESURIC(Rm) (benzbromarone) [online]. Available from URL: http://afssaps.sante.fr/htm/10/filcoprs/030403.htm [Accessed 2008 May 19]

100.

Benzbromarone: withdrawn due to reports of liver damage. WHO Pharmaceuticals Newsletter; 2003: 1

101.

Department des alertes [online]. Available from: http://afssap-s.sante.fr/pdf/5/bilan04b.pdf [Accessed 2008 May 19]

102.

Masbernard A, Giudicelli CP. Ten years’ experience with benzbromarone in cyclosporin-A-treated renal transplant patients: a prospective study. Nephrol Dial Transplant 1994; 9(5): 548–51

103.

Navarro VJ, Senior JR. Drug-related hepatotoxicity. N Engl J Med 2006 Feb 16; 354(7): 731–9PubMedCrossRef

104.

Department of Economic and Social Affairs United Nations. Population and vital statistics report series A Vol. LIX, No. 1. New York: United Nations; 2007

105.

Sarawate CA, Brewer KK, Yang W, et al. Gout medication treatment patterns and adherence to standards of care from a managed care perspective. Mayo Clinic Proceedings 2006; 81: 925–34PubMedCrossRef

106.

Sgro C, Clinard F, Ouazir K, et al. Incidence of drug-induced hepatic injuries: a French population-based study. Hepatology 2002; 36(2): 451–5PubMedCrossRef

107.

McInnes GT, Lawson DH, Jick H. Acute adverse reactions attributed to allopurinol in hospitalised patients. Ann Rheum Dis 1981 Jun; 40(3): 245–9PubMedCrossRef

108.

Bardin T. Current management of gout in patients unresponsive or allergic to allopurinol. Joint Bone Spine 2004 Nov; 71(6): 481–5PubMedCrossRef

109.

Bocquet H, Bagot M, Roujeau JC. Drug-induced pseudolymphoma and drug hypersensitivity syndrome (drug rash with eosinophilia and systemic symptoms: DRESS). Semin Cutan Med Surg 1996 Dec; 15(4): 250–7PubMedCrossRef

110.

Chan HL, Stern RS, Arndt KA, et al. The incidence of erythema multiforme, Stevens-Johnson syndrome, and toxic epidermal necrolysis: a population-based study with particular reference to reactions caused by drags among outpatients. Arch Dermatol 1990 Jan; 126(1): 43–7PubMedCrossRef

111.

Roujeau JC, Kelly JP, Naldi L, et al. Medication use and the risk of Stevens-Johnson syndrome or toxic epidermal necrolysis. N Engl J Med 1995 Dec 14; 333(24): 1600–7PubMedCrossRef

112.

Chung Y. Utilisation of allopurinol in the Australian community. Intern Med J. In Press

113.

Hung SI, Chung WH, Liou LB, et al. HLA-B*5801 allele as a genetic marker for severe cutaneous adverse reactions caused by allopurinol. Proc Natl Acad Sci U S A 2005 Mar 15; 102(11): 4134–9PubMedCrossRef

114.

Myers KW, Katial RK, Engler RJ. Probenecid hypersensitivity in AIDS: a case report. Ann Allergy Asthma Immunol 1998 May; 80(5): 416–8PubMedCrossRef

115.

Izzedine H, Brocheriou I, Becart J, et al. Probenecid-induced membranous nephropathy. Nephrol Dial Transplant 2007 Aug; 22(8): 2405–6PubMedCrossRef

116.

Cunningham RF, Israili ZH, Dayton PG. Clinical pharmacokinetics of probenecid. Clin Pharmacokinet 1981 Mar–Apr; 6(2): 135–51PubMedCrossRef

117.

Szczeklik A, Czerniawska-Mysik G, Nizankowska E. Sulfinpyrazone and aspirin-induced asthma. N Engl J Med 1980 Sep 18; 303(12): 702–3PubMed

118.

Committee on the Review of Medicines. Recommendations on phenylbutazone, oxyphenbutazone, feprazone, allopurinol, colchicine, probenecid, and sulphinpyrazone. BMJ 1978 Jun 3; 1(6125): 1466–7CrossRef

119.

Pedersen AK, Jakobsen P, Kampmann JP, et al. Clinical pharmacokinetics and potentially important drug interactions of sulphinpyrazone. Clin Pharmacokinet 1982 Jan–Feb; 7(1): 42–56PubMedCrossRef

120.

Caforio AL, Gambino A, Tona F, et al. Sulfinpyrazone reduces cyclosporine levels: a new drag interaction in heart transplant recipients. J Heart Lung Transplant 2000 Dec; 19(12): 1205–8PubMedCrossRef

121.

Ferrara LA, Mancini M, Marotta T, et al. Interference by sulphinpyrazone with the antihypertensive effects of oxprenolol. Eur J Clin Pharmacol 1986; 29(6): 717–9PubMedCrossRef

122.

Neogi T, Hunter DJ, Chaisson CE, et al. Frequency and predictors of inappropriate management of recurrent gout attacks in a longitudinal study. J Rheumatol 2006 Jan; 33(1): 104–9PubMed

Title: A Benefit-Risk Assessment of Benzbromarone in the Treatment of Gout
Was its Withdrawal from the Market in the Best Interest of Patients?
Authors: Ming-Han H. Lee
Garry G. Graham
Kenneth M. Williams
Dr Richard O. Day
Publication date: 01-08-2008
Publisher: Springer International Publishing
Published in: Drug Safety / Issue 8/2008
Print ISSN: 0114-5916
Electronic ISSN: 1179-1942
DOI: https://doi.org/10.2165/00002018-200831080-00002

At a glance: The ONWARDS insulin icodec trials

Springer Medicine

A Benefit-Risk Assessment of Benzbromarone in the Treatment of Gout

Was its Withdrawal from the Market in the Best Interest of Patients?

Abstract

At a glance: The ONWARDS insulin icodec trials

Springer Medicine

Abstract

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Influence of Chemical Structure on Hypersensitivity Reactions Induced by Antiepileptic Drugs

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Effects of Stratification on Data Mining in the US Vaccine Adverse Event Reporting System (VAERS)

Associations Between Venous Thromboembolism and Antipsychotics

Drug-Related Deaths