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In Reply: The clinical dilemma Dr. Keller describes is the inability to lower the serum urate to a consensually accepted target level of less than 6.0 mg/dL in patients with significant gouty arthritis, when using doses of febuxostat (or for that matter allopurinol) recommended by the US Food and Drug Administration (FDA). This problem is not limited to the management of the gouty patient with renal insufficiency, and we will describe our approach.
In patients failing to meet target serum urate levels, patient adherence to the prescribed dosing should be considered first, since as many as 50% of patients do not adhere to their prescribed hypouricemic medication regimen.1
As Dr. Keller notes, staying below the FDA-approved daily dosage (in the absence of renal insufficiency) of febuxostat (80 mg) or allopurinol (800 mg) will result in some patients not achieving adequate urate-lowering to ameliorate their gout. With clinical and laboratory monitoring for intolerance, we have increased the dose of allopurinol to above 800 mg when necessary; we have explained to patients that this was above the normally recommended dosage of the drug. Of those patients who have been truly intolerant to allopurinol whom we have needed to switch to febuxostat, there have been a few who have required greater than 80 mg daily, and we have increased the dosage, again with extra vigilance in monitoring (liver tests in particular) and after discussion with the patient. Thus far, we have been fortunate in not having had significant side effects, but we do not assume that all patients will tolerate more than 80 mg daily.
Since both febuxostat and allopurinol inhibit the same enzyme (xanthine oxidase) as their mechanism of action, we do not anticipate an advantage to using combined drug therapy, as opposed to increasing the dose of one or the other of the medications. There might even be some loss of efficacy due to inhibitor competition at the enzyme’s active site. Alternatively, in the patient with normal renal function, there might be an advantage to adding probenecid, a uricosuric drug, to either allopurinol or febuxostat, in order to gain some additional hypouricemic effect.
Finally, it is worth reemphasizing that in clinical trials, although febuxostat 80 mg may have outperformed allopurinol at a dose of 300 mg (or less), in clinical practice it is quite reasonable to significantly increase the dosage of allopurinol to at least 800 mg daily as long as it is tolerated, before switching to the very effective but much more expensive alternative. The goal of therapy is, after all, to safely lower the serum urate level to well below its saturation point. Surveys of prescribing habits indicate that physicians have been very reluctant to increase the dose of allopurinol to above 300 mg daily and, unfortunately, do not adequately monitor the efficacy of the therapy in lowering the serum urate level.
- Riedel AA, Nelson M, Joseph-Ridge N, Wallace K, Mac-Donald P, Becker M. Compliance with allopurinol therapy among managed care enrollees with gout: a retrospective analysis of administrative claims. J Rheumatol 2004; 31:1575–1581.
In Reply: The clinical dilemma Dr. Keller describes is the inability to lower the serum urate to a consensually accepted target level of less than 6.0 mg/dL in patients with significant gouty arthritis, when using doses of febuxostat (or for that matter allopurinol) recommended by the US Food and Drug Administration (FDA). This problem is not limited to the management of the gouty patient with renal insufficiency, and we will describe our approach.
In patients failing to meet target serum urate levels, patient adherence to the prescribed dosing should be considered first, since as many as 50% of patients do not adhere to their prescribed hypouricemic medication regimen.1
As Dr. Keller notes, staying below the FDA-approved daily dosage (in the absence of renal insufficiency) of febuxostat (80 mg) or allopurinol (800 mg) will result in some patients not achieving adequate urate-lowering to ameliorate their gout. With clinical and laboratory monitoring for intolerance, we have increased the dose of allopurinol to above 800 mg when necessary; we have explained to patients that this was above the normally recommended dosage of the drug. Of those patients who have been truly intolerant to allopurinol whom we have needed to switch to febuxostat, there have been a few who have required greater than 80 mg daily, and we have increased the dosage, again with extra vigilance in monitoring (liver tests in particular) and after discussion with the patient. Thus far, we have been fortunate in not having had significant side effects, but we do not assume that all patients will tolerate more than 80 mg daily.
Since both febuxostat and allopurinol inhibit the same enzyme (xanthine oxidase) as their mechanism of action, we do not anticipate an advantage to using combined drug therapy, as opposed to increasing the dose of one or the other of the medications. There might even be some loss of efficacy due to inhibitor competition at the enzyme’s active site. Alternatively, in the patient with normal renal function, there might be an advantage to adding probenecid, a uricosuric drug, to either allopurinol or febuxostat, in order to gain some additional hypouricemic effect.
Finally, it is worth reemphasizing that in clinical trials, although febuxostat 80 mg may have outperformed allopurinol at a dose of 300 mg (or less), in clinical practice it is quite reasonable to significantly increase the dosage of allopurinol to at least 800 mg daily as long as it is tolerated, before switching to the very effective but much more expensive alternative. The goal of therapy is, after all, to safely lower the serum urate level to well below its saturation point. Surveys of prescribing habits indicate that physicians have been very reluctant to increase the dose of allopurinol to above 300 mg daily and, unfortunately, do not adequately monitor the efficacy of the therapy in lowering the serum urate level.
In Reply: The clinical dilemma Dr. Keller describes is the inability to lower the serum urate to a consensually accepted target level of less than 6.0 mg/dL in patients with significant gouty arthritis, when using doses of febuxostat (or for that matter allopurinol) recommended by the US Food and Drug Administration (FDA). This problem is not limited to the management of the gouty patient with renal insufficiency, and we will describe our approach.
In patients failing to meet target serum urate levels, patient adherence to the prescribed dosing should be considered first, since as many as 50% of patients do not adhere to their prescribed hypouricemic medication regimen.1
As Dr. Keller notes, staying below the FDA-approved daily dosage (in the absence of renal insufficiency) of febuxostat (80 mg) or allopurinol (800 mg) will result in some patients not achieving adequate urate-lowering to ameliorate their gout. With clinical and laboratory monitoring for intolerance, we have increased the dose of allopurinol to above 800 mg when necessary; we have explained to patients that this was above the normally recommended dosage of the drug. Of those patients who have been truly intolerant to allopurinol whom we have needed to switch to febuxostat, there have been a few who have required greater than 80 mg daily, and we have increased the dosage, again with extra vigilance in monitoring (liver tests in particular) and after discussion with the patient. Thus far, we have been fortunate in not having had significant side effects, but we do not assume that all patients will tolerate more than 80 mg daily.
Since both febuxostat and allopurinol inhibit the same enzyme (xanthine oxidase) as their mechanism of action, we do not anticipate an advantage to using combined drug therapy, as opposed to increasing the dose of one or the other of the medications. There might even be some loss of efficacy due to inhibitor competition at the enzyme’s active site. Alternatively, in the patient with normal renal function, there might be an advantage to adding probenecid, a uricosuric drug, to either allopurinol or febuxostat, in order to gain some additional hypouricemic effect.
Finally, it is worth reemphasizing that in clinical trials, although febuxostat 80 mg may have outperformed allopurinol at a dose of 300 mg (or less), in clinical practice it is quite reasonable to significantly increase the dosage of allopurinol to at least 800 mg daily as long as it is tolerated, before switching to the very effective but much more expensive alternative. The goal of therapy is, after all, to safely lower the serum urate level to well below its saturation point. Surveys of prescribing habits indicate that physicians have been very reluctant to increase the dose of allopurinol to above 300 mg daily and, unfortunately, do not adequately monitor the efficacy of the therapy in lowering the serum urate level.
- Riedel AA, Nelson M, Joseph-Ridge N, Wallace K, Mac-Donald P, Becker M. Compliance with allopurinol therapy among managed care enrollees with gout: a retrospective analysis of administrative claims. J Rheumatol 2004; 31:1575–1581.
- Riedel AA, Nelson M, Joseph-Ridge N, Wallace K, Mac-Donald P, Becker M. Compliance with allopurinol therapy among managed care enrollees with gout: a retrospective analysis of administrative claims. J Rheumatol 2004; 31:1575–1581.