Role of Medication in Making Urine Less Acidic As Part of Kidney Stone Prevention

Background and Rationale

Urinary stone disease (USD) has been increasing with a recent prevalence estimate of 11% in the United States. Recurrence is common, with up to 50% of individuals experiencing another stone event within 10 years without treatment. This condition results in pain, diminished quality of life, missed work and school, as well as chronic kidney disease and renal failure, and carries significant economic implications as USD is the most expensive non-malignant urologic condition in the United States.

Diet modification and pharmacotherapy form the cornerstones of kidney stone prevention. Alkalinization of urine is commonly used to prevent kidney stone recurrence. Physiologically, urine alkalinization increases urinary pH and raises urinary citrate levels. Correction of acidic urine pH (<5.5) can counteract uric acid crystallization. Additionally, increased citrate levels are known to be a potent inhibitor of calcium stone formation by binding directly to urinary calcium and inhibiting crystal nucleation. Therefore, alkali therapy addresses risk factors for several types of kidney stones and is recommended for patients with recurrent calcium stones with or without hypocitraturia, uric acid stones, or cystine stones.

Potassium citrate is the most commonly prescribed form of alkali therapy. It is recommended by multiple national society guidelines for patients with recurrent calcium stones in whom modifiable 24-hour urine (24U) risk factors are absent, already addressed, or for those in whom dietary modification alone was ineffective. Unfortunately, the long-term compliance has been reported to be as low as 13%. Part of the problem is that potassium citrate is not well-tolerated due to its gastrointestinal side effect profile. So even if urinary alkalization is more robust with potassium citrate, the clinical effects will not be realized if patients are not compliant with the medication. Further exacerbating noncompliance is the unavailability of desirable powder forms of potassium citrate (crystal packets), or the cost of the slow-release form of potassium citrate (UroCit-K) estimated to be more than $150 per month, which may be prohibitively expensive for some patients. Additionally, the number of pills needed to be taken on a daily basis is another reason that could lead to noncompliance.

Alternative alkali therapies are available and should be considered. Over-the-counter (OTC) alkali therapy including medicinal foods and dietary supplements have been used as alternatives to traditional potassium citrate therapy for urinary alkalinization. Indeed, OTC therapies are growing in popularity, with half of recurrent stone-formers reporting utilization of alternative medicines. Moreover, the large number of available products further supports the high demand for such alternative agents. However, there is limited evidence to support their use and efficacy as the comparative efficacy, cost, and tolerability between these agents compared to the current gold standard potassium citrate therapy is unknown.

Our research group has previously studied commonly available OTC alternative alkali citrate products to determine the actual quantities of citrate and citrate as alkali in these supplements. This included powder products such as Litholyte®, Moonstone®, and NOW® Potassium citrate. Litholyte® powder was felt to provide reasonable balance between alkali citrate, cost, and ease of consumption. To build upon this work, we aim to perform an open-label Phase-1 clinical trial using Litholyte®, a dietary supplement containing potassium/magnesium citrate, and compare its metabolic effects to the gold standard potassium citrate (UroCit-K) therapy. We hypothesize that in recurrent stone formers, Litholyte® products will result in similar urinary alkalinization and urinary citrate levels compared to UroCit-K but will be better tolerated and less costly.