Allopurinol for mania: a randomized trial of allopurinol versus placebo as add-on
treatment to mood stabilizers and/or antipsychotic agents in manic patients with
bipolar disorder.
Author(s): Weiser M(1), Burshtein S, Gershon AA, Marian G, Vlad N, Grecu IG, Tocari E,
Tiugan A, Hotineanu M, Davis JM.
Affiliation(s): Author information:
(1)Division of Psychiatry, Chaim Sheba Medical Center, Tel-Hashomer, Israel;
Sackler School of Medicine, Tel Aviv University, Ramat Aviv, Israel.
Publication date & source: 2014, Bipolar Disord. , 16(4):441-7
OBJECTIVE: An emerging body of evidence supports a role for dysfunctional
purinergic neurotransmission in mood disorders. Adenosine agonists have been
shown to have properties similar to those of dopamine antagonists; there is a
well-characterized interaction between adenosine and dopamine receptors in the
ventral striatum, and increasing adenosinergic transmission has been demonstrated
to reduce the affinity of dopamine agonists for dopamine receptors. Allopurinol
increases adenosine levels in the brain, and hence is hypothesized to reduce the
symptoms of mania. Two randomized, placebo-controlled trials administering add-on
allopurinol to manic patients showed significantly greater improvements in Young
Mania Rating Scale (YMRS) scores for drug compared to placebo, while a more
recent, relatively small, add-on study showed negative results. Based on these
data, our objective was to examine the efficacy of allopurinol as add-on
treatment to mood stabilizers and/or antipsychotic agents in manic patients with
bipolar disorder.
METHODS: We performed a large, well-powered, multicenter, six-week, randomized,
placebo-controlled trial of allopurinol added to mood stabilizers and/or
antipsychotic agents in 180 patients with bipolar disorder in an acute manic
episode.
RESULTS: Both groups showed improvement on the YMRS (effect size of 1.5 for
placebo and 1.6 for allopurinol), with no difference observed between groups on
YMRS scores (t = 0.28, p = 0.78). There was no difference in the proportion of
patients who responded to treatment (defined as showing at least 50% improvement
in YMRS score) between the two groups (p = 0.92), or in dropout rates (p = 0.84).
LIMITATIONS: None of our patients received lithium. However, the side effects of
lithium and its narrow therapeutic index made the use of lithium less common and,
therefore, our study results reflect common current clinical practice. In the
present study, we used a variety of antipsychotic and/or mood stabilizing
treatments, to which we added allopurinol; one might hypothesize that add-on
allopurinol has a different effect in combination with different antipsychotic
agents or mood stabilizers.
CONCLUSIONS: The findings of this large, well-powered study do not support add-on
allopurinol as a treatment for acute mania. This study did not test the efficacy
of allopurinol as monotherapy.
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