Chronic Urticaria Clinical Trial
Official title:
A Multi-center, Randomized, Double Blind, Dose Escalating Phase III Study on the Efficacy, Safety and Long Term Outcome of Continuous vs. on Demand Treatment of Chronic Spontaneous Urticaria With Rupatadine.
To compare CSU disease activity at the end of the follow up phase between patients that had been treated daily continuously vs. on-demand in the treatment phase
The treatment of CSU with nsAHs is currently the most common and only licensed therapeutic
option to reduce the patients' wheal and flare type skin reactions and pruritus. CSU is a
highly fluctuating disease and the severity of symptoms can change markedly from day to day.
This is one of the reasons why, in routine daily practice, many patients tend to perform an
on demand rather than a continuous, daily, preventive treatment of their symptoms with nsAHs.
While in the field of allergic rhinitis several studies point towards a better efficacy of
nsAHs if continuously given (6-8), the only study in CSU comparing both treatment approaches
was published by Grob and colleagues (9). They were able to demonstrate that continuous daily
treatment with the nsAH desloratadine resulted in significantly better quality of life as
compared to on demand therapy. While these studies indicate that the treatment schedule can
generally have a major impact on the outcome of treatment, the results on the efficacy of on
demand nsAHs in CSU remains to be confirmed independently.
In addition to the optimal treatment schedule, there is an ongoing discussion regarding the
long-term outcome of nsAH treatment. While the mode of action of nsAHs suggests a pure
symptomatic therapeutic effect, there have been speculations that a disease modification
effect might also occur. Indeed, in 2010, a Japanese group (Kono et al.) presented data on
the EADV meeting in Gothenburg demonstrating that continuous prophylactic antihistamine
therapy of CSU patients with ebastine (a nsAH) for a period of three months was associated
with a lower recurrence rate after discontinuation than the same treatment lasting for only
one month, provided that the drug was effective and safe during early treatment. As of yet,
these results also have to be confirmed independently.
Sufficient reduction of urticarial symptoms requires higher than the licensed dosing of
antihistamines in many CSU patients (10-14). In fact, increasing the dose of nsAHs up to
fourfold has been shown to be more effective as compared to the standard dose in different
subforms of chronic urticaria (10, 11, 14). However, for some patients even high dosed nsAHs
are not enough to effectively suppress disease symptoms (11-14). The exact reasons for this
are still unknown. Probably, other mediators than histamine are also involved in the
development of urticaria symptoms. One such other candidate mediator is platelet activating
factor (PAF). PAF is a potent phospholipid mediator with various biological activities,
including platelet aggregation, airway constriction, hypotension, and vascular permeation.
PAF also mediates allergic reactions and has been claimed to contribute to the pathogenesis
of urticaria. Intradermal PAF injection results in a pruritic wheal and flare reaction in
subjects with and without allergies (15). PAF injection is followed by a dose-dependent
histamine release in vivo (16) and in cold contact urticaria, there is evidence available
that PAF is an additional important mediator associated with the inflammatory reaction in the
skin (17, 18). Notably, Krause et al. could demonstrate that intradermal PAF injection
results in a wheal and flare type skin reaction without inducing mast cell degranulation
(19). PAF may, therefore, be a relevant mediator in the pathogenesis of urticaria that acts
downstream of mast cell activation and is independent of H1-receptor activation.
Rupatadine, is a drug which possesses a potent antihistamine and PAF antagonistic activity
and, recently, it has been demonstrated to be safe and effective in the treatment of chronic
urticaria (3, 4) and cold contact urticaria (5). Notably, it has also been shown that an
increased dose of 20 mg rupatadine is more effective in the treatment of CSU symptoms as
compared to the licensed 10 mg dose (20).
In summary, it seems more than reasonable to use rupatadine as a study drug in patients with
CSU in order to better characterize the best nsAH treatment schedule (continuous vs.
on-demand), the long-term outcome of nsAH therapy and the influence of updosing on the
latter.
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