Title
A Trial of the Efficacy and Safety of Topical Nitric Oxide in Patients With Anogenital Warts
A Randomised, Multicentre, Double-blind, Placebo-controlled, Dose-ranging Trial to Evaluate the Efficacy, Safety and Tolerability of Three Dose Regimens of Topical Nitric Oxide in Patients With Anogenital Warts
Phase
Phase 2Lead Sponsor
University of AberdeenStudy Type
InterventionalStatus
Completed No Results PostedIndication/Condition
Anogenital Warts Condylomata AcuminataIntervention/Treatment
nitrous oxide ...Study Participants
299Objective To assess the efficacy of the topical application of Nitric Oxide, delivered using acidified nitrite.
Design Multicentre, randomized, controlled, dose ranging trial. A control arm and three doses of acidified nitrite applied topically for 12 weeks with a further 12 weeks of follow up.
Setting The trial setting was in European genitourinary medicine clinics
Participants Male and female volunteers over 18 years of age with between 2 and 50 ano-genital warts, 328 were screened for eligibility and 299 subjects from 40 centres were randomised.
Exclusions Pregnancy; concomitant Sexually Transmitted Disease; internal warts requiring treatment other than surgery /laser; diabetes ; Human Immunodeficiency Virus-positive, immunosuppressed and/or using immunosuppressive therapies; drug abuse.
interventions compared
Control Placebo nitrite cream and placebo citric acid cream twice daily
A) 3% sodium nitrite + 4.5% citric acid creams twice daily
B) 6% sodium nitrite + 9% citric acid creams once daily
C) 6% sodium nitrite + 9% citric acid creams twice daily
Outcomes
Primary proportion of patients with complete clearance of target warts Secondary
Time to clearance
Wart area
Wart count
Patient and investigator assessment of efficacy
Safety
Tolerability
Adherence
Varying doses of sodium nitrite and citric acid co-applied to warts
Placebo
3% sodium nitrite + 4.5% citric acid twice daily
Inclusion Criteria: Males and females over 18 years of age 2-50 warts in the anogenital region. Female patients of child-bearing potential had to be willing to use a non-barrier method of contraception at entry and for the duration of the study. all patients had to be willing to use barrier protection for the duration of the study. All patients had to be able to comply with the requirements of the protocol and be likely to return for follow-up visits and had to be contactable for the duration of the study. Exclusion Criteria: Patients with clinically relevant abnormal haematology or biochemistry results (determined from the sample taken at Visit 1). Patients who had used an active therapy for anogenital warts within 2 weeks of randomisation to study drug, i.e. Visit 2. Patients who had used any local supportive medication, including topical corticosteroids or beta-interferon, within 2 weeks of study entry. Patients who had used medication known to adversely affect their haematology profile, including local anaesthetics (benzocaine, lidocaine, etc), nitrofurantoin, sulphonylureas and sulphonamides within 2 weeks of study entry. [Word 'adversely' added by Protocol Amendment 2, 7 May 2002.] Patients with abnormal anogenital skin, such as eczema, or skin that had not healed following surgery (cryosurgery, laser ablation or similar). Patients who were known to have a concomitant sexually transmitted disease that inhibited accurate assessment of their warts. Patients who required treatment other than surgery or laser for internal warts. Male patients with intra-urethral warts [deleted by Protocol Amendment 2, 7 May 2002]. Patients with diabetes (Type I or Type II diabetes). Patients who were known to be HIV-positive. Patients who were known to be immunosuppressed and/or using immunosuppressive therapies. Patients known to abuse alcohol and/or drugs or with a history of chronic alcohol or drug abuse.
