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NCT00321178 Clinical Trial

BURULICO Drug Trial Study Protocol: RCT SR8/SR4+CR4, GHANA

Buruli Ulcer Clinical Trial

BURULICO

Official title:
Randomised Trial for Early Lesions Caused by M. Ulcerans - Comparison Between 8 Weeks Streptomycin and Rifampicin (SR), or 4 Weeks SR Followed by 4 Weeks R Plus Clarithromycin

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT00321178
Other study ID # BURULICODRUGTRIAL
Secondary ID EU FP6 2003-INCO
Status Completed
Phase Phase 2/Phase 3
First received May 2, 2006
Last updated June 29, 2010
Start date May 2006
Est. completion date February 2009

Study information
Verified date April 2010
Source University Medical Center Groningen
Contact n/a
Is FDA regulated No
Health authority Ghana: Ministry of Health
Study type Interventional

Clinical Trial Summary

The standard for treatment Buruli ulcer disease (BUD) used to be surgery but the WHO now advises streptomycin (S, 15 mg/kg daily, intramuscularly) and rifampicin (R,10 mg/kg daily) along with surgery. This preliminary advice was based on observations in 21 patients with pre-ulcerative lesions of BUD, who were given daily SR treatment for varying periods of time. In patients treated with SR for at least 4 weeks, M. ulcerans could no longer be cultured from excised lesions. SR has been introduced without a formal evaluation or comparison with other treatments have been conducted or published, but the impression is that this treatment is beneficial and may cure BUD without additional surgical management.

This study protocol evaluated the hypothesis that early, limited lesions of BUD(pre-ulcerative or ulcerated lesions, ≤ 10 cm maximum diameter), can be healed without recurrence using antimycobacterial drug therapy, without the need for debridement surgery.

In endemic regions in Ghana, patients will be actively recruited and followed if ≥ 5 years of age, and with early (i.e., onset < 6 months) BUD.

- consent by patients and / or care givers / legal representatives

- clinical evaluation, and by

- analysis of three 0.3 cm punch biopsies under local anaesthesia.

- disease confirmation: dry reagent-based polymerase chain reaction (DRB-PCR IS2404)

- randomization: either SR for 8 weeks, or 4 weeks of SR followed by R and clarithromycin (C)

- stratification: ulcerative or pre-ulcerative lesions.

Biopsies processed for histopathology, DRB-PCR-, microscopy, culture, genomic, and sensitivity tests. Lesions assessed regularly for progression or healing during treatment. Drug toxicity monitoring included blood cell counts, liver enzymes and renal tests; and ECG and audiographic tests.

Primary endpoint: healing without recurrence at 12 months follow-up after start of treatment Secondary endpoint: reduction in lesion surface area and/or clinically assessed improvement on completion of treatment, averting the need for debridement surgery.

Recurrences biopsied for confirmation, using PCR, histopathology, and culture. Sample size calculation: 2x74 fully evaluable patients; 80% power to detect a difference of 20 % in recurrence-free cure 12 months after start of treatment between the two groups (60 versus 80%). A Data Safety and Monitoring Board made interim analysis assessments.

Description:

Buruli ulcer disease (BUD) is caused by infection with Mycobacterium ulcerans. It usually starts as a small nodule under the skin but may progress to an ulcerative lesion; and eventually large, usually painless ulcers may develop. When it heals - with surgery or without - it may cause severe scarring resulting in disability and deformity. BUD has emerged as an important infectious disease among rural populations in West Africa. The standard treatment used to be surgical excision for all forms and stages. In 2004. The World Health Organisation advised the use of streptomycin (S, 15 mg/kg daily, intramuscularly) and rifampicin (R,10 mg/kg daily) along with surgery. This preliminary advice was based on the observation in 21 patients with pre-ulcerative lesions of BUD, who were given daily SR treatment for varying periods of time. If patients had received such treatment for at least 4 weeks, M. ulcerans could not be cultured again from the lesions that were excised. The treatment has been implemented in areas with poor access to surgical facilities, in Pobe, Benin, and although no formal evaluation or comparison with other treatments have been conducted or published, the impression is that this treatment is probably beneficial and may cure BUD without the need for additional surgical management.

This study protocol was designed to evaluate the hypothesis that early, limited lesions of Buruli ulcer (M. ulcerans disease; pre-ulcerative or ulcerated lesions, less than or equal to 10 maximum diameter), can be healed without recurrence using antimycobacterial drug therapy, without the need for debridement surgery.

In endemic regions in Ghana, active case finding will be followed by accrual of patients

- 5 years of age and over, with

- limited early (i.e., onset less than 6 months) lesions of Buruli ulcer.

After appropriate consent by patients and / or their care givers or legal representatives, patients will be diagnosed both by

- clinical evaluation, and

- by analysis of three punch biopsies (0.3 cm each) under local anaesthesia.

Only patients with confirmation of M. ulcerans disease - presence of dry reagent-based polymerase chain reaction (DRB-PCR) signal with insertion sequence IS2404, were to be randomised to receive either SR for 8 weeks, or 4 weeks of SR followed by oral treatment consisting of R and clarithromycin (C), as allocated by a computer-generated program; patients will be stratified for ulcerative or pre-ulcerative lesions.

Patients who meet the clinical criteria for M ulcerans disease but are PCR negative, will be offered 8 weeks RS treatment, as is presently provisionally recommended by WHO, and will be evaluated separately, according to the protocol for patients allocated to 8 weeks RS treatment. All biopsies from lesions will be subjected to histopathology, DRB-PCR-, microscopy, culture, genomic, sensitivity tests and external quality control in laboratories in Kumasi (KNUST), Hamburg (BNITM), Munich (DITM) and Antwerp (ITM). Lesions will be assessed regularly for progression or healing during treatment. Drug toxicity will likewise be monitored: renal and audiographic tests for S and C, ECG for C, and liver enzymes for R and C, and blood cell counts for C.

The primary endpoint is healing without recurrence at 12 months follow-up after start of treatment Secondary endpoint is reduction in lesion surface area and/or clinically assessed improvement on completion of treatment, averting the need for debridement surgery.

Recurrences will be biopsied for confirmation, using PCR, histopathology, and culture. In all, 200 patients will need to be screened according to protocol, and 2x74 evaluable patients will be randomised based on a power analysis to detect a difference of 20 % in recurrence-free cure 12 months after start of treatment between the two groups (60 versus 80%). A Data Safety and Monitoring Board will make interim analyses.

Recruitment information / eligibility
Status Completed
Enrollment 151
Est. completion date February 2009
Est. primary completion date January 2008
Accepts healthy volunteers No
Gender Both
Age group 5 Years and older
Eligibility Inclusion Criteria:

- Male or female patients

- At least 5 years of age

- A clinical diagnosis of early M. ulcerans disease including:

- Nodules

- Plaques and small ulcers with or without oedema and less than or equal to 10cm in maximum diameter

- Disease duration no longer than six months

- DRB-PCR positive for M. ulcerans

Exclusion Criteria:

- Treatment with macrolide or quinolone antibiotics, or antituberculous medication, or immunomodulatory drugs including corticosteroids within the previous one month.

- Current treatment with any drugs likely to interact with the study medication, e.g, anticoagulants, cyclosporin, phenytoin, oral contraceptive, and phenobarbitone.

- History of hypersensitivity to rifampicin, streptomycin and or clarithromycin.

- History or having current clinical signs of ascites, jaundice, partial or complete deafness, myasthenia gravis, renal dysfunction (known or suspected), diabetes mellitus, and immune compromise; or evidence for past or present tuberculosis.

- Pregnancy

- Inability to take oral medication or having gastrointestinal disease likely to interfere with drug absorption.

- Excessive alcohol intake.

- Any situation or condition which may compromise ability to comply with the trial procedures.

- Lack of willingness to give informed consent (and/or assent by parent/legal representative).

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment

Related Conditions & MeSH terms

Intervention

Drug:
SR4 - switch to CR4
switch to oral treatment after 4 weeks SR 'standard' therapy

Locations
Country Name City State
Ghana Agogo Hospital Agogo Ashanti Region
Ghana Nkawie-Toaso Hospital Nkawie Ashanti Region

Sponsors (1)
Lead Sponsor Collaborator
University Medical Center Groningen

Country where clinical trial is conducted

Ghana, 

References & Publications (3)

Etuaful S, Carbonnelle B, Grosset J, Lucas S, Horsfield C, Phillips R, Evans M, Ofori-Adjei D, Klustse E, Owusu-Boateng J, Amedofu GK, Awuah P, Ampadu E, Amofah G, Asiedu K, Wansbrough-Jones M. Efficacy of the combination rifampin-streptomycin in preventing growth of Mycobacterium ulcerans in early lesions of Buruli ulcer in humans. Antimicrob Agents Chemother. 2005 Aug;49(8):3182-6. — View Citation

van der Werf TS, Stienstra Y, Johnson RC, Phillips R, Adjei O, Fleischer B, Wansbrough-Jones MH, Johnson PD, Portaels F, van der Graaf WT, Asiedu K. Mycobacterium ulcerans disease. Bull World Health Organ. 2005 Oct;83(10):785-91. Epub 2005 Nov 10. Review. — View Citation

van der Werf TS, van der Graaf WT, Tappero JW, Asiedu K. Mycobacterium ulcerans infection. Lancet. 1999 Sep 18;354(9183):1013-8. Review. — View Citation

Outcome
Type Measure Description Time frame Safety issue
Primary healing without recurrence and without debridement surgery at 12 months follow-up after start of treatment 12 months follow-up after start of treatment Yes
Secondary reduction in lesion surface area and/or clinically assessed improvement on completion of treatment, averting the need for debridement surgery during treatment and follow-up x 12 months Yes
Secondary adverse events during treatment and follow-up x 12 months Yes
Secondary functional limitations at end of follow-up (12 months) Yes
See also
  Status Clinical Trial Phase
Completed NCT01432925 - Timing of Surgical Intervention in Buruli Ulcer Patients Treated With Antibiotics N/A
Completed NCT02281643 - Concomitant Infections of Mansonella Perstans in Tuberculosis and Buruli Ulcer Disease Patients From Ghana Phase 2
Recruiting NCT03957447 - Treat Early and Broad: Thermotherapy of Buruli Ulcer Integrated Into WHO-recommended Wound Management in West Africa
Active, not recruiting NCT02153034 - Pathogenesis and Management of M. Ulcerans Disease, Buruli Ulcer N/A
Recruiting NCT03683745 - Integrated Mapping of Skin-presenting Neglected Tropical Diseases in Liberia
Withdrawn NCT03969940 - Thermotherapy of Buruli Ulcer at Community Level in the Health District of Akonolinga
Recruiting NCT05169554 - Beta-Lactam Containing Regimen for the Shortening of Buruli Ulcer Disease Therapy Phase 2

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