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Buruli ulcer from a difficult past to a hopeful future
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Buruli ulcer (Mycobacterium ulcerans infection)

12 January 2023

Key facts

  • Buruli ulcer is a chronic debilitating disease caused by an environmental Mycobacterium ulcerans.
  • At least 33 countries with tropical, subtropical and temperate climates have reported Buruli ulcer in Africa, South America and Western Pacific regions.
  • It often affects the skin and sometimes bone and can lead to permanent disfigurement and long-term disability.
  • The mode of transmission is not known and there is no prevention for the disease.

Overview

Buruli ulcer is caused by a bacterium called Mycobacterium ulcerans. The bacterium produces a toxin that causes the skin damage. Without early treatment, Buruli ulcer can  lead to long-term disability. The germ that causes Buruli ulcer belongs to the same family of those that cause tuberculosis and leprosy. It is still unclear how people get Buruli ulcer from the environment.

Scope of the problem

Buruli ulcer has been reported in 33 countries in Africa, the Americas, Asia and the Western Pacific. Most cases occur in tropical and subtropical regions except in Australia and Japan. Out of the 33 countries, 14 regularly report data to WHO.

The annual number of suspected Buruli ulcer cases reported globally was around 5000 cases up until 2010, when it started to decrease until 2016, reaching its minimum with 1961 cases reported. The number of cases then started to rise again every year, up to 2713 cases in 2018. Since then, the numbers of cases have been declining in 2019 (2271); 2020 (1458) and 2021 (1370). The reductions seen in 2020 and 2021 could be linked to the impact of COVID-19 on active detection activities.

Transmission

The exact mode of transmission of M. ulcerans is still unknown.

Signs and symptoms

Buruli ulcer often starts as a painless swelling (nodule), a large painless area of induration (plaque) or a diffuse painless swelling of the legs, arms or face (oedema). The disease may progress with no pain and fever. Without treatment or sometimes during antibiotics treatment, the nodule, plaque or oedema will ulcerate within 4 weeks. Bone is occasionally affected, causing deformities.

The disease has been classified into three categories of severity: Category I, single small lesion (32%) less than 5 cm on diameter; Category II, non-ulcerative and ulcerative plaque and oedematous forms between 5-15 cm (35%); and Category III lesions more than 15 cm in diameter including, disseminated and mixed forms such as, osteomyelitis and joint involvement (33%).

Lesions frequently occur in the limbs: 35% on the upper limbs, 55% on the lower limbs, and 10% on the other parts of the body. Health workers should be careful in the diagnosis of Buruli ulcer in patients with lower leg lesions to avoid confusion with other causes of ulceration such as diabetes, arterial and venous insufficiency lesion.

Diagnosis

In most cases, experienced health professionals in endemic areas can make a reliable clinical diagnosis, but training is essential.

Differential diagnoses of Buruli ulcer include tropical phagedenic ulcers, chronic lower leg ulcers due to arterial and venous insufficiency (often in elderly populations), diabetic ulcers, cutaneous leishmaniasis, extensive ulcerative yaws and ulcers caused by Haemophilus ducreyi.

Early nodular and papular lesions may be confused with insect bite, boils, lipomas, ganglions, lymph node tuberculosis, onchocerciasis nodules or deep fungal subcutaneous infections. 

Cellulitis may look like oedema caused by M. ulcerans infection but in the case of cellulitis, there is pain and fever. 

HIV infection complicates the management of the patient, making clinical progression more aggressive and resulting in poor treatment outcomes. WHO has published a technical guide to help clinicians in the management of co-infection. 

Four standard laboratory methods can be used to confirm Buruli ulcer: IS2404 polymerase chain reaction (PCR), direct microscopy, histopathology and culture. The bacterium grows best at temperatures between 29–33 °C (Mycobacterium tuberculosis grows at 37 °C) and needs a low (2.5%) oxygen concentration.

In 2019, WHO established the Buruli ulcer Laboratory Network for Africa (1) to help strengthen PCR confirmation in 9 endemic countries in Africa. Thirteen laboratories participate in this network, supported by the American Leprosy Missions, Anesvad, Raoul Follereau Foundation and the Foundation for Innovative Diagnostic and coordinated by the Pasteur Center of Cameroon.

In 2021, WHO completed an online consultation for a draft document on Target Product Profiles to develop rapid test for the diagnosis of Buruli ulcer. This document was published in 2022 and is intended to guide manufacturers in the development of appropriate diagnostic tests. With the availability of simple oral treatment for Buruli ulcer, a rapid test to allow early confirmation of diagnosis can facilitate the timely treatment of the disease. The current turnaround time of a PCR test is too long to guide early treatment decisions.

Treatment

Treatment consists of a combination of antibiotics and complementary treatments. Treatment guidance for health workers can be found in the WHO publication Treatment of mycobacterium ulcerans disease (Buruli ulcer).

A recent study suggests the combination of rifampicin (10 mg/kg once daily) and clarithromycin (7.5 mg/kg twice daily) is now the recommended treatment.

In Australia, a combination of rifampicin (10 mg/kg once daily) and moxifloxacin (400 mg once daily) is routinely used with good results, but its effectiveness has not been proven in a randomized trial.

Priority research for treatment is to shorten the duration of treatment from 8 weeks and studies are in progress to achieve that (2).

Interventions such as wound and lymphoedema management and surgery (mainly debridement and skin grafting) are used to speed up healing, thereby shortening the duration of hospitalization. Physiotherapy is needed in severe cases to prevent disability. Those left with disability require long-term rehabilitation. These same interventions are applicable to other neglected tropical diseases, such as leprosy and lymphatic filariasis.

Prevention and control

There are currently no primary preventive measures for Buruli ulcer. The mode of transmission is not known. Bacillus Calmette–Guérin (BCG) vaccination appears to provide limited protection.

The objective of Buruli ulcer control is to minimize the suffering, disabilities and socioeconomic burden. Early detection and antibiotic treatment are the cornerstones of the control strategy. In many countries, community health workers play a critical role in case detection.

These are the core indicators to measure the progress in the control of Buruli ulcer

  • proportion of cases in category III (late stage) at diagnosis
  • proportion of laboratory-confirmed cases
  • proportion of confirmed cases who have completed a full course of antibiotic treatment.

WHO response

WHO provides technical guidance, develops policies, and coordinates control and research efforts. WHO brings together all major actors involved in Buruli ulcer on a regular basis to share information, coordinate disease control and research efforts, and monitor progress.

WHO supports worked towards three research priorities:

  1. understand the mode of transmission
  2. develop rapid diagnostic tests
  3. establish best-case antibiotic treatments.

To ensure efficiency, sustainability and scale, WHO recommends that Buruli ulcer control should be integrated within skin NTDs approach adapted to the diseases present in a particular country. WHO has developed a Skin App to assist health workers in the field in the diagnosis of skin NTDs including Buruli ulcer.

 

References

  1. https://www.africabulabnet.org/index.php/en/
  2. Beta-Lactam Containing Regimen for the Shortening of Buruli Ulcer Disease Therapy - Full Text View - ClinicalTrials.gov