Available in Brazil
The study presented here is the Swiss-Brazil co-sponsored adaptation of the UNITY trial based
on the WHO core protocol. It has an original governance to better respond to public health
priorities, each country being its own sponsor, allowing for an easier scale-up of the trial
and local adaptations of the protocol.
Background and rationale:
Monkeypox is an emerging viral zoonosis caused by a virus of the same name that is closely
related to smallpox. It is usually endemic in central and West Africa but since May 2022, the
virus has rapidly disseminated to Europe, North and South America, Africa and Australia, and
has predominantly affected gay, bisexual and other men who have sex with men (MSM) with
multiple partners. On 23 July 2022, the World Health Organization (WHO) declared that the
monkeypox outbreak was an international public health emergency. In particular, the WHO
called for the use of antivirals for the treatment of monkeypox cases. This declaration must
therefore be translated not only into extraordinary public health measures but also as a call
for greater investment in research.
This study proposal is a national adaptation for Switzerland and Brazil based on the 'CORE
protocol' developed by the WHO. The research team would like to emphasize that this
randomized trial is international in scope. Thus, they are joining forces to achieve a more
effective and rapid response to important questions, with a harmonized follow-up and in a
time frame that can be useful to the patients the medical staff have been caring for since
the very beginning of this epidemic. Candidate antivirals are already available for testing
in monkeypox. The first studied treatment in this adaptative trial is the antiviral
tecovirimat. Tecovirimat (TPOXX®, SIGA Technologies Inc.) is a treatment for smallpox,
monkeypox and cowpox. Tecovirimat is approved by the European Medicine Agency (EMA) for this
indication for adults and children weighing at least 13 kg, as well as by the United States
Food and Drugs Administration (FDA) under expanded access investigational new drug protocol,
but it is not yet approved in Switzerland and Brazil.
Objectives:
This study aims to evaluate whether tecovirimat is an efficient and safe antiviral in the
treatment of monkeypox in adults and adolescents (14 years old and over).
The primary objective is to evaluate the clinical efficacy of tecovirimat treatment +
standard of care (SOC) compared to placebo + SOC for patients with monkeypox as assessed by
time to visible lesion(s) resolution. The secondary objectives are to evaluate the clinical
efficacy and safety of tecovirimat treatment + SOC compared to placebo + SOC in patients with
monkeypox as assessed by mortality, hospitalization, complications, duration of symptoms and
virological shedding.
Methods:
This study will include adult and adolescent patients aged ≥14 years with a confirmed or
highly suspected monkeypox virus infection and with at least one visible active skin or
mucosal lesion. Individuals with a known hypersensitivity to tecovirimat, who are taking
medications which cannot be interrupted and for which a major interaction has been described
or who, in the judgement of the investigator, will be at significantly increased risk as a
result of participation in the study will not be included. Randomization will be in a ratio
of 1:1 to either tecovirimat treatment combined with SOC or to placebo combined with SOC. All
participants will be followed-up until day 29 and additionally at day 60 for those who accept
this last optional follow-up visit.
Outcome:
The primary outcome is the time for all visible lesions (skin, mucosal) to heal with a new
fresh layer of skin re-epithelialization (i.e. resurfacing of a wound with a new epithelium
layer).
Expected results:
The hypothesis is that prompt oral treatment with tecovirimat will result in a reduction of
the duration of illness in patients with monkeypox that may correlate with the duration of
contagiousness. It is expected that tecovirimat will be well tolerated and acceptable for
these patients.
5Research sites
150Patients around the world