Sotyktu

Sotyktu can only be obtained with a prescription. Treatment should be started by a doctor experienced in the diagnosis and treatment of the conditions for which Sotyktu is used.

Sotyktu is available as tablets to be taken once a day. The doctor should evaluate the effect of the treatment regularly and may stop treatment if the condition does not improve after 24 weeks.

For more information about using Sotyktu, including dose recommendations, see the package leaflet or contact your doctor or pharmacist. 

Plaque psoriasis

Two main studies involving 1,686 adults with moderate to severe plaque psoriasis compared Sotyktu with placebo (a dummy treatment) and apremilast, another systemic therapy for plaque psoriasis. The studies looked at an improvement of patients’ symptoms after 16 weeks of treatment.

Around 55% of patients treated with Sotyktu had a reduction of at least 75% in their PASI score (a measure of the severity and extent of skin lesions) compared with around 38% of those treated with apremilast and around 11% of those who received placebo.

Additionally, around 51% of patients treated with Sotyktu achieved a sPGA score (a measure of the severity and extent of skin lesions) of 0 or 1 (where 0 and 1 refer to skin clear or almost clear, respectively) and had a reduction of 2 points or more in their sPGA score. Around 33% of those treated with apremilast and around 8% in those who received placebo had these results.

Improvement of symptoms were maintained after 52 weeks of treatment with Sotyktu.

Psoriatic arthritis

Sotyktu was compared with placebo in two main studies involving a total of 1,458 adults with psoriatic arthritis who could not take, or whose condition had not improved enough with, a DMARD. In both studies, the main measure of effectiveness was the number of people who had at least a 20% improvement in signs and symptoms of the disease (ACR20) after 16 weeks of treatment. In the first study, around 54% of people taking Sotyktu achieved ACR20, compared with around 34% of those taking placebo. In the second study, around 54% of people taking Sotyktu achieved ACR20, compared with around 39% of those given placebo. 

Symptoms continued to improve after 16 weeks of treatment with Sotyktu, and results were maintained for up to 52 weeks.

Studies carried out with Sotyktu are described in more detail in the medicine’s assessment reports. 

For the full list of side effects and restrictions with Sotyktu, see the package leaflet.

The most common side effect with Sotyktu (which may affect more than 1 in 10 people) is upper respiratory infection (nose and throat infection). 

Patients who have an important or long-term infection, or an infection that keeps coming back, must not take this medicine.

Sotyktu was shown to be effective at reducing symptoms of moderate to severe plaque psoriasis. Sotyktu provides an additional treatment option for patients with plaque psoriasis who have not yet been treated with systemic therapy and those who do not benefit from other systemic therapies. Sotyktu was also shown to be effective at treating psoriatic arthritis in adults who could not take, or whose condition had not improved enough with a prior DMARD. 

Side effects are mild to moderate and manageable.

Therefore, the European Medicines Agency decided that Sotyktu’s benefits are greater than its risks and it can be authorised for use in the EU. 

Recommendations and precautions to be followed by healthcare professionals and patients for the safe and effective use of Sotyktu have been included in the summary of product characteristics and the package leaflet.

As for all medicines, data on the use of Sotyktu are continuously monitored. Suspected side effects reported with Sotyktu are carefully evaluated and any necessary action taken to protect patients.