Effect of Tirzepatide on Cardiovascular and Metabolic Parameters in Obese Adult Patients With Congenital Heart Disease (TEACH)

Introduction Obesity is a complex multifactorial disease with major impact on the cardiovascular system and subsequent adverse cardiovascular events.

Congenital heart disease (CHD) is the most common congenital disease. With the advancement of the treatment nowadays around 90% of patients with mild, 75% with moderate, and 40% with complex congenital heart disease reach the age of 60 years. With aging, acquired heart disease is becoming more prevalent and poses a growing concern in adults with CHD (ACHD). The ACHD patients are at an increased risk for atherosclerotic cardiovascular disease and its risk factors. In comparison to the general population, patients with ACHD have more severe risk factors for atherosclerosis, which frequently clinically presents at an earlier age and has increased morbidity and mortality.

Among well known risk factors for atherosclerotic cardiovascular disease, obesity plays an important role. It is estimated that, similarly to general population, up to 40-50% of ACHD patients are overweight or obese. These patients are at an increased risk for arterial hypertension, hyperlipidaemia, and diabetes. The development of obesity in ACHD is multifactorial, potentially including inadequate education on healthy lifestyle, sedentary lifestyle, and overfeeding during infancy.

CHD is a long-life disease, requiring frequent interventions throughout life, among them also surgical and catheter interventions. Obesity poses a risk for complications in surgical and catheter interventions, which increase morbidity and mortality in these patients.

Novel pharmacological treatment of obesity is an emerging help in reducing not only weight in obese patients but also contributing to diminishing obesity-related adverse effects.

Tirzepatide (Mounjaro), a drug developed for the treatment of type 2 diabetes, is a dual glucose-dependent insulinotropic polypeptide and glucagon-like peptide-1 that has been recently approved also for the treatment of obesity. Studies have shown that treatment with tirzepatide significantly reduces blood pressure, LDL cholesterol, and triglycerides, all of them established cardiovascular risk factors. There is a large-scale ongoing study, assessing the impact of tirzepatide on major adverse cardiovascular events, such as myocardial infarction and stroke in patients with type 2 diabetes and cardiovascular disease. A recent study has shown that tirzepatide led to a lower risk of a composite of death from cardiovascular causes or worsening heart failure than placebo and improved health status in patients with heart failure with preserved ejection fraction and obesity.

Today, there are no studies on novel antiobesity drugs in patients with ACHD. Therefore, the investigators aim to study the effects of tirzepatide on cardiovascular and metabolic factors in obese patients with ACHD.

Aim of the study The investigators aim to determine the effects of the treatment with tirzepatide on obese patients with ACHD. The investigators will focus on several cardiovascular parameters, such as echocardiographic function of the left ventricle, exercise capacity parameters on exercise testing, blood pressure changes, changes in the arterial stiffness, and endothelial function. Metabolic parameters, encompassing weight change, blood sugar and lipid status, inflammation parameters, and hormones, will be assessed. The investigators expect that 24-week treatment with tirzepatide will result in the improvement of cardiovascular and metabolic parameters.

Study design The investigators designed a 24-week, randomized, open-label, placebo-controlled clinical trial to compare the effects of tirzepatide versus placebo in patients with ACHD diagnosed with obesity. Patients will be randomized in a 1:1 ratio to either the intervention or placebo group.

Study population and eligibility criteria The investigators will enroll approximately 30-40 participants with ACHD who meet the established criteria for pharmacological intervention in obesity, as outlined in current international guidelines. The cohort inclusion criteria will be limited to a body mass index (BMI) between 30 and 40 kg/m². To mitigate potential confounding variables, the study will exclude participants with secondary causes of obesity, such as thyroid disorders, autonomous glucocorticoid activity, or syndromic conditions. Additionally, any evident syndromic forms of obesity will be ruled out through clinical examination during the endocrinological assessment.

Patients with ACHD are followed in the tertiary national centre for ACHD at the Department of Cardiology, University Medical Centre Ljubljana. The patients will be enrolled during their regular follow-up at the outpatient clinic for ACHD. All potentially eligible patients will receive written and oral information about the study including the potential adverse effects of the treatment, the procedures conducted, the reporting of these effects, and the recommended measures upon their occurrence. A screening examination will be performed after the patient has agreed to participate and has signed the informed consent form. At the time of screening, the patients will undergo examinations to ensure that all inclusion criteria and none of the exclusion criteria are met. All patients who meet the inclusion and exclusion criteria at screening will be enrolled for randomization followed by a 24-week study period.

Intervention Tirzepatide (Mounjaro, Eli Lilly) will be administered as a subcutaneous injection using prefilled pens, following a modified titration protocol. Participants in the intervention group will begin with a 2.5 mg weekly dose for 4 weeks, followed by potential increases of 2.5 mg every 4 weeks, based on clinical response and tolerability of adverse effects, up to a maximum dose of 15 mg. Participants in the placebo group will receive 0.9% saline via identical pens. At the study's outset, participants will receive education on self-administration and perform their first injection under supervision in-clinic. Thereafter, participants will self-administer the treatment at home, attending monthly clinic visits for monitoring and dose adjustments.

Treatment allocation After the screening phase, participants will be randomized after the test day to one of the two study groups in a 1:1 ratio in accordance with a subject randomization list.

Trial visits and examinations The study will include two main sets of visits: an initial set before the start of treatment (V1) and a follow-up set after 24 weeks of treatment (V6). Throughout the treatment period, independent of the two main sets of visits (V1 and V6), participants will undergo monthly laboratory tests to monitor an extended panel of electrolytes, liver and kidney function tests to ensure safety (V2-5).

Visit 1 and 6 will include:

• Clinical examination
• Quality of life assessment, HADS, IPAQ, DEBQ, OP, FFQ and TFEQ-R18 questionnaire
• Heart rate and heart rate variability measurement
• Measurement of body composition, bone mineral density, and muscle strength
• Continuous glucose monitoring
• Basic and extended laboratory investigations
• Echocardiography
• Cardiopulmonary exercise testing
• Endothelial function and arterial stiffness measurement

Visit 2-5 will include:

• Clinical examination
• Basic laboratory investigations