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Finding Treatments for Eating Disorders — FED

Anorexia in Adolescence Clinical Trial

Official title:
Finding Treatments for Eating Disorders

Clinical Trial Summary

Currently, Family Based Treatment (FBT) is the leading evidence-based, manualized treatment for adolescents with anorexia nervosa (AN). FBT emphasizes parental involvement in addressing disordered eating by supporting the child in eating and refeeding to achieve a healthy body weight and independent eating. Based on multiple RCTs, 50% of AN patients who receive FBT recover, and those who do not are more likely to develop a chronic illness. Research demonstrates that weight gain of less than 2.3kg (4.8 pounds) by week 4 of FBT predicts that 75% of adolescents with AN will not achieve weight restoration by the end of treatment. FBT works in part by reducing the avoidance of food and increasing the exposure to food triggers, like the treatment of anxiety disorders and obsessive-compulsive disorder (OCD). Thus, researchers postulate that anxiety may be a negative predictor of FBT treatment outcome in the early phase of FBT. In addition, elevated baseline anxiety has been shown to be associated with poorer outcomes at end of treatment and may also impact the likelihood of early response. To improve clinical response, we need to develop viable biological treatment targets (i.e., brain areas implicated in anxiety) that could be combined with FBT. Such targets can be defined by 1) initially targeting brain areas that mediate symptoms hindering treatment response (i.e., anxiety), and 2) looking at changes in brain chemistry and function. Thus, repetitive transcranial magnetic stimulation (rTMS) could be an alternative and promising treatment approach for adolescents with AN who do not respond to Phase 1 of FBT. Using rTMS, we can target the brain areas implicated in anxiety in people with anorexia and modulate that activity to reduce symptoms, and thus, facilitate response to FBT. Several studies have shown the rTMS to the right dorsolateral prefrontal cortex (DLPFC) is effective in reducing anxiety across a range of neuropsychiatric disorders. Therefore, it is possible that stimulating the right DLPFC could facilitate treatment efficacy of FBT in youth with AN. Additional explorations of the connections between, and neurochemistry of, the right DLPFC and those mediating emotion in the brain (e.g., amygdala) could aid in our understanding of the networks impeding effective treatment responses and allow for more tailored, precision targeting with TMS.

Clinical Trial Description

norexia nervosa (AN) is a serious psychiatric illness with the highest mortality rate of any other psychiatric disorder. Medical complications from starvation and malnutrition and suicide are the most common cause of death. AN is characterized by a person's fear of gaining weight, becoming fat, and body dissatisfaction, and it has a lifetime prevalence of 0.6 to 2.0% in females. Currently, Family Based Treatment (FBT) is the leading evidence-based, manualized treatment for adolescents with AN. FBT emphasizes parental involvement in addressing disordered eating by supporting the child in eating and refeeding in order to achieve a healthy body weight and independent eating. FBT has been shown to promote rapid weight gain in AN patients in several randomized control trials and reduced hospitalization in AN patients . Based on multiple RCTs, 50% of AN patients who receive FBT recover, and those who do not are more likely to develop a chronic illness. Research demonstrates that weight gain of less than 2.3kg (4.8 pounds) by week 4 of FBT predicts that 75% of adolescents with AN will not achieve weight restoration by the end of treatment . There continues to be limited empirical research and clinical knowledge about what differentiates those who consistently gain weight and those who do not in the critical window for weight gain in the first month of FBT. FBT works in part by reducing the avoidance of food and increasing the exposure to food triggers, similar to the treatment of anxiety disorders and obsessive-compulsive disorder (OCD). Thus, researchers postulate that anxiety may be a negative predictor of FBT treatment outcome in the early phase of FBT. In addition, elevated baseline anxiety has been shown to be associated with poorer outcomes at end of treatment, and may also impact the likelihood of early response. While FBT is the first-line treatment for adolescents with AN, response is unfortunately not universal. An understanding of the neurobiology of AN could potentially improve treatment development and response. Unfortunately, the neurobiology of AN is poorly understood, and in turn, neuroscientifically-sound treatments are lacking. In order to improve clinical response, we need to develop viable biological treatment targets (i.e. brain areas implicated in anxiety) that could be combined with FBT. Such targets can be defined by 1) initially targeting brain areas that mediate symptoms hindering treatment response (i.e. anxiety), and 2) looking at changes in brain chemistry and function. Thus, repetitive transcranial magnetic stimulation (rTMS) could be an alternative and promising treatment approach for adolescents with AN who do not respond to Phase 1 of FBT. rTMS involves a safe, non-invasive, painless application of a magnetic field over the skull to a target brain area in order to change its activity and function. Using rTMS, we can target the brain areas implicated in anxiety in people with anorexia and modulate that activity to reduce symptoms, and thus, facilitate response to FBT. Several studies have shown the rTMS to the right dorsolateral prefrontal cortex (DLPFC) is effective in reducing anxiety across a range of neuropsychiatric disorders. Furthermore, some studies have shown that rTMS is effective in reducing core symptoms of anorexia in adults, however, this has yet to be explored in adolescents. Therefore, it is possible that stimulating the right DLPFC could facilitate treatment efficacy of FBT in youth with AN. Additional explorations of the connections between, and neurochemistry of, the right DLPFC and those mediating emotion in the brain (e.g. amygdala) could aid in our understanding of the networks impeding effective treatment responses and allow for more tailored, precision targeting with TMS. ;

Study Design

Related Conditions & MeSH terms

Clinical Trial Details
NCT number NCT05249140
Study type Interventional
Source University of Calgary
Contact Frank P MacMaster, PhD
Phone 4039552784
Email fmacmast@ucalgary.ca
Status Not yet recruiting
Phase N/A
Start date December 31, 2022
Completion date May 31, 2025
View Details
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