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Digital Phenotyping of emotion (dys-)regulation as transdiagnostic process and proxy for clinical and neurobiological markers of treatment (non-)response

Subject Area Personality Psychology, Clinical and Medical Psychology, Methodology
Biological Psychology and Cognitive Neuroscience
Term since 2022
Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 442075332
 
Predictors of treatment non-response (NR) that focus on emotion regulation (ER) should be ecologically valid, readily available at low-cost. Such predictors enable treatment-informing single case-predictions. Collecting neural and psycho-physiological predictors of NR in a laboratory context is time-consuming and difficult to implement outside of the university context. Clinical practice needs proxies that transfer the predictive value of neural NR-signatures and related ER-(dys-)functions of internalizing disorders into clinical settings and can be assessed repeatedly with minimal effort for therapists and patients during different treatment periods (e.g., before, during, and after therapy). Embedded within the Research Unit, the present project uses digital phenotyping to derive such proxies. We use data actively and passively collected by personal electronic devices such as smartphones and wearables, to derive phenotypes of individuals at risk of NR based on indicators of ER as the overarching core construct. Smartphones are particularly well-suited for this purpose. First, smartphones allow assessing mood and cognition actively and ecologically valid by means of Ecological Momentary Assessment (EMA, i.e., repeated short surveys of the current state of mind and activities). Second, the sensor-rich environment of smartphones provides multimodal objective data about behavior, physiology, and mood collected passively through built-in applications and connected smart devices (e.g., wearables). The present project (SP6) collects, prior to a CBT treatment, sensor- and EMA data focusing on ER in n = 468 patients with mental disorders from the internalizing spectrum (e.g., patients suffering from specific phobia, social anxiety disorder, panic disorder, agoraphobia, generalized anxiety disorder, obsessive-compulsive disorder, post-traumatic stress disorder, unipolar depressive disorders). Furthermore, we collect sensor and EMA data (2 additional measurement bursts at T20, and post/12-months) throughout the entire treatment in a subsample of n = 350. The sensor-based assessment on mobile devices focusses on markers that are either (A) regulatory (e.g., physical activity, smartphone usage), (B) affect the individual's ability to regulate emotions (e.g., sleep, heart rate variability), or (C) serve as proxies for regulatory efforts or environmental characteristics that influence ER (e.g., GPS tracked spatial resolution of activity patterns, physical activity, and smartphone use). ER indicators are calculated based on (A) the dynamics of self-reported emotional experiences and/or (B) patterns in the self-reported application of ER strategies. Combined with the data modalities of the remaining SPs, this SP provides a unique opportunity to establish a comprehensive cross-level understanding of ER and its value for NR prediction in naturalistic settings.
DFG Programme Research Units
 
 

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