Hypotheses

We hypothesise that physiological data captured through a wearable device will accurately and objectively (a) reflect illness activity during acute affective episodes in bipolar disorder, (b) differentiate between different acute affective episodes and (c) predict treatment response.

Objectives

The primary objective of the study is to identify digital signatures of illness activity in bipolar disorder at the intra- (acute, response, remission) and between-individual (manic, depressed, euthymic, healthy controls) levels, and identify digital signatures of treatment response.

The secondary objectives are to (a) correlate physiological data to specific affective symptoms; (b) identify which digital biomarkers are most relevant for the former models; (c) assess generalisation across patients, to evaluate the role of the severity of symptoms, circadian rhythms and confounders in the identification of illness activity and treatment response; and (d) assess clustering among participants.

Inclusion criteria

The inclusion criteria for group A are as follows: (a) age 18–75 years; (b) current acute manic episode (A1), major depressive episode (A2) or mixed features manic episode (A3) in the context of bipolar disorder (for groups A1, A2 and A3) and major depressive disorder (MDD) (for 12 patients from group A2), according to the DSM-5 criteria²⁴ and confirmed by a semi-structured interview using the Structured Clinical Interview for DSM-5, Research Version (SCID-5-RV)^{Reference First, Williams, Karg and Spitzer25}; (c) requiring admission to the acute in-patient or home hospitalisation units; and (d) willing and able to give consent (reconfirmed on clinical remission).

Current acute DSM-5 affective episodes will be measured at time point 0. Symptom response will be measured at time point 1, defined as a 30% improvement in the Young Mania Rating Scale (YMRS)^{Reference Young, Biggs, Ziegler and Meyer26} score or 17-item Hamilton Depression Rating Scale (HDRS)^{Reference Hamilton27} score. Time point 2 will measure symptomatic remission, defined as a YMRS or HDRS score ≤7. Time point 3 will assess remission, defined as ≥8 weeks of sustained remission. If patients do not show clinical improvement (i.e. 30% improvement in clinical scores after time point 0), such as treatment-resistant patients, they will only be recorded at time point 0 (acute phase). Likewise, patients attaining clinical remission (i.e. YMRS or HDRS ≤7) rapidly (e.g. in <1 week), will skip the time point 1 recording and will be recorded at time point 0 (acute) and time point 2 (remission phase). Patients in acute phases will be assessed by the research team on a weekly basis to assess psychopathological changes corresponding to response or remission.

The inclusion criteria for group B are as follows: (a) age 18–75 years; (b) patients with a current diagnosis of bipolar disorder (n = 12) or MDD (n = 12), according to DSM-5 criteria and confirmed with a semi-structured interview (SCID-5-RV); (c) sustained YMRS and HDRS scores of ≤7 for at least 8 weeks; and (d) willing and able to give consent.

The inclusion criteria for group C are as follows: (a) age 18–75 years; (b) no current or previous psychiatric disorder, according to the DSM-5 criteria and confirmed with a semi-structured interview (SCID-5-RV), excluding nicotine substance use disorder; and (c) willing and able to give consent.

Exclusion criteria for all groups

The exclusion criteria for all groups are as follows: (a) presence of severe cardiovascular or neurological medical conditions that may lead to autonomic dysfunction, ongoing cardiovascular arrhythmia or pacemaker use; (b) current comorbid substance use disorder as per DSM-5 criteria, excluding nicotine substance use disorder; (c) current comorbid psychiatric disorder causing significant interference with symptoms; (d) current pharmacological treatment involving beta-blockers or other medications affecting the autonomic nervous system; and (e) ongoing pregnancy.

Sample size

Determining the required number of participants is contingent on the primary end-point, which is the identification of digital signatures indicating illness activity in bipolar disorder. There is a lack of precedent and similar studies reporting α-error, 1–β error and a mean/s.d. ratio assessing severity in bipolar disorder from digital biomarkers to calculate the sample size. Given the exploratory nature of this study because of the totally novel measuring methods employed, we adopted a conservative pragmatic approach to estimate the sample size with balanced and practical feasible groups, as recommended in pilot studies.^{Reference Moore, Carter, Nietert and Stewart28} Indeed, previous works using wearable physiological data to identify digital signatures of illness activity in bipolar disorder find significant differences with samples smaller than 20 per group.^{Reference Jakobsen, Stautland, Riegler, Côté-Allard, Sepasdar and Nordgreen29,Reference Krane-Gartiser, Henriksen, Morken, Vaaler and Fasmer30} Our approach seeks to maximise the sample size according to our recruitment capacities for the period of the study and the availability of patients with acute affective episodes at our centre. Thus, taking into account the multiple and continuous data points for each individual during the study period provided by the wearable devices, we have determined that a minimum of 12 patients each for acute affective episode (manic, depressive and mixed), 12 euthymic patients and 12 healthy controls will be necessary to establish composite models to identify illness activity patterns. Twenty-four patients with MDD (12 acute and 12 euthymic) will be added to compare with bipolar depression and euthymia. Of note, from a total of 84 participants, 48 will be recorded longitudinally at different time points, according to the resolution of an acute episode. Therefore, although the sample size is limited, it will have the strength of being prospective and allowing for intra-individual comparisons. The sample size determined for the initial phase of the study could pose a challenge for machine learning because of the constraints on sample sizes for both training and testing data-sets. Consequently, the findings from our analyses will be validated using larger sample sizes in subsequent phases of the study.

Sociodemographic and clinical assessment

At baseline (time point 0), the following sociodemographic and clinical data will be gathered: age, gender, psychiatric diagnoses according to DSM-5 criteria, medical and psychiatric comorbidities, duration of illness, frequency of past manic and depressive episodes, longitudinal course specifiers (such as predominant polarity, seasonality and rapid cycling), history of mental illness among first-degree relatives and prior substance misuse patterns.

Symptoms, severity and functional assessment

Psychopathological assessments will be conducted with the YMRS for manic symptoms, the 17-item HDRS for depressive symptoms and the Positive and Negative Syndrome Scale (PANSS)^{Reference Hamilton27} for psychotic symptoms. Disease severity will be assessed with the Clinical Global Impression Scale: Severity of Illness (CGI-S)^{Reference Guy31}, with higher scores indicating greater severity. The Social and Occupational Functioning Assessment Scale (SOFAS)^{Reference Goldman, Skodol and Lave32} will be administered for functional evaluation without the influence of symptom severity. It employs a numerical scale ranging from 1 to 100, where higher scores signify improved functionality. Moreover, the Stroop Color Word Test (CWT)^{Reference Stroop33} will be performed as a stress-elicitation task for the study of autonomic nervous system alterations in mood episodes, on the basis of psychological, physiological and biochemical responses. Clinical assessments will be performed cross-sectionally for groups B and C and at different time points (time point 0: acute, time point 1: response, time point 2: remission, time point 3: recovery) for group A (Fig. 1).

Physical activity assessment

Physical activity will be evaluated using the Short Scale International Physical Activity Questionnaire (IPAQ), which assesses various types of activity such as walking, moderate-intensity activities and vigorous-intensity activities. The assessment includes collecting data on the frequency (measured in days per week) and duration (time per day) of each specific type of activity. The continuous score IPAQ results will be expressed in metabolic equivalent of task per min (MET-min) per week. This score is calculated by multiplying the MET assigned to each activity (8 MET-min for vigorous, 4 MET-min for moderate and 3.3 MET-min for walking) by the number of days it was performed during a week. MET-min corresponds to oxygen consumption during rest, and is equivalent to 3.5 ml of oxygen per kg of body mass per min. Physical activity assessments will be conducted cross-sectionally for groups B and C, and at various time points (time point 0: acute, time point 1: response, time point 2: remission, time point 3: recovery) for group A (Fig. 1). Indeed, objective wearable-collected actigraphy measures will be correlated with subjective physical activity assessments (IPAQ), to validate the objective measurements.

Pharmacological treatments

All pharmacological treatments (both psychopharmacological and others) as described in international treatment guidelines will be included registering their generic name, starting day and dose per day in each of the 48-h registers: cross-sectionally for groups B and C, and at different time points (time point 0: acute, time point 1: response, time point 2: remission, time point 3: recovery) for group A (Fig. 1). Because of the pragmatic design, treatment decisions (including inpatient discharge) will be exclusively determined by the judgement of the clinicians in charge of the case and patients’ agreement resembling routine clinical care. The researchers performing the recruitment of the study will not be involved in any clinical decisions of the patients included.

Other potential confounders

Other potential confounders, such as atmospheric conditions (humidity, temperature), diet (caffeine, water intake) and quantitative tobacco use, will be registered during each recording.