PHYSIOLOGICAL METRICS COLLECTED FROM WEARABLE DEVICES IDENTIFY INFLAMMATORY AND CLINICAL INFLAMMATORY BOWEL DISEASE FLARES

Abstract BACKGROUND Inflammatory bowel disease (IBD) flares are common and unpredictable. Disease monitoring relies on symptom reporting or single timepoint assessments of stool, blood, imaging, or endoscopy—these are inconvenient and invasive and do not always reflect the patient perspective. Advan...

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Veröffentlicht in:Inflammatory bowel diseases 2023-01, Vol.29 (Supplement_1), p.S21-S22
Hauptverfasser: Hirten, Robert, Danieletto, Matteo, Landell, Kyle, Lyu, Jinyan, Whang, Jessica, Zweig, Micol, Helmus, Drew, Rodrigues, Jovita, Bottinger, Erwin, Suarez-Farinas, Mayte, Nadkarni, Girish, Fayad, Zahi, Keefer, Laurie, Sands, Bruce
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Sprache:eng
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Zusammenfassung:Abstract BACKGROUND Inflammatory bowel disease (IBD) flares are common and unpredictable. Disease monitoring relies on symptom reporting or single timepoint assessments of stool, blood, imaging, or endoscopy—these are inconvenient and invasive and do not always reflect the patient perspective. Advances in wearable technology allow for passive, continuous and non-invasive assessment of physiological metrics including heart rate variability (HRV), the measure of small time differences between each heartbeat, a marker of autonomic nervous system function. Our group has previously demonstrated that changes in autonomic function precedes an IBD flare, can predict psychological state transitions and even identify inflammatory events including SARS-CoV-2 infection. To develop algorithms that can predict IBD flares using wearable device signatures, we launched a national wearable device study called The IBD Forecast study. To assess data quality and feasibility, the first 125 Apple Watch users to enroll were evaluated. METHODS The IBD Forecast study is a prospective cohort study enrolling anyone ≥18 years of age in the United States (US) with IBD who is willing to (1) use a commercially available wearable device, (2) download our custom eHive app and (3) answer daily survey questions. HRV metrics (mean of the standard deviations of all the NN intervals [SDNN]) were analyzed using a mixed-effect cosigner model that incorporated body mass index, age, and sex. SDNN is a time domain HRV index that reflects both sympathetic and parasympathetic nervous system activity and is calculated from the variance of intervals between adjacent QRS complexes (the normal-to-normal [NN] intervals). Clinical flare was assessed with daily Patient Reported Outcome (PRO)-2 surveys (flare; PRO-2 Crohn’s disease >7, PRO-2 ulcerative colitis >2). Inflammatory flare was assessed via patient reported C-reactive protein (CRP), with inflammatory flare defined as >5 mg/L. RESULTS The first 125 study participants were enrolled across 29 states in the US (Table 1). Circadian features of changes of HRV were modelled (Figure 1). The mesor, or midline of the circadian pattern of the SDNN was higher in those with clinical flare (mean 44.43; 95% CI 41.25-47.75) compared to those in clinical remission (mean 43.03; 95% CI 39.94-46.22) (p
ISSN:1078-0998
1536-4844
DOI:10.1093/ibd/izac247.041