The use of electrodermal activity in pulpal diagnosis and dental pain assessment

Aims To explore whether electrodermal activity (EDA) can serve as a complementary tool for pulpal diagnosis (Aim 1) and an objective metric to assess dental pain before and after local anaesthesia (Aim 2). Methodology A total of 53 subjects (189 teeth) and 14 subjects (14 teeth) were recruited for A...

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Veröffentlicht in:International endodontic journal 2023-03, Vol.56 (3), p.356-368
Hauptverfasser: Tran, Hanh T., Kong, Youngsun, Talati, Ankur, Posada‐Quintero, Hugo, Chon, Ki H., Chen, I‐Ping
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Sprache:eng
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Zusammenfassung:Aims To explore whether electrodermal activity (EDA) can serve as a complementary tool for pulpal diagnosis (Aim 1) and an objective metric to assess dental pain before and after local anaesthesia (Aim 2). Methodology A total of 53 subjects (189 teeth) and 14 subjects (14 teeth) were recruited for Aim 1 and Aim 2, respectively. We recorded EDA using commercially available devices, PowerLab and Galvanic Skin Response (GSR) Amplifier, in conjunction with cold and electric pulp testing (EPT). Participants rated their level of sensation on a 0–10 visual analogue scale (VAS) after each test. We recorded EPT‐stimulated EDA activity before and after the administration of local anaesthesia for participants who required root canal treatment (RCT) due to painful pulpitis. The raw data were converted to the time‐varying index of sympathetic activity (TVSymp), a sensitive and specific parameter of EDA. Statistical analysis was performed using Python 3.6 and its Scikit‐post hoc library. Results Electrodermal activity was upregulated by the stimuli of cold and EPT testing in the normal pulp. TVSymp signals were significantly increased in vital pulp compared to necrotic pulp by both cold test and EPT. Teeth that exhibited intensive sensitivity to cold with or without lingering pain had increased peak numbers of TVSymp than teeth with mild sensation to cold. Pre‐ and post‐anaesthesia EDA activity and VAS scores were recorded in patients with painful pulpitis. Post‐anaesthesia EDA signals were significantly lower compared to pre‐anaesthesia levels. Approximately 71% of patients (10 of 14 patients) experienced no pain during treatment and reported VAS score of 0 or 1. The majority of patients (10 of 14) showed a reduction of TVSymp after the administration of anaesthesia. Two of three patients who experienced increased pain during RCT (post‐treatment VAS > pre‐treatment VAS) exhibited increased post‐anaesthesia TVSymp. Conclusions Our data show promising results for using EDA in pulpal diagnosis and for assessing dental pain. Whilst our testing was limited to subjects who had adequate communication skills, our future goal is to be able to use this technology to aid in the endodontic diagnosis of patients who have limited communication ability.
ISSN:0143-2885
1365-2591
DOI:10.1111/iej.13868