Brain-to-brain mechanisms underlying pain empathy and social modulation of pain in the patient-clinician interaction

一致性 移情 背外侧前额叶皮质 医学 体感系统 心理学 慢性疼痛 社会关系 临床心理学 物理疗法 前额叶皮质 认知 精神科 内科学 社会心理学
作者
Dan‐Mikael Ellingsen,Kylie Isenburg,Chang Jin Jung,Jeungchan Lee,Jessica Gerber,Ishtiaq Mawla,Roberta Sclocco,Arvina Grahl,Alessandra Anzolin,Robert R. Edwards,John M. Kelley,Irving Kirsch,Ted J. Kaptchuk,Vitaly Napadow
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [Proceedings of the National Academy of Sciences]
卷期号:120 (26): e2212910120-e2212910120 被引量:40
标识
DOI:10.1073/pnas.2212910120
摘要

Social interactions such as the patient–clinician encounter can influence pain, but the underlying dynamic interbrain processes are unclear. Here, we investigated the dynamic brain processes supporting social modulation of pain by assessing simultaneous brain activity (fMRI hyperscanning) from chronic pain patients and clinicians during video-based live interaction. Patients received painful and nonpainful pressure stimuli either with a supportive clinician present (Dyadic) or in isolation (Solo). In half of the dyads, clinicians performed a clinical consultation and intake with the patient prior to hyperscanning (Clinical Interaction), which increased self-reported therapeutic alliance. For the other half, patient—clinician hyperscanning was completed without prior clinical interaction (No Interaction). Patients reported lower pain intensity in the Dyadic, relative to the Solo, condition. In Clinical Interaction dyads relative to No Interaction, patients evaluated their clinicians as better able to understand their pain, and clinicians were more accurate when estimating patients’ pain levels. In Clinical Interaction dyads, compared to No Interaction, patients showed stronger activation of the dorsolateral and ventrolateral prefrontal cortex (dlPFC and vlPFC) and primary (S1) and secondary (S2) somatosensory areas (Dyadic–Solo contrast), and clinicians showed increased dynamic dlPFC concordance with patients’ S2 activity during pain. Furthermore, the strength of S2-dlPFC concordance was positively correlated with self-reported therapeutic alliance. These findings support that empathy and supportive care can reduce pain intensity and shed light on the brain processes underpinning social modulation of pain in patient–clinician interactions. Our findings further suggest that clinicians’ dlPFC concordance with patients’ somatosensory processing during pain can be boosted by increasing therapeutic alliance.
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