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Sustained perturbation in functional connectivity induced by cold pain

Elena Makovac, Ottavia Dipasquale, Jade B Jackson, Sonia Medina, Owen O’Daly, Jonathan O’Muircheartaigh, Alfonso de Lara Rubio, Steven CR Williams, Stephen B McMahon, Matthew A Howard
doi: https://doi.org/10.1101/633263
Elena Makovac
1Department of Neuroimaging, King’s College London, UK
2Wolfson Centre for Age Related Diseases, King’s College London, UK
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  • For correspondence: elena.makovac@kcl.ac.uk
Ottavia Dipasquale
1Department of Neuroimaging, King’s College London, UK
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Jade B Jackson
1Department of Neuroimaging, King’s College London, UK
2Wolfson Centre for Age Related Diseases, King’s College London, UK
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Sonia Medina
1Department of Neuroimaging, King’s College London, UK
2Wolfson Centre for Age Related Diseases, King’s College London, UK
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Owen O’Daly
1Department of Neuroimaging, King’s College London, UK
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Jonathan O’Muircheartaigh
1Department of Neuroimaging, King’s College London, UK
3Sackler Institute for Translational Neurodevelopment, King’s College London, UK
4Centre for the Developing Brain, King’s College London, UK
5MRC Centre for Neurodevelopmental Disorders, King’s College London, London, UK
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Alfonso de Lara Rubio
1Department of Neuroimaging, King’s College London, UK
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Steven CR Williams
1Department of Neuroimaging, King’s College London, UK
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Stephen B McMahon
2Wolfson Centre for Age Related Diseases, King’s College London, UK
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Matthew A Howard
1Department of Neuroimaging, King’s College London, UK
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Abstract

Functional connectivity (FC) perturbations have been reported in multiple chronic pain phenotypes, but the nature of reported changes is varied and inconsistent between cohorts. Increases and decreases in connectivity strength in task negative and positive networks, for example, the default mode and salience networks (DMN/SN), respectively, have been described, but how other networks are effected, for example, descending pain control networks, remains unknown. Whether connectivity changes relate to peripherally-mediated nociceptive afferent input, represent coping strategies or are sequelae of chronic pain, e.g. anxiety/depression, is also unknown. Here, we examined FC changes in response to experimentally-administered tonic cold pain in healthy volunteers as a means of disambiguating the nature of connectivity changes. We assessed FC prior to, during, and following tonic cold painful stimulation in four seed regions: ventromedial prefrontal cortex (vmPFC), rostral anterior insula (rAI), subgenual anterior cingulate cortex (ACC) and periaqueductal grey (PAG) and recorded subjectively reported pain using a computerised visual analogue scale. We saw DMN FC changes during painful stimulation and that inter-network communication between the rAI and sgACC seeds with the vmPFC became less anti-correlated during pain, whereas PAG-precuneus FC decreased. Pain-induced FC alterations largely persisted during a 6-minute recovery period following cessation of the painful stimulus. Observed FC changes related to the magnitude of individuals’ subjectively reported pain. We provide new insights into FC changes during and following tonic cold-pain and suggest that some FC changes observed in chronic pain patients may relate to the presence of an ongoing afferent peripheral drive.

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The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-ND 4.0 International license.
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Posted May 09, 2019.
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Sustained perturbation in functional connectivity induced by cold pain
Elena Makovac, Ottavia Dipasquale, Jade B Jackson, Sonia Medina, Owen O’Daly, Jonathan O’Muircheartaigh, Alfonso de Lara Rubio, Steven CR Williams, Stephen B McMahon, Matthew A Howard
bioRxiv 633263; doi: https://doi.org/10.1101/633263
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Sustained perturbation in functional connectivity induced by cold pain
Elena Makovac, Ottavia Dipasquale, Jade B Jackson, Sonia Medina, Owen O’Daly, Jonathan O’Muircheartaigh, Alfonso de Lara Rubio, Steven CR Williams, Stephen B McMahon, Matthew A Howard
bioRxiv 633263; doi: https://doi.org/10.1101/633263

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