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Chronic back pain is associated with decreased prefrontal and thalamic gray matter density

Vania Apkarian, A.; Sosa, Yamaya; Sonty, Sreepadma; Levy, Robert M.; Norman Harden, R.; Parrish, Todd B.; Gitelman, Darren R.; Apkarian, A. V.

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  <identifier identifierType="URL"></identifier>
      <creatorName>Vania Apkarian, A.</creatorName>
      <familyName>Vania Apkarian</familyName>
      <creatorName>Sosa, Yamaya</creatorName>
      <creatorName>Sonty, Sreepadma</creatorName>
      <creatorName>Levy, Robert M.</creatorName>
      <givenName>Robert M.</givenName>
      <creatorName>Norman Harden, R.</creatorName>
      <familyName>Norman Harden</familyName>
      <creatorName>Parrish, Todd B.</creatorName>
      <givenName>Todd B.</givenName>
      <creatorName>Gitelman, Darren R.</creatorName>
      <givenName>Darren R.</givenName>
      <creatorName>Apkarian, A. V.</creatorName>
      <givenName>A. V.</givenName>
    <title>Chronic back pain is associated with decreased prefrontal and thalamic gray matter density</title>
    <date dateType="Issued">2004-12-01</date>
  <resourceType resourceTypeGeneral="JournalArticle"/>
    <alternateIdentifier alternateIdentifierType="url"></alternateIdentifier>
    <relatedIdentifier relatedIdentifierType="DOI" relationType="IsIdenticalTo">10.1523/jneurosci.2541-04.2004</relatedIdentifier>
    <rights rightsURI="info:eu-repo/semantics/openAccess">Open Access</rights>
    <description descriptionType="Abstract">The role of the brain in chronic pain conditions remains speculative. We compared brain morphology of 26 chronic back pain (CBP) patients to matched control subjects, using magnetic resonance imaging brain scan data and automated analysis techniques. CBP patients were divided into neuropathic, exhibiting pain because of sciatic nerve damage, and non-neuropathic groups. Pain-related characteristics were correlated to morphometric measures. Neocortical gray matter volume was compared after skull normalization. Patients with CBP showed 5–11% less neocortical gray matter volume than control subjects. The magnitude of this decrease is equivalent to the gray matter volume lost in 10 –20 years of normal aging. The decreased volume was related to pain duration, indicating a 1.3 cm3 loss of gray matter for every year of chronic pain. Regional gray matter density in 17 CBP patients was compared with matched controls
using voxel-based morphometry and nonparametric statistics. Gray matter density was reduced in bilateral dorsolateral prefrontal cortex and rightthalamus and was strongly relatedto pain characteristics in a pattern distinctfor neuropathic and non-neuropathic CBP. Our results imply that CBP is accompanied by brain atrophy and suggest that the pathophysiology of chronic pain includes thalamocortical processes.</description>
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