Journal of Endodontics
Volume 34, Issue 1 , Pages 7-10, January 2008

Quantification of Neural Protein in Extirpated Tooth Pulp

  • Curt A. Warren, DDS

      Affiliations

    • Department of Endodontics, University of Maryland Dental School, Baltimore, Maryland
  • ,
  • LeePeng Mok, MS

      Affiliations

    • Department of Biomedical Sciences, University of Maryland Dental School, Baltimore, Maryland
  • ,
  • Sharon Gordon, DDS, MPH, PhD

      Affiliations

    • Department of Biomedical Sciences, University of Maryland Dental School, Baltimore, Maryland
  • ,
  • Ashraf F. Fouad, DDS, MS

      Affiliations

    • Department of Endodontics, University of Maryland Dental School, Baltimore, Maryland
  • ,
  • Michael S. Gold, PhD

      Affiliations

    • Department of Medicine, University of Pittsburgh, Pittsburgh, PA.
    • Corresponding Author InformationAddress requests for reprints to Michael S. Gold, PhD, Department of Medicine, University of Pittsburgh, 3500 Terrace St, Room E1440 BST, Pittsburgh, PA 15213.

published online 23 November 2007.

Abstract 

Because the pulp tissue extirpated during root canal procedures might serve as a valuable resource with which to assess underlying mechanisms of persistent pain, we sought to determine whether standard Western blotting techniques could be used to quantify neural proteins in pulp extirpated from teeth with irreversible pulpitis. Pulp harvested from healthy intact teeth extracted for orthodontic reasons was used for comparison. The neural marker PGP9.5 was detectable in all samples tested. A membrane enrichment protocol enabled detection of even low abundance, high molecular weight proteins such as the sodium channel α-subunit NaV1.8. Importantly, it was possible to quantify a ∼6-fold increase in the relative density of NaV1.8 in inflamed pulp compared with control pulp. Our results suggest that it should be possible to use extirpated tooth pulp to validate mechanisms of persistent pain implicated in preclinical studies as well as evaluate the therapeutic efficacy of novel antinociceptive interventions.

Key Words: NaV1.8, nociceptor, pain, primary afferent

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PII: S0099-2399(07)00897-7

doi:10.1016/j.joen.2007.09.014

Journal of Endodontics
Volume 34, Issue 1 , Pages 7-10, January 2008