Abstract

Pain circuitry in the spinal cord develops over a prolonged period of late fetal and early postnatal life and is particularly vulnerable to tissue trauma and inflammation during this time. Over the first few weeks of postnatal life, the central terminals of myelinated primary afferents undergo significant reorganization to generate the stereotypical laminar termination patterns seen in the adult dorsal horn. Recent findings in newborn mice have revealed that tactile afferents generate strikingly adult laminar termination patterns early on and thus undergo little central reorganization postnatally. By contrast, myelinated nociceptors give rise to widespread, inappropriate central projections in early postnatal life and thus the characteristic adult termination patterns of these afferents appear to mature later. Due to the relative immaturity of myelinated nociceptor central projections in newborns, the subsequent postnatal maturation of this group of afferents may be acutely susceptible to early perturbations of the periphery. ? ? The proposed experiments will examine the postnatal time course over which myelinated nociceptors achieve maturity to determine the potential window of this vulnerability. These studies will address the hypothesis that this early central exuberance is normally transient but that early tissue trauma, such as that caused by persistent tissue inflammation, arrests the normal postnatal reorganization of their central anatomy, leading to permanent structural alterations in spinal pain circuitry. An isolated somatosensory system preparation developed for comprehensive analyses of individual skin sensory neurons will be used to study the postnatal maturation of myelinated nociceptors in both hairy and glabrous skin of mice. A model of adjuvant-induced inflammation in glabrous skin of newborn mice will be used to examine the effects of early tissue trauma on the anatomical, physiological, and neurochemical maturation of individual neurons. Through intracellular recordings, neurons will be physiologically characterized using a variety of natural skin stimuli and then labeled in their entirety through iontophoresis of Neurobiotin. Their central projections will be reconstructed and analyzed morphometrically for changes taking place throughout postnatal maturation. Somata will be analyzed immunocytochemically to determine neurochemical changes, and peripheral endings will be analyzed for correlated structural changes in both normal and traumatized skin. The results of these studies will provide a detailed understanding of the early maturation of this vital component of the pain system, and the susceptibility of these afferents to early perturbation. This information will be pivotal to the development of future strategies in pediatric pain management and the translation of these strategies into effective practice.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS044094-03
Application #
6803080
Study Section
Integrative, Functional and Cognitive Neuroscience 8 (IFCN)
Program Officer
Porter, Linda L
Project Start
2002-07-05
Project End
2007-06-30
Budget Start
2004-07-01
Budget End
2005-06-30
Support Year
3
Fiscal Year
2004
Total Cost
$175,625
Indirect Cost

  Institution

Name
University of Wyoming
Department
Zoology
Type
Schools of Arts and Sciences
DUNS #
069690956
City
Laramie
State
WY
Country
United States
Zip Code
82071

  Publications

Smith-Edwards, Kristen M; DeBerry, Jennifer J; Saloman, Jami L et al. (2016) Profound alteration in cutaneous primary afferent activity produced by inflammatory mediators. Elife 5:
Bai, Ling; Lehnert, Brendan P; Liu, Junwei et al. (2015) Genetic Identification of an Expansive Mechanoreceptor Sensitive to Skin Stroking. Cell 163:1783-1795
Rutlin, Michael; Ho, Cheng-Ying; Abraira, Victoria E et al. (2014) The cellular and molecular basis of direction selectivity of A?-LTMRs. Cell 159:1640-51
Bardoni, Rita; Tawfik, Vivianne L; Wang, Dong et al. (2014) Delta opioid receptors presynaptically regulate cutaneous mechanosensory neuron input to the spinal cord dorsal horn. Neuron 81:1312-1327
Li, Lishi; Rutlin, Michael; Abraira, Victoria E et al. (2011) The functional organization of cutaneous low-threshold mechanosensory neurons. Cell 147:1615-27
Ye, Yi; Woodbury, C Jeffery (2010) Early postnatal loss of heat sensitivity among cutaneous myelinated nociceptors in Swiss-Webster mice. J Neurophysiol 103:1385-96
Seal, Rebecca P; Wang, Xidao; Guan, Yun et al. (2009) Injury-induced mechanical hypersensitivity requires C-low threshold mechanoreceptors. Nature 462:651-5
Boada, M Danilo; Woodbury, C Jeffery (2008) Myelinated skin sensory neurons project extensively throughout adult mouse substantia gelatinosa. J Neurosci 28:2006-14
Lawson, Jeffrey J; McIlwrath, Sabrina L; Woodbury, C Jeffery et al. (2008) TRPV1 unlike TRPV2 is restricted to a subset of mechanically insensitive cutaneous nociceptors responding to heat. J Pain 9:298-308
Woodbury, C Jeffery; Kullmann, Florenta A; McIlwrath, Sabrina L et al. (2008) Identity of myelinated cutaneous sensory neurons projecting to nocireceptive laminae following nerve injury in adult mice. J Comp Neurol 508:500-9

Showing the most recent 10 out of 14 publications