4.6 Article

ASIC3 in muscle mediates mechanical, but not heat, hyperalgesia associated with muscle inflammation

Journal

PAIN
Volume 129, Issue 1-2, Pages 102-112

Publisher

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1016/j.pain.2006.09.038

Keywords

pain; acid; proton; ion; nociceptor; carrageenan

Funding

  1. NIAMS NIH HHS [K02 AR 02201, AR053409, R01 AR053509, R01 AR053509-01A1, K02 AR002201, K02 AR002201-05] Funding Source: Medline
  2. NINDS NIH HHS [R01 NS039734-05, R01 NS039734] Funding Source: Medline

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Peripheral initiators of muscle pain are virtually unknown, but likely key to development of chronic pain after muscle insult. The current study tested the hypothesis that ASIC3 in muscle is necessary for development of cutaneous mechanical, but not heat, hyperalgesia induced by muscle inflammation. Using mechanical and heat stimuli, we assessed behavioral responses in ASIC3-/- and ASIC3+/+ mice after induction of carrageenan muscle inflammation. ASIC3-/- mice did not develop cutaneous mechanical hyperalgesia after muscle inflammation when compared to ASIC3+/+ mice; heat hyperalgesia developed similarly between groups. We then tested if the phenotype could be rescued in ASIC3-/- mice by using a recombinant herpes virus vector to express ASIC3 in skin (where testing occurred) or muscle (where inflammation occurred). Infection of mouse DRG neurons with ASIC3-encoding virus resulted in functional expression of ASICs. Injection of ASIC3-encoding virus into muscle or skin of ASIC3-/- mice resulted in ASIC3 mRNA in DRG and protein expression in DRG and the peripheral injection site. Injection of ASIC3-encoding virus into muscle, but not skin, resulted in development of mechanical hyperalgesia similar to that observed in ASIC3+/+ mice. Thus, ASIC3 in primary afferent fibers innervating muscle is critical to development of hyperalgesia that results from muscle insult. (c) 2006 International Association for the Study of Pain. Published by Elsevier B.V. All rights reserved.

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