Role of CD38 in TNF-{alpha}-induced airway hyperresponsiveness

doi:10.1152/ajplung.00367.2007

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Am J Physiol Lung Cell Mol Physiol 294: L290-L299, 2008. First published November 30, 2007; doi:10.1152/ajplung.00367.2007
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Role of CD38 in TNF- ${alpha}$ -induced airway hyperresponsiveness

Alonso G. P. Guedes,¹ Joseph A. Jude,² Jaime Paulin,³ Hirohito Kita,⁴ Frances E. Lund,⁵ and Mathur S. Kannan²^,6

Departments of ¹Veterinary Small Animal Clinical Sciences, Texas A&M University, College Station, Texas; ²Veterinary and Biomedical Sciences, ³Veterinary Population Medicine, and ⁶Pediatrics, University of Minnesota, St. Paul, Minnesota; ⁴Department of Medicine and Immunology, Mayo Clinic, Rochester, Minnesota; and ⁵Trudeau Institute, Saranac Lake, New York

Submitted 6 September 2007 ; accepted in final form 26 November 2007

CD38 is involved in normal airway function, IL-13-induced airwayhyperresponsiveness (AHR), and is also regulated by tumor necrosisfactor (TNF)- ${alpha}$ in airway smooth muscle (ASM) cells. This studyaimed to determine whether TNF- ${alpha}$ -induced CD38 upregulation inASM cells contributes to AHR, a hallmark of asthma. We hypothesizedthat AHR would be attenuated in TNF- ${alpha}$ -exposed CD38-deficient(CD38KO) mice compared with wild-type (WT) controls. Mice (n= 6–8/group) were intranasally challenged with vehiclecontrol or TNF- ${alpha}$ (50 ng) once and every other day during 1 or4 wk. Lung inflammation and AHR, measured by changes in lungresistance after inhaled methacholine, were assessed 24 h followingthe last challenge. Tracheal rings were incubated with TNF- ${alpha}$ (50 ng/ml) to assess contractile changes in the ASM. While asingle TNF- ${alpha}$ challenge caused no airway inflammation, both multiple-challengeprotocols induced equally significant inflammation in CD38KOand WT mice. A single intranasal TNF- ${alpha}$ challenge induced AHRin the WT but not in the CD38KO mice, whereas both mice developedAHR after 1 wk of challenges. The AHR was suppressed by extendingthe challenges for 4 wk in both mice, although to a larger magnitudein the WT than in the CD38KO mice. TNF- ${alpha}$ increased ASM contractileproperties in tracheal rings from WT but not from CD38KO mice.In conclusion, CD38 contributes to TNF- ${alpha}$ -induced AHR after abrief airway exposure to the cytokine, likely by mediating changesin ASM contractile responses, and is associated with greaterAHR remission following chronic airway exposure to TNF- ${alpha}$ . Themechanisms involved in this remission remain to be determined.

tumor necrosis factor- ${alpha}$

Address for reprint requests and other correspondence: M. S. Kannan, Dept. of Veterinary and Biomedical Sciences, College of Veterinary Medicine, Univ. of Minnesota, 1971 Commonwealth Ave., St. Paul, MN 55108 (e-mail: kanna001{at}umn.edu)

Role of CD38 in TNF--induced airway hyperresponsiveness

Role of CD38 in TNF- ${alpha}$ -induced airway hyperresponsiveness