Author: van Benten, I.J.; van Drunen, C.M.; Koevoet, J.L.M.; Koopman, L.P.; Hop, W.C.J.; Osterhaus, A.D.M.E.; Neijens, H.J.; Fokkens, W.J.
Title: Reduced nasal ILâ€10 and enhanced TNFα responses during rhinovirus and RSVâ€induced upper respiratory tract infection in atopic and nonâ€atopic infants Cord-id: 3nb0ol6s Document date: 2004_12_15
ID: 3nb0ol6s
Snippet: Rhinovirus and respiratory syncytial virus (RSV) are the most prevalent inducers of upper respiratory tract infections (URTI) in infants and may stimulate immune maturation. To estimate the amount of immune stimulation, nasal immune responses were examined during rhinovirus and RSVâ€induced URTI in infants. Nasal brush samples were taken from infants (2–26 months; 57% atopic family) with rhinovirusâ€induced URTI (N = 20), with RSVâ€induced URTI (N = 7), and with rhinovirusâ€induced rhiniti
Document: Rhinovirus and respiratory syncytial virus (RSV) are the most prevalent inducers of upper respiratory tract infections (URTI) in infants and may stimulate immune maturation. To estimate the amount of immune stimulation, nasal immune responses were examined during rhinovirus and RSVâ€induced URTI in infants. Nasal brush samples were taken from infants (2–26 months; 57% atopic family) with rhinovirusâ€induced URTI (N = 20), with RSVâ€induced URTI (N = 7), and with rhinovirusâ€induced rhinitis (N = 11), from children with asymptomatic rhinovirus infection (N = 7) and from eight nonâ€infected children. Numbers of nasal brush cells positive for Th1â€, Th2â€, regulatory and proinflammatory cytokines were measured by immunohistochemistry or by measuring protein levels using a cytometric bead array analysis. During rhinovirus and RSVâ€induced URTI, fewer regulatory cytokine ILâ€10 positive cells were found compared to nonâ€infected children. This fall was accompanied by an increase in levels of the Th1 cytokine TNFα. ILâ€10 responses were inversely related to TNFα responses. No enhanced responses were observed for IFNγ, ILâ€12 and ILâ€18. Cytokine responses were comparable in children with rhinovirusâ€induced URTI and in children with rhinitis, while responses in asymptomatic rhinovirusâ€infected children were located between those for symptomatic and asymptomatic rhinovirusâ€infected children. Cytokine responses did not depend on the age of the child or atopy in the family. In conclusion, reduced nasal ILâ€10 responses during URTI in infants could facilitate the induction of a TNFα response. TNFα in turn could replace the immature production of ILâ€12, ILâ€18 and IFNγ during URTI to induce an effective clearance of the viral infection and which could stimulate the maturation of Th1 cytokine production in infancy. J. Med. Virol. 75:348–357, 2005. © 2004 Wileyâ€Liss, Inc.
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