Targeted disruption of the chemokine eotaxin partially reduces antigen-induced tissue eosinophilia

ME Rothenberg, JA MacLean, E Pearlman… - The Journal of …, 1997 - rupress.org
ME Rothenberg, JA MacLean, E Pearlman, AD Luster, P Leder
The Journal of Experimental Medicine, 1997rupress.org
The chemokines are a large group of chemotactic cytokines that regulate leukocyte
trafficking and have recently been shown to inhibit human immunodeficiency virus entry into
cells. Eotaxin is a C–C chemokine implicated in the recruitment of eosinophils in a variety of
inflammatory disorders and, unlike all other eosinophil chemoattractants, is eosinophil
specific. However, given the large number of chemoattractants that have activities on
eosinophils, it is unclear whether eotaxin has an important role in vivo. Furthermore, it …
The chemokines are a large group of chemotactic cytokines that regulate leukocyte trafficking and have recently been shown to inhibit human immunodeficiency virus entry into cells. Eotaxin is a C–C chemokine implicated in the recruitment of eosinophils in a variety of inflammatory disorders and, unlike all other eosinophil chemoattractants, is eosinophil specific. However, given the large number of chemoattractants that have activities on eosinophils, it is unclear whether eotaxin has an important role in vivo. Furthermore, it remains unclear why there is constitutive expression of eotaxin in healthy states in the absence of eosinophilic inflammation. To begin to determine the significance of eotaxin at baseline and during eosinophil-mediated disease processes, we have used targeted gene disruption to generate mice that are deficient in eotaxin. Such mice demonstrate that eotaxin enhances the magnitude of the early (but not late) eosinophil recruitment after antigen challenge in models of asthma and stromal keratitis. Surprisingly, a role for eotaxin in regulating the constitutive number of eosinophils in the peripheral circulation is also demonstrated. These results indicate a contributory role for eotaxin in the generation of peripheral blood and antigen-induced tissue eosinophilia.
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