Figure 7
Figure 7. Delayed HS administration facilitates the removal of tissue-associated CXC chemokines and resolution of neutrophilic inflammation. (A) Sdc1−/− mice were injected intraperitoneally with or without 50 μg HS/mouse at 10 hours after LPS, and tissue samples were analyzed at 40 hours after LPS. Tissues levels of KC and MIP-2 were determined by ELISA (n = 5). (B) Neutrophil accumulation was assessed by immunostaining with anti-GR1 and Alexa 594 anti–rat antibodies (original magnification, ×200). Error bars indicate SE.

Delayed HS administration facilitates the removal of tissue-associated CXC chemokines and resolution of neutrophilic inflammation. (A) Sdc1−/− mice were injected intraperitoneally with or without 50 μg HS/mouse at 10 hours after LPS, and tissue samples were analyzed at 40 hours after LPS. Tissues levels of KC and MIP-2 were determined by ELISA (n = 5). (B) Neutrophil accumulation was assessed by immunostaining with anti-GR1 and Alexa 594 anti–rat antibodies (original magnification, ×200). Error bars indicate SE.

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