To observe the effects of mPEG5000-KILDVA on the antigen-induced airway inflammation andthe expression of CC cheomokine Eotax in in mice asthma models.Approach the mechanisms of mPEG5000-KILDVA on ant-iasthma.The mice asthma models were established with ovalbumin (OVA),to observe thechange of behavior in mice,prepared serum of mice and collected cbronchoalveolar lavage (BAL) to performcouns of Leukocyte and EOS.The levels of Eotaxin in serum and BALF were measured by ELISA. The expressionof Eotaxin in lung tissue were detected by immunohisto chemistry.The Eotat in levels of serum and BALF inmodel group were significantly higher than that in normal control group with significant difference (p<0.01),mPEG5000-KILDVA group is significantly lower than that in the model group with significant difference (p<0.05),mPEG5000-KILDVA group and dexamethasone g roup are similar with no sig nificant difference (p>0.05).The Eotax in protein expression unit(PU) is significantly higher in the model group than that in the normalcontrol group with significant difference (p<0.05),mPEG5000-K ILDVA group and dexamethasone groupare similar with no significan (p>0.01).Total cell counts,the absolute number of Leukocyte and EOS in BALFin model group significantly increased compared with normal control group with significantly difference (p<0.01), mPEG5000-KILDVA group is significantly lower than that in the model group with significant difference(p<0.05),mPEG5000-KILDVA group and dexamethasone group are similar with no significant difference(p>0.05).mPEG5000-KILDVA can reduce airway inflammation and inhibit Eotax in excessive expression ofasthmatic mouse.