Lung cancer is one of the tenth leading causes of death in Taiwan. The average survival duration for patients with lung cancer is about 9-12 months and overall 5-year survival rate is about 10%. There are less than 20% lung cancer patients able to undergo curative resection. 80% of lung cancer patients undergo surgery died of metastasis within two years. More effective treatments for this devastating disease are urgently needed. Based on our previous findings, IAA induced cytochrome C release resulting in activation of caspase-3 and nuclear condensation in non-small cell lung cancer (NSCLC). In this study, we investigate possible molecular mechanism(s) of how IAA induced cell death in human lung cancer cell lines. Our results showed that IAA induced dose-dependent cell death as well as inhibited migration in anchorage dependent and anchorage independent assays. These responses could be reversed by dithiothreitol (DTT) or N-acetyl-L cystein (NAC) in most tested lung cancer cell lines, such as A549, H1299, H522, HOP62, H23, EKVX, PC14, H1975, H441 and H460. Though RT-PCR and microarray analysis, Notch-3 can be confirmed as the target of IAA. Pbx-1 is predicted as downstream oncogene of Notch-3. Cells treated with IAA for 16 or 24 hours, RT-PCR assay showed Pbx-1 mRNA suppression. However, this symptom can be reversed by DTT or NAC. As a conclusion, Notch-3 and it’s downstream, Pbx-1, involved in IAA-induced cell death, which suggesting that inactivation of Notch-3 or Pbx-1 may be a potential therapy for lung cancer.