The fatality rate of lung cancer is the highest among all kinds of cancer in Taiwan. It has been demonstrated that bitter melon (Momordica charantia) extracts (BMEs) can inhibit the proliferation of breast cancer and prostate cancer cell line. We use four different “ethyl acetate-ethyl alcohol (Et-EA)” BMEs to treat human lung carcinoma cell lines CL1-0 and CL1-5 and investigate the effects of BMEs on these cell lines. The four down-streamed Et-EA BMEs used are pure water extract [BME-A], 50% methanol extract [BME-B], 100% acetone extract [BME-C] and acid-hydrolyzed (AH) products of 50% methanol extract [BME-D]. The results revealed that: (1) 500 μg/ml [BME-C] extract and 300 μg/ml [BME-D] can inhibit the proliferation of CL1-0 and CL1-5 cells, and the higher concentration of [BME-C] or [BME-D], the more significant effect in inhibiting CL1 cells proliferation. Other two Et-EA down-streamed BMEs have no effect to CL1 cells in proliferation. (2) 100 μg/ml [BME-C] and [BME-D] can inhibit the migration ability of CL1-0 and CL1-5cells. The higher concentration of 100% acetone extract or [BME-D] exhibits significant effect to inhibit CL1 cells migration. (3) 200 μg/ml [BME-C] and [BME-D] not only inhibit the proliferation of CL1-0 and CL1-5 cells, but also have no effect to cell death. Under 200 μg/ml [BME-C] or [BME-D] treatment, the expression of migration-associated protein, ADAM and CD44, are inhibited.(4) Compare to [BME-C], [BME-D] can exert stronger effect to CL1-0 and CL1-5 cells in proliferation and migration. Taking together, we conclude that BMEs can inhibit the proliferation, migration and invasion of the lung cancer lines CL1-0 and CL1-5. It is suggested that the BMEs can be a potential anti-lung cancer therapeutic drug.