The standard treatments of breast cancer are operation, local radiotherapy, systemic chemotherapy and hormone therapy. Regarding chemotherapy for metastatic breast cancer, combination chemotherapy is more effective than single agent. However, most or the drugs used for chemotherapy are metabolized by the liver. Therefore, whether the live function is tolerable or not becomes the key point for patients receiving systemic chemotherapy. In this report, we present a case of a 43 year old female patient with metastatic breast cancer. She suffered from intolerable live dysfunction following chemotherapy with intravenous injection of Taxotere and 5FU. Liver function gradually recovered after chemotherapy combined with intravenous injection of glycyrrhiznin (GL) at a dosage of 80 mg/day for 2 days pre-chemotherapy and 80 mg/day post-chemotherapy. Although liver function improved, the regimen of chemotherapy was changed to another regimen with Taxol and Gemzar due to the findings of increased serum tumor marker (CA15-3) and lung metastasis. Following the first injection of Taxol and Gemzar, her liver function once again became abnormal She received intravenous injection of GL again. However, the dosage of GL was changed to 120 mg (IVD) before and immediately after chemotherapy. After the regimen of GL changed, her liver function recovered again and remained normal until the completion of the whole chemotherapy schedule (total of 4 months). During this period, chemotherapy was performed continuously and no significant side-effects appeared. Due to persistent chemotherapy, the tumor marker (CA15-3) decreased gradually, and the metastatic lung tumors, noted by chest CT scan, disappeared completely in Now. 2005. The above results suggest intravenous GL may attenuate or prevent liver dysfunction induced by chemotherapy. It is worthwhile evaluating the preventive and therapeutic effects of intravenous GL on liver dysfunction induced by chemotherapy with a large clinical trial in the future.