Ascorbic acid (AA) is an important water soluble antioxidant. It's been previously repotted that AA has preventive effects on the development of cancer and atherosclerosis. However, the anti-cancer mechanism and clinical therapeutic effect of AA remain unclear. Previously, consideration was given to the ability of AA to inhibit cancer metastasis by increasing collagen synthesis and inhibiting the activity of hyaluronidase front cancer cells. Recently, high concentration of AA was found to have direct inhibitory activities on the proliferation of cancer cells. The mechanism involved was thought to be due to the induction of apoptosis by hydrogen peroxide generated during the reductive process of DHA, an oxidized AA, which was taken up into cancer cells through glucose transporter. Cancer cells have larger numbers of glucose transporters but far less amounts of catalase to scavenge hydrogen peroxide than normal cells. Therefore, cancer cells are more susceptible to damage by AA than normal cells. Some clinical studies suggested that, high dose of AA (greater than 10 g per day) may prolong the survival of some terminal cancer patients while diminishing the tumor size in some cancer patients completely or partially, However, other studies reported no benefit of AA for cancer patients from taking high dose of AA (10g per day) The difference between these studies may be from the route of AA administration. The former studies used the intravenous route in combination with oral intake. In contrast, the latter studies used the oral intake only. Previous pharmacokinetic studies had shown that the effect cytotoxic serum concentration of AA could only be achieved though intravenous injection but not by oral intake. Despite the lack of large randomized controlled clinical trials with data for establishing the role of vitamin C in cancer therapy, the clinical activity of intravenous AA in cancer patient deserves further investigation.