Cordyceps militaris;acute toxicity;genotoxicity;micronucleus The Chinese herbal drug DongChongXiaChao. a medicinal and edible mushroom originating from the fungus Cordyceps sinensis (CS), is beneficial to human health in a number of aspects since it possesses anti-diabetic, anti-tumour, immunomodulatory, anti-oxidative and anti-ageing activity. Because CS is so scarce in nature and high in price, a counterfeit and a mimic derived are frequently found in markets. Cordyceps militaris (CM) is another species of Cordyceps spp., which has also been used as a folk medicine in China for a long time and it is a popularly using and cheaper natural of CS. Recently, a huge amount of effort has been devoted to cultivating CM in a controlled environment in order to improve its availability. The purpose of this study was to evaluate whether the cultured fruiting body of CM has acute toxicity and genotoxicity at SD rats and ICR mice. In the acute toxicity, a single maximum dose (2000 mg/kg) of CM were given by oral gavage to SD rats, we had measured the body weights of all animals at the 7th and 14th days. Then we planed to evaluate the genotoxicity of cultured fruiting body of CM by the micronucleus test. The micronucleus test is a convenient, cheap and fast assay to check genotoxicity by counting how many reticulocytes contained micronuclei (MN) in 1000 reticulocytes. Mitomycin C (MMC) is a famous anti-tumor cytotoxic drug, we used it as a positive control to induced MN. We had sampled bone marrow cells of SD rats at the 48 hours after 2000 mg/kg CM treatment, and collected the orbital peripheral blood of ICR mice at the 24, 48 and 72 hours with same treatment. We also evaluated the possible genotoxicity of CM in ICR mice with multiple doses (125~1000 mg/kg) for 7 days. The body weights and MN numbers were not significant difference between the groups of SD rats treated with CM or methylcellulose. Thus, we suggest that CM was no acute toxicity and genotoxicity at SD rats when a single maximum 2000 mg/kg dose was orally administered. The MN numbers were not significant difference between the groups of ICR mice treated with CM or methylcellulose. Thus, the cultured fruit body of CM also did not induce genotoxicity when treatment with a single maximum dose (2000 mg/kg) for 3 days or multiple doses continuous for 7 days in ICR mice.