We conducted a series of toxicity tests and short-term mutagenic assays of Asulam and 40% (W/V) sodium Asulam. It was found that the LD50 of Asulam with acute oral toxicity was 30000 mg/kg for mice, and the LD50 of sodium Asulam for mice and rats were equal (8250 mg/kg). The cumulative coefficient of sodium Asulam in Wistar rats was 9.42. None died from sodium Asulam absorbed via skin. Negative results were obtained in Ames test, Bacillus subtilis repair test and the micronucleus test. There was no significant difference between the control group and the treated groups in the chromosomal aberration rates of spermatogonia and primary spermatocytes of mice testis. The results indicated that Asulam should be regarded as a substance of low toxicity and low accumulation. No mutagenicity was observed in our experiment.