Primary dysmenorrhea is highly prevalent in the world, and is related to elevated prostaglandin F2α (PGF2α) levels. Non-steroidal anti-inflammatory drugs (NSAIDs) can provide effective pain relief. Since many severe side effects may occur after long-term use of NSAIDs, Chinese medicinal therapy has been considered as a feasible alternative medicine. Adlay (Coix lacryma-jobi L. var. ma-yuen Stapf.) has long been used in traditional Chinese medicine. Nevertheless, some medical reports have suggested the use of adlay with caution while pregnancy. Published studies have demonstrated that dehulled adlay water extracts (DAW) enhanced uterine contractions. On the other hand, adlay hull methanolic extracts (AHM) and adlay testa ethanolic extracts (ATE) showed inhibitory effects on uterine contractions. In summary, different parts of adlay seeds and different extractions gave various effects because of various active compounds. Therefore, the aims of the study are (1) to investigate the effects and mechanisms of the adlay ethanolic extracts on PGF2α-induced uterine contractions in the rats and human in vitro; (2) to understand the possible active compounds for regulating the uterine contractions; (3) to confirm effects of the adlay ethanolic extracts on oxytocin-induced dysmenorrheal model and acetic acid writhing test in mice in vivo. The present results demonstrated that (1) AHE-EA and ATE-EA have inhibitory effects on PGF2α-induced uterine contractions in the rats and human by blocking external calcium influx, and AHE-EA and ATE-EA are potent for preventing uterine overcontractions; (2) 3,5,7,4’-tetramethoxyflavone, nobiletin, tangeretin, naringenin, linoleic acid inhibit PGF2α-induced uterine contractions, while stigmasterol stimulates spontaneous uterine contractions in the rats; (3) AHE-EA and ATE-EA could remarkably reduce the writhing times and prolong the latent period in oxytocin-induced dysmenorrheal model, and furthermore ATE-EA are pain relieving in acetic acid writhing test. In conclusion, AHE and ATE have the potential for regulating the dysmenorrheal models in vitro and in vivo.