Allergic Contact Dermatitis (ACD) resulting from skin sensitization is a frequent inflammatory skin disease linked to the use of chemicals, called haptens. At this time, the sensitizing potential of a new chemical is evaluated on animal models. However, new European legislation requires alternative methods for skin sensitization. In this context, a better knowledge of ACD and the capacity to reproduce in vitro its mechanisms lead to the development of new alternative methods. The aim of this study performed with human dendritic cells (DCs) and the human cell line U937 was to determine the early events involved in dendritic cell activation induced by contact sensitizers and especially by the mercury compound thimerosal. Data show that oxidative stress induced by sensitizers is an early signaling event leading to DC activation (expression of CD86 and IL-8 release) and to apoptosis. Using antioxidants, our data show that oxidative stress, characterized by ROS production in correlation with the depletion of the mitochondrial membrane potential and of intracellular glutathione, is a key player in signal transduction induced by sensitizers, especially in the response of DCs towards thimerosal and DNCB. More specifically, these studies demonstrate that thiol groups play a direct role in the initiating events leading to DC activation. In addition, calcium influx was detected in DCs exposed to sensitizers, in correlation with oxidative stress. These data highlight the great interest in the development of a hapten-protein binding assay based on thiol groups and the necessity to better understand the redox status of chemicals as well as cell metabolism for predicting skin sensitization.