Atopic dermatitis (AD) is a common chronic inflammatory skin disease that affects all ethnic groups. Serial studies from both histological and transcriptomic analyses have highlighted the primary pathogenic role of barrier dysfunction and adaptive immune dysregulation in AD, which is centered with aberrant immune activation of type 2 cells that drives overly expressed type 2 cytokines such as IL-4 and IL-13. In chronic disease, the additional contribution from type 1, 17, and 22 cells also secrete many cytokines and recruit cells, resulting in the chronic feature of the disease. The understanding of AD pathogenesis relies mostly on translational analysis from Western population. In this article, we would introduce the recent study progress in Asian and Taiwanese AD populations that obviously are different from Western populations. With an aim to clarify the clinical and molecular heterogeneity of AD from diverse ethnic backgrounds, this report will focus on the alternation of immune axis of AD. By means of illustrating this population-centered analyses from underlying molecular signatures of Asian and Taiwanese AD, we hope to identify the best immune modifying therapies according to the underlying pathogenic pathway to bring excellent therapeutic responses. With the help of the next-generation sequencing technique, precision medicine would not only be focused on choosing specific agents but also specific individuals, and at the same time reduce the global economic burden of the disease.