Abstract
CD4+T helper (Th) cells are important mediators of immune responses in asthma and cancer. When counteracted by different classes of pathogens, naïve CD4+T cells undergo programmed differentiation into distinct types of Th cells. Th cells orchestrate antigen-specific immune responses upon their clonal T-cell receptor (TCR) interaction with the appropriate peptide antigen presented on MHC class II molecules expressed by antigen-presenting cells (APCs). T helper 9 (Th9) cells and regulatory T (Treg) cells and their corresponding cytokines have critical roles in tumor and allergic immunity. In the context of asthma and cancer, the dynamic internal microenvironment, along with chronic inflammatory stimuli, influences development, differentiation, and function of Th9 cells and Treg cells. Furthermore, the dysregulation of the balance between Th9 cells and Treg cells might trigger aberrant immune responses, resulting in development and exacerbation of asthma and cancer. In this review, the development, differentiation, and function of Th9 cells and Treg cells, which are synergistically regulated by various factors including cytokine signals, transcriptional factors (TFs), costimulatory signals, microenvironment cues, metabolic pathways, and different signal pathways, will be discussed. In addition, we focus on the recent progress that has helped to achieve a better understanding of the roles of Th9 cells and Treg cells in allergic airway inflammation and tumor immunity. We also discuss how various factors moderate their responses in asthma and cancer. Finally, we summarize the recent findings regarding potential mechanisms for regulating the balance between Th9 and Treg cells in asthma and cancer. These advances provide opportunities for novel therapeutic strategies that are aimed at reestablishing the balance of these cells in the diseases.
Highlights
When detected of a wide variety of pathogens, the adaptive immune system utilizes T lymphocytes to establish and maintain immune response [1, 2]
Upon interaction with antigen presented by antigen-presenting cells (APCs) such as dendritic cells (DCs), naïve CD4+T cells can differentiate into distinct types of CD4+T helper cells (Th cells) including Th1, Th2, Th17, T helper 9 (Th9), Th22, follicular T helper (Tfh), and partial regulatory T cell (Treg) subsets [3]
During the severity of allergic airway inflammation and tumor, Treg cells adapt to the local environmental changes through functional and phenotypic reprogramming [213, 214]
Summary
When detected of a wide variety of pathogens, the adaptive immune system utilizes T lymphocytes to establish and maintain immune response [1, 2]. Treg cells play indispensable roles in preventing immune pathology induced by pathogens and in maintaining tolerance to allergens by regulating allergen-triggered immune response [8, 9]. Th9 cells and Treg cells exhibit some degree of plasticity of coexpressing specific cytokines [19]. These concepts may be at the core of the mechanisms involved in regulating balance between these cells in asthma and cancer (discussed in detail below). We focus on potential methods and mechanisms of reestablishing the balance between Th9 and Treg cells that control the development of asthma and cancer
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