ABSTRACT
Developing the ability to regulate actions, thoughts, and emotions is necessary for successfully engaging in goal-directed activities, which form the essence of success in many life situations. In this regard, executive function (EF), as an aspect of these top-down control processes, has been the subject of inquiry in many developmental studies aiming to identify its link with various other aspects of a child's life, including family socioeconomic status (SES). This article presents a critical look at the association between family SES and childhood EF by reviewing studies that provide contrasting perspectives compared to the generally reported positive correlation between these two constructs. We first address the various aspects of assessing SES and childhood EF, emphasizing their multifaceted nature. Next, we discuss the interplays between different components of these two constructs, especially as it unfolds in various cultural contexts. Finally, we conclude by discussing mainly neglected lines of research that could further improve our understanding of the extent of socioeconomic impacts on child development, specifically regarding executive function. Considering these lines of research is a necessary step to a more accurate analysis of the link between socioeconomic factors and childhood executive function.
ABSTRACT
Innate lymphoid cells (ILCs) are a heterogeneous family of immune cells that play a critical role in a variety of immune processes including host defence against infection, wound healing and tissue repair. Whether these cells are involved in lipid-dependent immunity remains unexplored. Here we show that murine ILCs from a variety of tissues express the lipid-presenting molecule CD1d, with group 3 ILCs (ILC3s) showing the highest level of expression. Within the ILC3 family, natural cytotoxicity triggering receptor (NCR)-CCR6+ cells displayed the highest levels of CD1d. Expression of CD1d on ILCs is functionally relevant as ILC3s can acquire lipids in vitro and in vivo and load lipids on CD1d to mediate presentation to the T-cell receptor of invariant natural killer T (iNKT) cells. Conversely, engagement of CD1d in vitro and administration of lipid antigen in vivo induce ILC3 activation and production of IL-22. Taken together, our data expose a previously unappreciated role for ILCs in CD1d-mediated immunity, which can modulate tissue homeostasis and inflammatory responses.
Subject(s)
Antigens, CD1d/genetics , Immunity, Innate , Interleukins/biosynthesis , Lymphocyte Activation , Lymphocyte Subsets/metabolism , Lymphocytes/metabolism , Animals , Antigen Presentation/immunology , Antigens, CD1d/metabolism , Biomarkers , Gene Expression , Immunophenotyping , Lipid Metabolism , Lipids/immunology , Lymphocyte Activation/immunology , Lymphocyte Subsets/immunology , Lymphocytes/immunology , Mice , Mice, Transgenic , Phenotype , Interleukin-22ABSTRACT
BACKGROUND: The diverse roles of innate immune cells in the pathogenesis of asthma remain to be fully defined. Natural killer (NK) cells are innate lymphocytes that can regulate adaptive immune responses. NK cells are activated in asthma; however, their role in allergic airway inflammation is not fully understood. OBJECTIVE: We investigated the importance of NK cells in house dust mite (HDM)-triggered allergic pulmonary inflammation. Specifically, we aimed to determine the role of the major NK-cell activating receptor NKG2D and NK-cell effector functions mediated by granzyme B. METHODS: Allergic airway inflammation was induced in the airways of mice by repeated intranasal HDM extract administration and responses in wild-type and NKG2D-deficient mice were compared. Adoptive transfer studies were used to identify the cells and mechanisms involved. RESULTS: Mice that lacked NKG2D were resistant to the induction of allergic inflammation and showed little pulmonary eosinophilia, few airway TH2 cells, and no rise in serum IgE after multiple HDM-allergen exposures. However, NKG2D was not required for pulmonary inflammation after a single inoculation of allergen. NKG2D-deficient mice showed no alteration in responses to respiratory virus infection. Transfer of wild-type NK cells (but not CD3(+) cells) into NKG2D-deficient mice restored allergic inflammatory responses only if the NK cells expressed granzyme B. CONCLUSIONS: These studies established a pivotal role for NK-cell NKG2D and granzyme B in the pathogenesis of HDM-induced allergic lung disease, and identified novel therapeutic targets for the prevention and treatment of asthma.
