ABSTRACT
Malaria is a fatal human parasitic disease transmitted by a mosquito vector. Although the evolution of within-host malaria virulence has been the focus of many theoretical and empirical studies, the vector's contribution to this process is not well understood. Here, we explore how within-vector resource exploitation would impact the evolution of within-host Plasmodium virulence. By combining within-vector dynamics and malaria epidemiology, we develop a mathematical model, which predicts that non-competitive parasitic resource exploitation within-vector restricts within-host parasite virulence. To validate our model, we experimentally manipulate mosquito lipid trafficking and gauge within-vector parasite development and within-host infectivity and virulence. We find that mosquito-derived lipids determine within-host parasite virulence by shaping development (quantity) and metabolic activity (quality) of transmissible sporozoites. Our findings uncover the potential impact of within-vector environment and vector control strategies on the evolution of malaria virulence.
Subject(s)
Malaria/parasitology , Plasmodium/pathogenicity , Animals , Humans , Malaria/transmission , Mosquito Vectors/parasitology , VirulenceABSTRACT
TH17 cells are major drivers of inflammation and involved in several autoimmune diseases. Tissue inflammation is a beneficial host response to infection, but it can also contribute to autoimmunity. The crosstalk between a tissue and the immune system during an inflammatory response is key for preserving tissue integrity and restoring physiological processes. However, how the inflamed tissue regulates the magnitude of an immune response by controlling pro-inflammatory T cells is not well characterized so far. Here we show that TH17 cells accumulating in the small intestine upon inflammation express the IL-33 receptor (ST2) and intestinal epithelial cells (IEC) are the main source of the alarmin interleukin-33 (IL-33). We show that pro-inflammatory TH17 cells acquire a regulatory phenotype with immunosuppressive properties in response to IL-33. Absence of ST2 signaling promotes the secretion of pro-inflammatory cytokines by TH17 cells and dampens the secretion of IL-10. Our results provide new insights into the mechanisms by which IEC, via IL-33/ST2 axis, may control pro-inflammatory TH17 cells in the small intestine to sustain homeostasis.
Subject(s)
Alarmins/metabolism , Inflammation/immunology , Interleukin-1 Receptor-Like 1 Protein/metabolism , Interleukin-33/metabolism , Intestine, Small/immunology , T-Lymphocytes, Regulatory/immunology , Th17 Cells/immunology , Animals , Cells, Cultured , Homeostasis , Interleukin-1 Receptor-Like 1 Protein/genetics , Interleukin-10/metabolism , Mice , Mice, Inbred C57BL , Mice, Knockout , Signal TransductionABSTRACT
During systemic immune responses, plasma blasts are generated in secondary lymphoid organs and migrate to the bone marrow, where they can become long-lived, being responsible for the maintenance of long-term antibody titers. Plasma blasts generated in mucosal immune responses of the small intestine home to the lamina propria (LP), producing mainly immunoglobulin A. The migration of these antibody-secreting cells is well characterized during acute immune responses. Less is known about their lifetime and contribution to the long-lived bone marrow compartment. Here we investigate the lifetime of plasma cells (PCs) and the relationship between the PC compartments of the gut and bone marrow after oral immunization. Our findings indicate that PCs in the LP can survive for extended time periods. PCs specific for orally administered antigens can be detected in the bone marrow for at least 9 months after immunization, indicating that the mucosal PC compartment can contribute to the long-lived PC pool in this organ, independent of the participation of splenic B cells. Our findings suggest that the compartmentalization between mucosal and systemic PC pools is less strict than previously thought. This may have implications for the development of vaccines as well as for autoantibody-mediated diseases.
Subject(s)
Bone Marrow Cells/immunology , Cell Lineage/immunology , Immunity, Mucosal , Plasma Cells/immunology , Administration, Oral , Animals , Bone Marrow Cells/cytology , Bone Marrow Cells/drug effects , Cell Movement/drug effects , Cell Movement/immunology , Cholera Toxin/administration & dosage , Immunity, Mucosal/drug effects , Immunization , Immunoglobulin A/biosynthesis , Immunoglobulin G/biosynthesis , Immunoglobulin M/biosynthesis , Immunologic Memory , Intestine, Small/cytology , Intestine, Small/drug effects , Intestine, Small/immunology , Mice , Mice, Inbred C57BL , Mucous Membrane/cytology , Mucous Membrane/drug effects , Mucous Membrane/immunology , Ovalbumin/administration & dosage , Plasma Cells/cytology , Plasma Cells/drug effectsABSTRACT
The Greek term stroma literally means in translation mattress, covering or bed. In the medical context this describes the connective tissue framework of an organ which is composed of the stromal cells and the extracellular matrix components which are produced by these cells. According to the original definition stromal cells have a non-hematopoietic origin and adherently grow in cell culture. Nowadays the term is used to cover a heterogeneous group of connective tissue cells of mesenchymal origin which includes fibroblasts, reticular stromal cells and endothelial cells as well as tissue-specific connective tissue cells, such as osteoblasts and adipocytes. Because the stromal cells in the various tissues are very different with respect to morphology and functional characteristics, the manifold aspects of the individual stromal cell populations are now just beginning to be understood. This article presents a summary of new knowledge on the various functions of stromal cells in the immune response.
