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Cells and organs of Immune system Parmar Krupal Classification of organ of immune system • Primary Lymphoid Organs—Where Immune Cells develop • Site for development and maturation of lymphocytes. • i.e. the bone marrow and the thymus—regulate the development of immune cells from immature precursors. • Secondary Lymphoid Organs—Where the Immune response Is Initiated • Sites for lymphocytes and antigen interaction. • i.e. including the spleen, lymph nodes, and specialized sites in the gut and other mucosal tissues, MALT Diagram of a lymph node, showing the flow of lymph through the lymph sinuses. • hematopoietic stem cell (HSC) : all functionally specialized, mature blood cells (red blood cells, granulocytes, macrophages, dendritic cells, and lymphocytes) arise from a single cell type. • The process by which HSCs differentiate into mature blood cells is called hematopoiesis. • Two primary lymphoid organs are responsible for the development of stem cells into mature immune cells: • the bone marrow, – where HSCs reside and give rise to all cell types; and • thymus, – where T cells complete their maturation • Stem cells are defined by two capacities: • (1) the ability to regenerate or “self-renew” • (2) the ability to differentiate into all diverse cell types. • Types of stem cell » Embryogenic stem cell capacity to generate every specialized cell type in an organism( in other words, they are pluripotent ) » Adult stem cell have the capacity to give rise to the diverse cell types that specify a particular tissue. Multiple adult organs harbor stem cells (“adult stem cells”) that can give rise to mature tissue-specific cells. •Self-renewing hematopoietic stem cells give rise to lymphoid and myeloid progenitors. • Most immune cells mature in the bone marrow and then travel to peripheral organs via the blood. Some, including mast cells and macrophages, undergo further maturation outside the bone marrow. T cells develop to maturity in the thymus. • HSC can become a common myeloiderythroid progenitor (CMP), which gives rise to all red blood cells (the erythroid lineage), granulocytes, monocytes, and macrophages (the myeloid lineage), or • Either it can become a common lymphoid progenitor (CLP), which gives rise to B lymphocytes, T lymphocytes, and NK cells. • Regulation of Lineage Commitment during Hematopoiesis • Multiple genes that specify lineage commitment have been identified. Many of these are transcriptional regulators Transcription factor Importance GATA-2 required form the development of all hematopoietic lineages. in its absence animals die during embryogenesis. Bmi-1 It is required for the self-renewal capacity of HSCs, and in its absence animals die within 2 months of birth because of the failure to repopulate their red and white blood cells. Ikaros is required for lymphoid but not myeloid development; animals survive in its absence but cannot mount a full immune response (i.e., they are severely immunocompromised). Notch1 regulates the choice between T and B lymphocyte lineages
