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B cells are lymphocytes that play a large role in the humoral immune response as opposed to the cell-mediated immune response that is governed by T cells. The abbreviation "B" comes from bursa of Fabricius that is an organ in birds in which avian B cells mature. The principal function of B cells is to make antibodies against soluble antigens. B cells are an essential component of the adaptive immune system.

Contents 1 Development of B cells 2 Functions 2.1 B cell types 3 Recognition of antigen by B cells 4 Activation of B cells 4.1 T-cell dependent activation 4.2 T-cell independent activation 5 The ancestral roots of B cells 6 References 7 See also 8 External links

[edit] Development of B cells

B cells are produced in the bone marrow of most mammals. Rabbits are an exception; their B cells develop in the appendix-sacculus rotundus. B cell development occurs through several stages, each stage representing a change in the genome content at the antibody loci. An antibody is composed of two light (L) and two heavy (H) chains, and the genes specifying them are found in the 'H' chain locus and the 'L' chain locus. In the H chain loci there are three regions, V, D and J, which recombine randomly, in a process called VDJ recombination, to produce a unique variable domain in the immunoglobulin of each individual B cell. Similar rearrangements occur for L chain locus except there are only two regions, namely V and J. The list below describes the process of immunoglobulin formation at the different stages of B cell development.

• Progenitor B cells - Contains Germline H genes, Germline L genes
• Early Pro-B cells - undergoes D-J rearrangement on the H chains
• Late Pro-B cells - undergoes V-DJ rearrangement on the H chains
• Large Pre-B cells - the H chain is VDJ rearranged, Germline L genes
• Small Pre-B cells - undergoes V-J rearrangement on the L chains
• Immature B cells - VJ rearranged on L chains, VDJ rearranged on H chains. There is start of expression of IgM receptors.
• Mature B cells - There is start of expression of IgD

When the B cell fails in any step of the maturation process, it will die by a mechanism called apoptosis. If it recognizes self-antigen during the maturation process, the B cell will become suppressed (known as anergy) or undergo apoptosis. B cells are continuously produced in the bone marrow, but only a small portion of newly made B cells survive to participate a part in the long-lived peripheral B cell pool.

[edit] Functions

The human body makes millions of different types of B cells each day that circulate in the blood and lymph performing the role of immune surveillence. They do not produce antibodies until they become fully activated. Each B cell has a unique receptor protein (referred to as the B cell receptor (BCR)) on its surface that will bind to one particular antigen. The BCR is a membrane-bound immunoglobulin, and it is this molecule that allows the distinction of B cells from other types of lymphocyte, as well as being the main protein involved in B cell activation. Once a B cell encounters its cognate antigen and receives an additional signal from a helper T cell, it can further differentiate into one of the two types of B cells listed below. The B cell has two choices at this stage; it can either become one of these cell types directly or it can go through an intermediate differentiation step (the germinal center reaction) where the B cell will hypermutate the variable region of its immunoglobulin gene and possibly undergo class switching.

[edit] B cell types

• Plasma B cells are large B cells often referred to as antibody factories. Their main function is to secrete antibodies, which assist in the destruction of microbes by binding to them and making them easier targets for phagocytes.
• Memory B cells are formed from activated B cells that are specific to the antigen encountered during the primary immune response. These cells are able to live for a long time, and can respond quickly following a second exposure to the same antigen.

• B-1 cells are B cells that express CD5, which can bind to another B cell surface protein, CD72. CD5-CD72 is thought to mediate B cell-B cell interaction. B-1 cells express IgM in greater quantities than IgG and its receptors show polyspecificity, meaning that they have low affinities for many different antigens, but have a preference for other immunoglobulins, self antigens and common bacterial polysaccharides. B-1 cells are present in low numbers in the lymph nodes and spleen and are instead found predominantly in the peritoneal and pleural cavities. B-1 cells generate diversity mainly via recombinatorial recombination (there is a preferential recombination between D-proximal VH gene segments). B-1 cells are first produced in the fetus, unlike conventional B-2 cells that are produced after birth and replaced in the bone marrow.
• B-2 cells are the conventional B cells most texts refer to.

[edit] Recognition of antigen by B cells

A critical difference between B cells and T cells is how each lymphocyte "sees" its antigen. B cells recognize their cognate antigen in its native form. They recognize free (soluble) antigen in the blood or lymph using their BCR or membrane bound-immunoglobulin. In contrast, T cells recognize their cognate antigen in a processed form, as a peptide fragment presented by a MHC molecule to the T cell receptor.

[edit] Activation of B cells

B cell recognition of antigen is not the only element necessary for B cell activation (a combination of clonal proliferation and terminal differentiation into plasma cells). Naive B cells can be activated in a T-cell dependent or independent manner.

[edit] T-cell dependent activation

When a B cell ingests a pathogen, it attaches parts of the pathogen's proteins to a class II MHC protein. This complex is moved to the outside of the cell membrane, where it can be recognized by a T lymphocyte, which is compatible with similar structures on the cell membrane of a B lymphocyte. If the B cell and T cell structures match, the T lymphocyte activates the B lymphocyte, which produces antibodies against the bits of pathogen, called antigen, it has presented on its surface.

Most antigens are T-dependent, meaning T cell help is required for maximal antibody production. With a T-dependent antigen, the first signal comes from antigen cross linking the B cell receptor (BCR) and the second signal comes from co-stimulation provided by a T cell. T dependent antigens contain proteins that are presented on B cell Class II MHC to a special subtype of T cell called a Th2 cell. When a B cell processes and presents the same antigen to the primed T_h cell, the T cell secretes cytokines that activate the B cell. These cytokines trigger B cell proliferation and differentiation into plasma cells. Isotype switching to IgG, IgA, and IgE and memory cell generation occur in response to T-dependent antigens.

[edit] T-cell independent activation

Many antigens are T-independent, meaning they can deliver both of the signals to the B cell. Mice without a thymus (nude or athymic mice that do not produce any T cells) can respond to T-independent antigens. Many bacteria have repeating carbohydrate epitopes that stimulate B cells, through so called pattern recognition receptors, to respond with IgM synthesis in the absence of T cell help. There are two types of T-cell independent activation; Type 1 T cell-independent (polyclonal) activation, and type 2 T cell-independent activation (in which macrophages present several of the same antigen in a way that causes cross-linking of antibodies on the surface of B cells).

[edit] The ancestral roots of B cells

In an October 2006 issue of Nature Immunology, it was reported that certain B-cells of primitive vertebrates (like fish and amphibians) are capable of phagocytosis, a function usually associated with cells of the innate immune system. The authors of this article postulate that these phagocytic B-cells represent the ancestral history shared between macrophages and lymphocytes; B-cells may have evolved from macrophage-like cells during the formation of the adaptive immune system<ref>J. Li, D.R. Barreda, Y.-A. Zhang, H. Boshra, A.E. Gelman, S. LaPatra, L. Tort & J.O. Sunyer (2006). "B lymphocytes from early vertebrates have potent phagocytic and microbicidal abilities". Nature Immunology 7: 1116–1124.</ref>.

[edit] References

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[edit] See also

• Affinity maturation
• Antibody
• Clonal selection
• Original antigenic sin

[edit] External links

• MeSH A11.063.438

v • d • e</span>  Blood - Blood plasma
Pluripotential hemopoietic stem cells | Red blood cells (Reticulocyte, Normoblast) | White blood cells
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Myeloid
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v • d • e</span>  Immune system
Adaptive immune system | Innate immune system | Humoral immune system | Cellular immune system | Immunological tolerance | Lymphatic system | White blood cells | Antibodies | Antigen (MHC) | Complement system | Inflammation

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