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CD20 antibody

MS4A1 Reactivity: Human FACS, ELISA, IP, IHC (fro) Host: Mouse Monoclonal NKI-B20 unconjugated
Catalog No. ABIN1042459
  • Target See all CD20 (MS4A1) Antibodies
    CD20 (MS4A1) (Membrane-Spanning 4-Domains, Subfamily A, Member 1 (MS4A1))
    Reactivity
    • 259
    • 57
    • 23
    • 18
    • 17
    • 16
    • 11
    • 7
    • 6
    • 5
    • 2
    • 2
    Human
    Host
    • 190
    • 96
    • 2
    • 2
    Mouse
    Clonality
    • 208
    • 80
    • 1
    Monoclonal
    Conjugate
    • 107
    • 21
    • 18
    • 16
    • 13
    • 8
    • 6
    • 6
    • 6
    • 6
    • 6
    • 6
    • 5
    • 4
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 2
    • 2
    • 2
    • 2
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    This CD20 antibody is un-conjugated
    Application
    • 218
    • 93
    • 77
    • 46
    • 46
    • 37
    • 25
    • 20
    • 19
    • 16
    • 14
    • 13
    • 11
    • 11
    • 6
    • 5
    • 3
    • 2
    • 2
    • 1
    • 1
    • 1
    Flow Cytometry (FACS), ELISA, Immunoprecipitation (IP), Immunohistochemistry (Frozen Sections) (IHC (fro))
    Specificity
    See Background.
    Characteristics
    CD markers
    Purification
    Purified
    Clone
    NKI-B20
    Isotype
    IgG1, IgG2a, IgG2b
    Top Product
    Discover our top product MS4A1 Primary Antibody
  • Application Notes
    NKI-B20 is used in research and human diagnostics, cell separation for research or clinical application. NKI-B0is useful for ELISA, immunoprecipitation, flow cytometry and immunohistochemisitry on frozen sections. Optimal antibody dilution should be determined by titration.
    Comment

    NKI-B20 is a combination of three switch variants mouse monoclonal (IgG1, IgG2a, IgG2b) antibody derived by fusion of SP2/0 mouse myeloma cells with spleen cells from a BALB/c mouse immunized with Daudi cells (Burkitt lymphoma).

    Restrictions
    For Research Use only
  • Buffer
    PBS containing 0.09% sodium azide.
    Preservative
    Sodium azide
    Precaution of Use
    This product contains sodium azide: a POISONOUS AND HAZARDOUS SUBSTANCE which should be handled by trained staff only.
    Storage
    4 °C
  • Hooijberg, Sein, van den Berk, Hekman: "Characterization of a series of isotype switch variants of a new CD20 monoclonal antibody." in: Hybridoma, Vol. 15, Issue 1, pp. 23-31, (1997) (PubMed).

  • Target
    CD20 (MS4A1) (Membrane-Spanning 4-Domains, Subfamily A, Member 1 (MS4A1))
    Alternative Name
    CD20 (MS4A1 Products)
    Synonyms
    B1 antibody, Bp35 antibody, CD20 antibody, CVID5 antibody, LEU-16 antibody, MS4A2 antibody, S7 antibody, AA960661 antibody, Cd20 antibody, Ly-44 antibody, Ms4a2 antibody, MS4A1 antibody, bp35 antibody, cd20 antibody, ms4a2 antibody, leu-16 antibody, ms4a4c antibody, cd20-like antibody, membrane spanning 4-domains A1 antibody, membrane-spanning 4-domains, subfamily A, member 1 antibody, B-lymphocyte antigen CD20 antibody, MS4A1 antibody, Ms4a1 antibody, ms4a1 antibody, LOC101694281 antibody
    Background
    The antigen recognized by CD20 MAbs is a 35-37 kDa non-glycosylated phosphoprotein, that may function as a Ca2+ ion channel The protein structure deduced from cloned DNA sequence suggests that the CD20 antigen is a transmembrane protein that passes the membrane four times, with both the C- and the N-terminus on the cytoplasmic side and only a small part exposed on the cell surface. Expression of CD20 antigen is specific for B lymphocytes and is present during most differentiation stages, beginning at the early pre-B cell stage and disappearing upon differentiation into plasma cells. The CD20 molecule appears to be involved in the activation and cell cycle progress of B lymphocytes. Stimulating as well as inhibitory effects in different phases of the cell cycle have been reported for different CD20 MAbs. Pokeweed mitogen induced differentiation of B lymphocytes into Ig-producing cells is inhibited by CD20 MAbs. The CD20 antigen is also expressed on most malignant B cells. In agreement with the expression during normal B cell differentiation, all malignancies of mature B cells are CD20 positive, but early pre-B ALL cells often lack CD20 antigen. The restriction of its expression to B lineage cells, together with the lack of expression on progenitor cells, makes CD20 antigen an interesting target for (antibody-based) immunotherapy for B cell lymphoid malignancies. Moreover, CD20 antigen is expressed at relatively high density on most normal and malignant B cells and it is not susceptible to antibody induced modulation. A series of heavy chain switch variants has been isolated from a new B cell-specific monoclonal antibody belonging in the CD20 cluster. The antibodies NKI-B20/1, NKI-B20/2b, and NKI-B20/2a (of isotype IgG1, IgG2b, and IgG2a, respectively) have been used to study the influence of isotype and of the target antigen on the capacity to mediate cytotoxicity with a number of effector mechanisms. Unlike many mouse MAbs, NKI-B20/2b and NKI-B20/2a are cytolytic with human complement on human target cells that did not express the complement regulatory factor HRF20. All 3 isotypes of NKI-B20 mediated antibody-dependent cell-mediated cytotoxicity (ADCC) with rIL-2-activated NK cells from mouse spleen. Here the antigen density seemed the most important factor in determining the level of cell kill. With mouse peritoneal macrophages as effector cells again all 3 isotypes of NKI-B20 mediated cytotoxicity. For the IgG1 and IgG2b variants of NKI-B20 this is at variance to what has been reported for MAbs of other specificities. Despite the high activity with murine effector cells none of the NKI-B20 MAbs mediated ADCC with human peripheral blood NK cells, with or without stimulation with rIL-2, due to the lack of interaction of the murine MAbs with the human Fc receptor. The CD20 antigen appears to be a good target antigen for various forms of cytotoxicity, to which its relatively high antigenic density, its resistance to antibody-induced modulation, and its unusual structure all contribute.
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