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Monocyte Chemotactic Protein-2 (Mcp-2) Uses Ccr1 and Ccr2b As Its Functional Receptors

  1. Author:
    Gong, X. Q.
    Gong, W. H.
    Kuhns, D. B.
    Benbaruch, A.
    Howard, O. M. Z.
    Wang, J. M.
  2. Author Address

    Wang JM NCI IRSP SAIC FREDERICK FCRDC BLDG 560 RM 31-19 FREDERICK, MD 21702 USA NCI IRSP SAIC FREDERICK FCRDC FREDERICK, MD 21702 USA NCI CLIN IMMUNOL SERV SAIC FREDERICK FCRDC FREDERICK, MD 21702 USA NCI MOL IMMUNOREGULAT LAB DIV BASIC SCI FCRDC FREDERICK, MD 21702 USA
    1. Year: 1997
  1. Journal: Journal of Biological Chemistry
    1. 272
    2. 18
    3. Pages: 11682-11685
  2. Type of Article: Article
  1. Abstract:

    Monocyte chemotactic protein (MCP)-2 is a member of the C-C chemokine subfamily, which shares more than 60% sequence homology with MCP-1 and MCP-8 and about 30% homology with macrophage inflammatory protein (MIP)-1 alpha, regulated on activation of normal T cell expressed (RANTES), and MIP-1 beta. Despite this considerable sequence homology to other C-C chemokines, MCP-2 appears to have unique functional properties in comparison with other C-C chemokines such as MCP-1 and MCP-3. Although evidence obtained from studies on leukocytes suggested that MCP-2 may share the receptors with these C-C chemokines, the actual functional receptors for MCP-2 have not yet been identified. In this study, by using radioiodinated MCP-2, we identified high affinity binding sites for MCP-2 on human peripheral blood monocytes. The MCP-2 binding was competed for by MCP-1 and MCP-3, but less well by MIP-1 alpha or RANTES. In experiments using cells transfected with C-C chemokine receptors, I-125-MCP-2 bound to human embryonic kidney 293 cells transfected with CCR1 or CCR2B, known to also bind MIP-1 alpha/RANTES and MCP-1, respectively, but both shared by MCP-3. The binding of I-125-MCP-2 to these receptor-transfected cells was displaced completely by chemokines that bind to these receptors. Both CCR1- and CCR2B-transfected 293 cells showed significant migration in response to MCP-2, in addition to responding to other specific chemokines. These results clearly demonstrate that MCP-2, unlike MCP-1, uses both CCR1 as well as CCR2B as its functional receptors, and this accounts for the unique activities of MCP-2. [References: 26]

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