Evidence for multiple sites of interaction between IL-12 and its receptor

Publication

Evidence for multiple sites of interaction between IL-12 and its receptor

Journal Paper/Review - Oct 31, 1996

Presky D H, Minetti L J, Gillessen Sommer Silke, Gubler U, Chizzonite R, Stern A S, Gately M K

Units

Medizinische Onkologie und Hämatologie

PubMed

8958964

Citation

Presky D, Minetti L, Gillessen Sommer S, Gubler U, Chizzonite R, Stern A, Gately M. Evidence for multiple sites of interaction between IL-12 and its receptor. Annals of the New York Academy of Sciences 1996; 795:390-3.

Type

Journal Paper/Review (English)

Journal

Annals of the New York Academy of Sciences 1996; 795

Publication Date

Oct 31, 1996

Issn Print

0077-8923

Pages

390-3

Brief description/objective

We have previously described the identification of a protein, now designated IL-12R beta 1, that binds 125I-huIL-12 with a Kd of about 10 nM, corresponding to the low affinity 125I-huIL-12 binding sites seen on PHA-activated human lymphoblasts. Using expression cloning techniques, we have recently identified an additional IL-12-binding protein subunit, IL-12R beta 2, which binds 125I-huIL-12 with a Kd of about 5 nM when expressed alone in COS-7 cells. Coexpression of IL-12R beta 1 and IL-12R beta 2 in COS-7 cells results in formation of two classes of 125 I-huIL-12-binding sites with Kds of about 50 pM and 5 nM. Mouse IL-12 p40 subunit homodimer (mo(p40)2) blocked 125I-huIL-12 binding to human IL-12R beta 1, but did not inhibit binding to human IL-12R beta 2. In contrast, anti-huIL-12 monoclonal antibody 20C2, which does not block 125I-huIL-12 binding to human IL-12R beta 1, completely blocked binding to human IL-12R beta 2. These results demonstrate that two classes of IL-12 inhibitors, one that primarily blocks IL-12/IL-12R beta 1 interaction (e.g., mo(p40)2), and one that primarily blocks IL-12/IL-12R beta 2 interaction (e.g., 20C2), can be identified.