T cell clones specific for hybrid I-A molecules. Discrimination with monoclonal anti-I-A (k) antibodies

doi:10.1084/jem.156.4.1186

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T cell clones specific for hybrid I-A molecules. Discrimination with monoclonal anti-I-A (k) antibodies

BN Beck, JG Frelinger, M Shigeta, AJ Infante, D Cummings, G Hammerling, and CG Fathman

Alloreactive and soluble antigen-reactive, I-A-restricted T cell clones were examined for their ability to recognize hybrid I-A antigens. Several clones that recognized hybrid I-A(b)/I-A(k) molecules on (C57BL/6 x A/J)F(1) [(B6A)F(1)] spleen cells were studied. We were able to distinguish clones that recognized hybrid I-A molecules of the A(b)(a)A(k)( $beta$ ) type from those that recognized A(k)(a)A(b)( $beta$ ) molecules. We reached this conclusion by considering data from three independent types of experiments. (a) Monoclonal antibodies were used to inhibit T cell stimulation. Antibodies 10.2.16 and H116.32 distinguished two mutually exclusive �families� of T cell clones. One group of clones was inhibited by 10-2.16 and not H116.32, the other group exhibited reciprocal inhibition. (b) T cell proliferation was assayed using antigen-presenting cells from B6.C-H-2(bml2) (bml2) and [bml2 � B10.A(4R)]F(1) mice. Because the bml2 strain has a mutation that results in an altered A(b)( $beta$ ) polypeptide chain (A(bm12)( $beta$ )), we reasoned that clones that could recognize the [bm12 � B 10.A(4R)]F(1) cells were recognizing A(b)(a)A(k)( $beta$ ) molecules. Alternatively, clones not recognizing [bml2 � B10.A(4R)]F(1) cells had specificity for A(k)(a)A(b)( $beta$ ) molecules. (c) I-A molecules immunoprecipitated from radiolabeled (B6A)F(1) splenocyte extracts were analyzed by two-dimensional sodium dodecyl sulfate-polyacrylamide gel electrophoresis. These experiments confirmed an earlier report that antibody 10.2.16 recognized determinants on the A(k)( $beta$ ) chain (12). Antibody H116.32 immunoprecipitated products consistent with recognition of A(k)(a) determinants. Taken together, these three types of results offer conclusive evidence that T cell clones recognizing �hybrid� I-A molecules use either A(b(k)A(k)( $beta$ ) or A(k)(a)A(b)( $beta$ ) molecules as recognition or restriction sites. Clones whose proliferation was supported by [bm 12 x B10.A(4R)]F(1) cells and blocked by anti-I-A(k) antibody 10-2.16 recognized A(b)(a)A(k)( $beta$ ) B molecules. Clones that were blocked by antibody H116.32 and did not recognize [bml2 X B10.A(4R)]F(1) cells use a recognition site(s) on A(b)(a)A(k)( $beta$ ) molecules. Thus, we can demonstrate both functionally and biochemically that hybrid F(1) I-A molecules of the structure A(k)(a)A(b)( $beta$ ) and A(b)(a)A(k)( $beta$ ) both exist on (B6A)F(1) splenocytes and that both configurations are used in immune recognition phenomena.
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