Induction of lymphoproliferative popliteal lymph node reaction by hydantoin derivatives: structure-activity relationships.

We evaluated the ability of a series of 3-phenylhydantoin derivatives to induce a lymphoproliferative popliteal lymph node reaction in C57B1/6 mice. 5-Aryl-3-phenylhydantoins induced a significant lymphoproliferative reaction, whereas the 5-alkyl-substituted and the unsubstituted 3-phenylhydantoins did not. 5-Alkyl-3-phenylhydantoins were unable to induce a lymphoproliferative reaction, unlike the corresponding 5-alkyl-3-phenyl-2-thiohydantoins, which have been reported to induce a significant lymphoproliferative reaction in the same strain of mice. Based on these results, we suggest that, to induce a lymphoproliferative popliteal lymph node reaction, hydantoins have to bind covalently to proteins through the N-atoms if they are activated by electrophilic groups bound to the hydantoin ring. We also suggest that 2-thiohydantoins can bind through their S-atom, whereas hydantoins cannot do so through their O-atoms.

Immunological alterations inducible by mercury compounds. III. H-2A acts as an immune response and H-2E as an immune "suppression" locus for HgCl2-induced antinucleolar autoantibodies.

In responder mouse strains repeated injections of subtoxic doses of HgCl2 induce formation of antinuclear autoantibodies (ANA) and antinucleolar autoantibodies (ANolA). Others have shown that responsiveness to HgCl2-induced formation of ANA and ANolA is linked to H-2. Here, we extend these studies to a variety of mouse strains not tested previously. After confirming that strain B10.S (H-2s) is a high responder we have shown that strains B10.D2 (H-2d) and B10.BR (H-2k) are nonresponders. By comparing a panel of strains carrying appropriate intra-H-2 recombinant haplotypes derived from d, k and s, we were able to map responsiveness to As. Interestingly, among four strains all of which were As, and thus responsive, only the two H-2E- ones, B10.S and B10.RSD2, were high responders whereas the two H-2E+ ones, B10.HTT and B10.S(9R), were significantly less responsive. Thus, the genetics of HgCl2-induced autoantibody formation follow the rules established for immune responses to a variety of different antigens in that expression of H-2E "suppressed" the response.