Binding of Synthetic LKEKK Peptide to Human T-Lymphocytes.

Biochemistry. Biokhimiia2016PMID: 27677554

View on PubMed DOI: 10.1134/S0006297916080071

Plain Language Summary

Researchers identified a non-protein receptor on human T cells that binds the synthetic peptide LKEKK -- a sequence shared by both thymosin alpha-1 and interferon alpha-2 -- with very high affinity. The binding was blocked by both thymosin alpha-1 and interferon alpha-2, as well as by cholera toxin B subunit, revealing a shared receptor mechanism that may explain overlapping immune effects of these molecules.

Abstract

The synthetic peptide LKEKK corresponding to sequence 16-20 of human thymosin-α1 and 131-135 of human interferon-α2 was labeled with tritium to specific activity 28 Ci/mol. The [3H]LKEKK bound with high affinity (Kd = 3.7 ± 0.3 nM) to donor blood T-lymphocytes. Treatment of cells with trypsin or proteinase K did not abolish [3H]LKEKK binding, suggesting the non-protein nature of the peptide receptor. The binding was inhibited by thymosin-α1, interferon-α2, and cholera toxin B subunit (Ki = 2.0 ± 0.3, 2.2 ± 0.2, and 3.6 ± 0.3 nM, respectively). Using [3H]LKEKK, we demonstrated the existence of a non-protein receptor common for thymosin-α1, interferon-α2, and cholera toxin B-subunit on donor blood T-lymphocytes.

Authors

Navolotskaya, E V; Zinchenko, D V; Zolotarev, Y A; Kolobov, A A; Lipkin, V M