Inhibition of in vitro and in vivo T cell responses by recombinant human Tim-1 extracellular domain proteins.

نویسندگان

  • Mehdi Mesri
  • Glennda Smithson
  • Ashwini Ghatpande
  • Andrei Chapoval
  • Suresh Shenoy
  • Ferenc Boldog
  • Craig Hackett
  • Carol E Pena
  • Catherine Burgess
  • Alison Bendele
  • Richard A Shimkets
  • Gary C Starling
چکیده

Members of the T cell, Ig domain and mucin domain (Tim) family of proteins have recently been implicated in the control of T cell-mediated immune responses. Tim-1 (HUGO designation HAVCR1) polymorphisms have been linked to the regulation of atopy in mice and humans, suggestive of a role in immune regulation. Tim-1 is expressed upon activation of T cells. In concert with the increased expression of Tim-1, a binding partner for the extracellular domain of Tim-1 (eTim-1) was induced on activated T cells, and mRNA expression data was consistent with the binding partner being Tim-4. We found that co-immobilized recombinant eTim-1 was able to inhibit T cell activation mediated by CD3 + CD28 mAb. eTim-1 mediated its inhibitory effects on proliferation by arresting cell cycle at G(0)/G(1) phase through regulation of cell cycle proteins. In vivo, administration of eTim-1 proteins led to a decrease in both ear (contact hypersensitivity to oxazolone) and joint (methylated BSA antigen-induced arthritis) swelling. The inhibitory activity of eTim-1 in the T(h)1-dependent models was evidence that eTim-1 is able to modulate T cell responses. Manipulation of the Tim-1 interaction with its binding partner on T cells may therefore provide a novel target for therapeutic intervention in T cell-mediated diseases.

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عنوان ژورنال:
  • International immunology

دوره 18 3  شماره 

صفحات  -

تاریخ انتشار 2006