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In vivo restoration of T cell functions by human IL-1β or its 163-171 nonapeptide in immunodepressed mice

TitoloIn vivo restoration of T cell functions by human IL-1β or its 163-171 nonapeptide in immunodepressed mice
Tipo di pubblicazioneArticolo su Rivista peer-reviewed
Anno di Pubblicazione1988
AutoriFrasca, D., Boraschi D., Baschieri Selene, Bossu P., Tagliabue A., Adorini L., and Doria G.
RivistaJournal of Immunology
Volume141
Paginazione2651-2655
ISSN00221767
Parole chiaveAdjuvants, Aging, animal, animal experiment, Dose-Response Relationship, Helper-Inducer, human, immune deficiency, Immunologic, Immunologic Deficiency Syndromes, Immunomodulation, interleukin 1beta, interleukin 1beta[163-171], interleukin 2, Interleukin-1, Interleukin-2, male, Mice, mouse, Non-U.S. Gov't, nonapeptide, Peptide Fragments, priority journal, Recombinant Proteins, Spleen, spleen cell, Support, T lymphocyte, T-Lymphocytes, Whole-Body Irradiation
Abstract

The immunorestorative capacities of human (hu) IL-1β or its synthetic fragment 163-171 (VQGEESNDK) were assessed in vivo in mice immunodepressed by aging, sublethal irradiation, or both. Subcutaneous administrtion of hu rIL-1β into immunodepressed animals immediately after carrier (horse red blood cells, HRBC) priming could restore to normal levels Th cell activity. This was measured as the ability of spleen cells from HRBC-primed mice to induce a hapten-specific antibody response in spleen cells from nonimmune mice in vitro stimulated with the hapten-carrier conjugate TNP-HRBC. In parallel, the ability of spleen cells from hu rIL-1β-treated immunodepressed animals to produce T cell growth factor activity upon in vitro mitogen stimulation was also increased significantly as compared to that of untreated mice and approached that of immunocompetent controls. The immunorestorative activity of hu rIL-1β on Th cell activity and T cell growth factor production could be mimicked by the synthetic nonapeptide 163-171 which, at the doses used, produced in most instances even greater effects than the whole protein. Although the optimal immunorestorative doses of the 163-171 peptide were several orders of magnitude higher than those of hu rIL-1β, the complete lack of IL-1-like inflammatory and toxic effects suggests that the synthetic hu IL-1β fragment may be successfully used as immunomodulating agent in the therapy of T cell immunodeficiencies.

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cited By 32

URLhttps://www.scopus.com/inward/record.uri?eid=2-s2.0-0023790536&partnerID=40&md5=841a596268bb9b96a8c5689414e1c4d3
Citation KeyFrasca19882651