IL-4 is an essential factor for the IgE synthesis induced in vitro by human T cell clones and their supernatants

The property of 109 CD4+ T cell clones (TCC) to induce IgE synthesis in vitro in human B cells was compared with their ability to produce IL-2, IL-4, and IFN-gamma in their supernatants (SUP) after 24-h stimulation with PHA. A significant positive correlation was found between the property of TCC to...

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Veröffentlicht in:	The Journal of immunology (1950) 1988-06, Vol.140 (12), p.4193-4198
Hauptverfasser:	Del Prete, G, Maggi, E, Parronchi, P, Chretien, I, Tiri, A, Macchia, D, Ricci, M, Banchereau, J, De Vries, J, Romagnani, S
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Sprache:	eng
Schlagworte:	Adult Analysis of the immune response. Humoral and cellular immunity Animals Antibodies, Monoclonal - physiology B-Lymphocytes - metabolism Biological and medical sciences Cell-Free System Clone Cells - immunology Fundamental and applied biological sciences. Psychology Fundamental immunology Humans Immunobiology Immunoglobulin E - biosynthesis Immunoglobulin E - physiology Immunosuppressive Agents - physiology Interleukin-4 Interleukins - immunology Interleukins - physiology Lymphokines - biosynthesis Lymphokines - physiology Lymphokines, interleukins ( function, expression) Prostatic Secretory Proteins Rabbits Regulatory factors and their cellular receptors Subcellular Fractions T-Lymphocytes, Helper-Inducer - immunology
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container_end_page	4198
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container_title	The Journal of immunology (1950)
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creator	Del Prete, G Maggi, E Parronchi, P Chretien, I Tiri, A Macchia, D Ricci, M Banchereau, J De Vries, J Romagnani, S
description	The property of 109 CD4+ T cell clones (TCC) to induce IgE synthesis in vitro in human B cells was compared with their ability to produce IL-2, IL-4, and IFN-gamma in their supernatants (SUP) after 24-h stimulation with PHA. A significant positive correlation was found between the property of TCC to induce or enhance spontaneous IgE synthesis and their ability to release IL-4. In contrast, there was an inverse relationship between the IgE helper activity of TCC and their ability to release IFN-gamma, whereas no statistical correlation between the property to induce IgE synthesis and to produce IL-2 was observed. The ability of PHA-SUP from 71 CD4+ TCC to induce IgE synthesis in B cells was also investigated. Twenty-nine SUP (all derived from TCC active on IgE synthesis) induced production of substantial amounts of IgE in target B cells. There was a correlation between the amount of IgE synthesized by B cells in response to these SUP and their IL-4 content. An even higher correlation was found between the IgE synthesis induced by these SUP and the ratio between the amount of IL-4 and IFN-gamma present in the same SUP. Like IL-4-containing SUP, rIL-4 also showed the ability to induce IgE production in B cells from both atopic and nonatopic donors. The addition to B cell cultures of anti-IL-4 antibody virtually abolished not only the IgE synthesis induced by rIL-4, but also that stimulated by TCC and their SUP. In contrast, the IgG synthesis induced by TCC SUP was not or only slightly inhibited by the anti-IL-4 antibody. These data indicate that IL-4 is an essential mediator for the IgE synthesis induced in vitro by human TCC and their SUP in the absence of a polyclonal activator, whereas IFN-gamma seems to exert a negative regulatory effect on the production of IgE.
doi_str_mv	10.4049/jimmunol.140.12.4193
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A significant positive correlation was found between the property of TCC to induce or enhance spontaneous IgE synthesis and their ability to release IL-4. In contrast, there was an inverse relationship between the IgE helper activity of TCC and their ability to release IFN-gamma, whereas no statistical correlation between the property to induce IgE synthesis and to produce IL-2 was observed. The ability of PHA-SUP from 71 CD4+ TCC to induce IgE synthesis in B cells was also investigated. Twenty-nine SUP (all derived from TCC active on IgE synthesis) induced production of substantial amounts of IgE in target B cells. There was a correlation between the amount of IgE synthesized by B cells in response to these SUP and their IL-4 content. An even higher correlation was found between the IgE synthesis induced by these SUP and the ratio between the amount of IL-4 and IFN-gamma present in the same SUP. Like IL-4-containing SUP, rIL-4 also showed the ability to induce IgE production in B cells from both atopic and nonatopic donors. The addition to B cell cultures of anti-IL-4 antibody virtually abolished not only the IgE synthesis induced by rIL-4, but also that stimulated by TCC and their SUP. In contrast, the IgG synthesis induced by TCC SUP was not or only slightly inhibited by the anti-IL-4 antibody. 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A significant positive correlation was found between the property of TCC to induce or enhance spontaneous IgE synthesis and their ability to release IL-4. In contrast, there was an inverse relationship between the IgE helper activity of TCC and their ability to release IFN-gamma, whereas no statistical correlation between the property to induce IgE synthesis and to produce IL-2 was observed. The ability of PHA-SUP from 71 CD4+ TCC to induce IgE synthesis in B cells was also investigated. Twenty-nine SUP (all derived from TCC active on IgE synthesis) induced production of substantial amounts of IgE in target B cells. There was a correlation between the amount of IgE synthesized by B cells in response to these SUP and their IL-4 content. An even higher correlation was found between the IgE synthesis induced by these SUP and the ratio between the amount of IL-4 and IFN-gamma present in the same SUP. Like IL-4-containing SUP, rIL-4 also showed the ability to induce IgE production in B cells from both atopic and nonatopic donors. The addition to B cell cultures of anti-IL-4 antibody virtually abolished not only the IgE synthesis induced by rIL-4, but also that stimulated by TCC and their SUP. In contrast, the IgG synthesis induced by TCC SUP was not or only slightly inhibited by the anti-IL-4 antibody. These data indicate that IL-4 is an essential mediator for the IgE synthesis induced in vitro by human TCC and their SUP in the absence of a polyclonal activator, whereas IFN-gamma seems to exert a negative regulatory effect on the production of IgE.</description><subject>Adult</subject><subject>Analysis of the immune response. 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A significant positive correlation was found between the property of TCC to induce or enhance spontaneous IgE synthesis and their ability to release IL-4. In contrast, there was an inverse relationship between the IgE helper activity of TCC and their ability to release IFN-gamma, whereas no statistical correlation between the property to induce IgE synthesis and to produce IL-2 was observed. The ability of PHA-SUP from 71 CD4+ TCC to induce IgE synthesis in B cells was also investigated. Twenty-nine SUP (all derived from TCC active on IgE synthesis) induced production of substantial amounts of IgE in target B cells. There was a correlation between the amount of IgE synthesized by B cells in response to these SUP and their IL-4 content. An even higher correlation was found between the IgE synthesis induced by these SUP and the ratio between the amount of IL-4 and IFN-gamma present in the same SUP. Like IL-4-containing SUP, rIL-4 also showed the ability to induce IgE production in B cells from both atopic and nonatopic donors. The addition to B cell cultures of anti-IL-4 antibody virtually abolished not only the IgE synthesis induced by rIL-4, but also that stimulated by TCC and their SUP. In contrast, the IgG synthesis induced by TCC SUP was not or only slightly inhibited by the anti-IL-4 antibody. These data indicate that IL-4 is an essential mediator for the IgE synthesis induced in vitro by human TCC and their SUP in the absence of a polyclonal activator, whereas IFN-gamma seems to exert a negative regulatory effect on the production of IgE.</abstract><cop>Bethesda, MD</cop><pub>Am Assoc Immnol</pub><pmid>2967330</pmid><doi>10.4049/jimmunol.140.12.4193</doi><tpages>6</tpages><oa>free_for_read</oa></addata></record>
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subjects	Adult Analysis of the immune response. Humoral and cellular immunity Animals Antibodies, Monoclonal - physiology B-Lymphocytes - metabolism Biological and medical sciences Cell-Free System Clone Cells - immunology Fundamental and applied biological sciences. Psychology Fundamental immunology Humans Immunobiology Immunoglobulin E - biosynthesis Immunoglobulin E - physiology Immunosuppressive Agents - physiology Interleukin-4 Interleukins - immunology Interleukins - physiology Lymphokines - biosynthesis Lymphokines - physiology Lymphokines, interleukins ( function, expression) Prostatic Secretory Proteins Rabbits Regulatory factors and their cellular receptors Subcellular Fractions T-Lymphocytes, Helper-Inducer - immunology
title	IL-4 is an essential factor for the IgE synthesis induced in vitro by human T cell clones and their supernatants
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