Requirement of Cognate CD4(+) T-Cell Recognition for the Regulation of Allospecific CTL by Human CD4(+)CD127(−)CD25(+)FOXP3(+) Cells Generated in MLR

Although immunoregulation of alloreactive human CTLs has been described, the direct influence of CD4(+) Tregs on CD8(+) cytotoxicity and the interactive mechanisms have not been well clarified. Therefore, human CD4(+)CD127(−)CD25(+)FOXP3(+) Tregs were generated in MLR, immunoselected and their allos...

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Autores principales: Yu, Yuming, Miller, Joshua, Leventhal, Joseph R., Tambur, Anat R., Chandrasekaran, Dhivya, Levitsky, Josh, Luo, Xunrong, Mathew, James M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3142165/
https://www.ncbi.nlm.nih.gov/pubmed/21799858
http://dx.doi.org/10.1371/journal.pone.0022450
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author Yu, Yuming
Miller, Joshua
Leventhal, Joseph R.
Tambur, Anat R.
Chandrasekaran, Dhivya
Levitsky, Josh
Luo, Xunrong
Mathew, James M.
author_facet Yu, Yuming
Miller, Joshua
Leventhal, Joseph R.
Tambur, Anat R.
Chandrasekaran, Dhivya
Levitsky, Josh
Luo, Xunrong
Mathew, James M.
author_sort Yu, Yuming
collection PubMed
description Although immunoregulation of alloreactive human CTLs has been described, the direct influence of CD4(+) Tregs on CD8(+) cytotoxicity and the interactive mechanisms have not been well clarified. Therefore, human CD4(+)CD127(−)CD25(+)FOXP3(+) Tregs were generated in MLR, immunoselected and their allospecific regulatory functions and associated mechanisms were then tested using modified (51)Chromium release assays (Micro-CML), MLRs and CFSE-based multi-fluorochrome flow cytometry proliferation assays. It was observed that increased numbers of CD4(+)CD127(−)CD25(+)FOXP3(+) cells were generated after a 7 day MLR. After immunoselection for CD4(+)CD127(−)CD25(+) cells, they were designated as MLR-Tregs. When added as third component modulators, MLR-Tregs inhibited the alloreactive proliferation of autologous PBMC in a concentration dependent manner. The inhibition was quasi-antigen specific, in that the inhibition was non-specific at higher MLR-Treg modulator doses, but non-specificity disappeared with lower numbers at which specific inhibition was still significant. When tested in micro-CML assays CTL inhibition occurred with PBMC and purified CD8(+) responders. However, antigen specificity of CTL inhibition was observed only with unpurified PBMC responders and not with purified CD8(+) responders or even with CD8(+) responders plus Non-T “APC”. However, allospecificity of CTL regulation was restored when autologous purified CD4(+) T cells were added to the CD8(+) responders. Proliferation of CD8(+) cells was suppressed by MLR-Tregs in the presence or absence of IL-2. Inhibition by MLR-Tregs was mediated through down-regulation of intracellular perforin, granzyme B and membrane-bound CD25 molecules on the responding CD8(+) cells. Therefore, it was concluded that human CD4(+)CD127(−)CD25(+)FOXP3(+) MLR-Tregs down-regulate alloreactive cytotoxic responses. Regulatory allospecificity, however, requires the presence of cognate responding CD4(+) T cells. CD8(+) CTL regulatory mechanisms include impaired proliferation, reduced expression of cytolytic molecules and CD25(+) activation epitopes.
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spelling pubmed-31421652011-07-28 Requirement of Cognate CD4(+) T-Cell Recognition for the Regulation of Allospecific CTL by Human CD4(+)CD127(−)CD25(+)FOXP3(+) Cells Generated in MLR Yu, Yuming Miller, Joshua Leventhal, Joseph R. Tambur, Anat R. Chandrasekaran, Dhivya Levitsky, Josh Luo, Xunrong Mathew, James M. PLoS One Research Article Although immunoregulation of alloreactive human CTLs has been described, the direct influence of CD4(+) Tregs on CD8(+) cytotoxicity and the interactive mechanisms have not been well clarified. Therefore, human CD4(+)CD127(−)CD25(+)FOXP3(+) Tregs were generated in MLR, immunoselected and their allospecific regulatory functions and associated mechanisms were then tested using modified (51)Chromium release assays (Micro-CML), MLRs and CFSE-based multi-fluorochrome flow cytometry proliferation assays. It was observed that increased numbers of CD4(+)CD127(−)CD25(+)FOXP3(+) cells were generated after a 7 day MLR. After immunoselection for CD4(+)CD127(−)CD25(+) cells, they were designated as MLR-Tregs. When added as third component modulators, MLR-Tregs inhibited the alloreactive proliferation of autologous PBMC in a concentration dependent manner. The inhibition was quasi-antigen specific, in that the inhibition was non-specific at higher MLR-Treg modulator doses, but non-specificity disappeared with lower numbers at which specific inhibition was still significant. When tested in micro-CML assays CTL inhibition occurred with PBMC and purified CD8(+) responders. However, antigen specificity of CTL inhibition was observed only with unpurified PBMC responders and not with purified CD8(+) responders or even with CD8(+) responders plus Non-T “APC”. However, allospecificity of CTL regulation was restored when autologous purified CD4(+) T cells were added to the CD8(+) responders. Proliferation of CD8(+) cells was suppressed by MLR-Tregs in the presence or absence of IL-2. Inhibition by MLR-Tregs was mediated through down-regulation of intracellular perforin, granzyme B and membrane-bound CD25 molecules on the responding CD8(+) cells. Therefore, it was concluded that human CD4(+)CD127(−)CD25(+)FOXP3(+) MLR-Tregs down-regulate alloreactive cytotoxic responses. Regulatory allospecificity, however, requires the presence of cognate responding CD4(+) T cells. CD8(+) CTL regulatory mechanisms include impaired proliferation, reduced expression of cytolytic molecules and CD25(+) activation epitopes. Public Library of Science 2011-07-22 /pmc/articles/PMC3142165/ /pubmed/21799858 http://dx.doi.org/10.1371/journal.pone.0022450 Text en Yu et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Yu, Yuming
Miller, Joshua
Leventhal, Joseph R.
Tambur, Anat R.
Chandrasekaran, Dhivya
Levitsky, Josh
Luo, Xunrong
Mathew, James M.
Requirement of Cognate CD4(+) T-Cell Recognition for the Regulation of Allospecific CTL by Human CD4(+)CD127(−)CD25(+)FOXP3(+) Cells Generated in MLR
title Requirement of Cognate CD4(+) T-Cell Recognition for the Regulation of Allospecific CTL by Human CD4(+)CD127(−)CD25(+)FOXP3(+) Cells Generated in MLR
title_full Requirement of Cognate CD4(+) T-Cell Recognition for the Regulation of Allospecific CTL by Human CD4(+)CD127(−)CD25(+)FOXP3(+) Cells Generated in MLR
title_fullStr Requirement of Cognate CD4(+) T-Cell Recognition for the Regulation of Allospecific CTL by Human CD4(+)CD127(−)CD25(+)FOXP3(+) Cells Generated in MLR
title_full_unstemmed Requirement of Cognate CD4(+) T-Cell Recognition for the Regulation of Allospecific CTL by Human CD4(+)CD127(−)CD25(+)FOXP3(+) Cells Generated in MLR
title_short Requirement of Cognate CD4(+) T-Cell Recognition for the Regulation of Allospecific CTL by Human CD4(+)CD127(−)CD25(+)FOXP3(+) Cells Generated in MLR
title_sort requirement of cognate cd4(+) t-cell recognition for the regulation of allospecific ctl by human cd4(+)cd127(−)cd25(+)foxp3(+) cells generated in mlr
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3142165/
https://www.ncbi.nlm.nih.gov/pubmed/21799858
http://dx.doi.org/10.1371/journal.pone.0022450
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