Targeting age‐specific changes in CD4(+) T cell metabolism ameliorates alloimmune responses and prolongs graft survival

Age impacts alloimmunity. Effects of aging on T‐cell metabolism and the potential to interfere with immunosuppressants have not been explored yet. Here, we dissected metabolic pathways of CD4(+) and CD8(+) T cells in aging and offer novel immunosuppressive targets. Upon activation, CD4(+) T cells fr...

Descripción completa

Detalles Bibliográficos
Autores principales: Nian, Yeqi, Iske, Jasper, Maenosono, Ryoichi, Minami, Koichiro, Heinbokel, Timm, Quante, Markus, Liu, Yang, Azuma, Haruhito, Yang, Jinrui, Abdi, Reza, Zhou, Hao, Elkhal, Abdallah, Tullius, Stefan G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Original Papers
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7884034/
https://www.ncbi.nlm.nih.gov/pubmed/33497523
http://dx.doi.org/10.1111/acel.13299
_version_ 1783651329293418496
author Nian, Yeqi
Iske, Jasper
Maenosono, Ryoichi
Minami, Koichiro
Heinbokel, Timm
Quante, Markus
Liu, Yang
Azuma, Haruhito
Yang, Jinrui
Abdi, Reza
Zhou, Hao
Elkhal, Abdallah
Tullius, Stefan G.
author_facet Nian, Yeqi
Iske, Jasper
Maenosono, Ryoichi
Minami, Koichiro
Heinbokel, Timm
Quante, Markus
Liu, Yang
Azuma, Haruhito
Yang, Jinrui
Abdi, Reza
Zhou, Hao
Elkhal, Abdallah
Tullius, Stefan G.
author_sort Nian, Yeqi
collection PubMed
description Age impacts alloimmunity. Effects of aging on T‐cell metabolism and the potential to interfere with immunosuppressants have not been explored yet. Here, we dissected metabolic pathways of CD4(+) and CD8(+) T cells in aging and offer novel immunosuppressive targets. Upon activation, CD4(+) T cells from old mice failed to exhibit adequate metabolic reprogramming resulting into compromised metabolic pathways, including oxidative phosphorylation (OXPHOS) and glycolysis. Comparable results were also observed in elderly human patients. Although glutaminolysis remained the dominant and age‐independent source of mitochondria for activated CD4(+) T cells, old but not young CD4(+) T cells relied heavily on glutaminolysis. Treating young and old murine and human CD4(+) T cells with 6‐diazo‐5‐oxo‐l‐norleucine (DON), a glutaminolysis inhibitor resulted in significantly reduced IFN‐γ production and compromised proliferative capacities specifically of old CD4(+) T cells. Of translational relevance, old and young mice that had been transplanted with fully mismatched skin grafts and treated with DON demonstrated dampened Th1‐ and Th17‐driven alloimmune responses. Moreover, DON diminished cytokine production and proliferation of old CD4(+) T cells in vivo leading to a significantly prolonged allograft survival specifically in old recipients. Graft prolongation in young animals, in contrast, was only achieved when DON was applied in combination with an inhibition of glycolysis (2‐deoxy‐d‐glucose, 2‐DG) and OXPHOS (metformin), two alternative metabolic pathways. Notably, metabolic treatment had not been linked to toxicities. Remarkably, immunosuppressive capacities of DON were specific to CD4(+) T cells as adoptively transferred young CD4(+) T cells prevented immunosuppressive capacities of DON on allograft survival in old recipients. Depletion of CD8(+) T cells did not alter transplant outcomes in either young or old recipients. Taken together, our data introduce an age‐specific metabolic reprogramming of CD4(+) T cells. Targeting those pathways offers novel and age‐specific approaches for immunosuppression.
format Online
Article
Text
id pubmed-7884034
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher John Wiley and Sons Inc.
record_format MEDLINE/PubMed
spelling pubmed-78840342021-02-19 Targeting age‐specific changes in CD4(+) T cell metabolism ameliorates alloimmune responses and prolongs graft survival Nian, Yeqi Iske, Jasper Maenosono, Ryoichi Minami, Koichiro Heinbokel, Timm Quante, Markus Liu, Yang Azuma, Haruhito Yang, Jinrui Abdi, Reza Zhou, Hao Elkhal, Abdallah Tullius, Stefan G. Aging Cell Original Papers Age impacts alloimmunity. Effects of aging on T‐cell metabolism and the potential to interfere with immunosuppressants have not been explored yet. Here, we dissected metabolic pathways of CD4(+) and CD8(+) T cells in aging and offer novel immunosuppressive targets. Upon activation, CD4(+) T cells from old mice failed to exhibit adequate metabolic reprogramming resulting into compromised metabolic pathways, including oxidative phosphorylation (OXPHOS) and glycolysis. Comparable results were also observed in elderly human patients. Although glutaminolysis remained the dominant and age‐independent source of mitochondria for activated CD4(+) T cells, old but not young CD4(+) T cells relied heavily on glutaminolysis. Treating young and old murine and human CD4(+) T cells with 6‐diazo‐5‐oxo‐l‐norleucine (DON), a glutaminolysis inhibitor resulted in significantly reduced IFN‐γ production and compromised proliferative capacities specifically of old CD4(+) T cells. Of translational relevance, old and young mice that had been transplanted with fully mismatched skin grafts and treated with DON demonstrated dampened Th1‐ and Th17‐driven alloimmune responses. Moreover, DON diminished cytokine production and proliferation of old CD4(+) T cells in vivo leading to a significantly prolonged allograft survival specifically in old recipients. Graft prolongation in young animals, in contrast, was only achieved when DON was applied in combination with an inhibition of glycolysis (2‐deoxy‐d‐glucose, 2‐DG) and OXPHOS (metformin), two alternative metabolic pathways. Notably, metabolic treatment had not been linked to toxicities. Remarkably, immunosuppressive capacities of DON were specific to CD4(+) T cells as adoptively transferred young CD4(+) T cells prevented immunosuppressive capacities of DON on allograft survival in old recipients. Depletion of CD8(+) T cells did not alter transplant outcomes in either young or old recipients. Taken together, our data introduce an age‐specific metabolic reprogramming of CD4(+) T cells. Targeting those pathways offers novel and age‐specific approaches for immunosuppression. John Wiley and Sons Inc. 2021-01-26 2021-02 /pmc/articles/PMC7884034/ /pubmed/33497523 http://dx.doi.org/10.1111/acel.13299 Text en © 2021 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Papers
Nian, Yeqi
Iske, Jasper
Maenosono, Ryoichi
Minami, Koichiro
Heinbokel, Timm
Quante, Markus
Liu, Yang
Azuma, Haruhito
Yang, Jinrui
Abdi, Reza
Zhou, Hao
Elkhal, Abdallah
Tullius, Stefan G.
Targeting age‐specific changes in CD4(+) T cell metabolism ameliorates alloimmune responses and prolongs graft survival
title Targeting age‐specific changes in CD4(+) T cell metabolism ameliorates alloimmune responses and prolongs graft survival
title_full Targeting age‐specific changes in CD4(+) T cell metabolism ameliorates alloimmune responses and prolongs graft survival
title_fullStr Targeting age‐specific changes in CD4(+) T cell metabolism ameliorates alloimmune responses and prolongs graft survival
title_full_unstemmed Targeting age‐specific changes in CD4(+) T cell metabolism ameliorates alloimmune responses and prolongs graft survival
title_short Targeting age‐specific changes in CD4(+) T cell metabolism ameliorates alloimmune responses and prolongs graft survival
title_sort targeting age‐specific changes in cd4(+) t cell metabolism ameliorates alloimmune responses and prolongs graft survival
topic Original Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7884034/
https://www.ncbi.nlm.nih.gov/pubmed/33497523
http://dx.doi.org/10.1111/acel.13299
work_keys_str_mv AT nianyeqi targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT iskejasper targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT maenosonoryoichi targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT minamikoichiro targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT heinbokeltimm targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT quantemarkus targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT liuyang targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT azumaharuhito targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT yangjinrui targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT abdireza targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT zhouhao targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT elkhalabdallah targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival
AT tulliusstefang targetingagespecificchangesincd4tcellmetabolismamelioratesalloimmuneresponsesandprolongsgraftsurvival

Ejemplares similares