Regulatory myeloid cells paralyze T cells through cell–cell transfer of the metabolite methylglyoxal | Zendy

Tobias Baumann | Zendy; Andreas Dunkel | Zendy; Christian Schmid | Zendy; Sabine Schmitt | Zendy; Michael Hiltensperger | Zendy; Kerstin Lohr | Zendy; Vibor Laketa | Zendy; Sainitin Donakonda | Zendy; Uwe Ahting | Zendy; Bettina LorenzDepiereux | Zendy; Jan E. Heil | Zendy; Johann Schredelseker | Zendy; Luca Simeoni | Zendy; Caroline Fecher | Zendy; Nina Körber | Zendy; Tanja Bauer | Zendy; Norbert Hüser | Zendy; Daniel Hartmann | Zendy; Melanie Laschinger | Zendy; Kilian Eyerich | Zendy; Stefanie Eyerich | Zendy; Martina Anton | Zendy; Matthew D. Streeter | Zendy; Tina Wang | Zendy; Burkhart Schraven | Zendy; David A. Spiegel | Zendy; Farhah F. Assaad | Zendy; Thomas Misgeld | Zendy; Hans Zischka | Zendy; Peter J. Murray | Zendy; Annkristin Heine | Zendy; Mathias Heikenwälder | Zendy; Thomas Korn | Zendy; Corinna Dawid | Zendy; Thomas Hofmann | Zendy; Percy A. Knolle | Zendy; Bastian Höchst | Zendy

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Regulatory myeloid cells paralyze T cells through cell–cell transfer of the metabolite methylglyoxal

Author(s) -

Tobias Baumann,

Andreas Dunkel,

Christian Schmid,

Sabine Schmitt,

Michael Hiltensperger,

Kerstin Lohr,

Vibor Laketa,

Sainitin Donakonda,

Uwe Ahting,

Bettina LorenzDepiereux,

Jan E. Heil,

Johann Schredelseker,

Luca Simeoni,

Caroline Fecher,

Nina Körber,

Tanja Bauer,

Norbert Hüser,

Daniel Hartmann,

Melanie Laschinger,

Kilian Eyerich,

Stefanie Eyerich,

Martina Anton,

Matthew D. Streeter,

Tina Wang,

Burkhart Schraven,

David A. Spiegel,

Farhah F. Assaad,

Thomas Misgeld,

Hans Zischka,

Peter J. Murray,

Annkristin Heine,

Mathias Heikenwälder,

Thomas Korn,

Corinna Dawid,

Thomas Hofmann,

Percy A. Knolle,

Bastian Höchst

Publication year - 2020

Publication title -

nature immunology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 9.074

H-Index - 388

eISSN - 1529-2916

pISSN - 1529-2908

DOI - 10.1038/s41590-020-0666-9

Subject(s) - immune system , methylglyoxal , cytotoxic t cell , myeloid derived suppressor cell , cancer cell , cancer research , adoptive cell transfer , t cell , cd8 , biology , tumor microenvironment , effector , microbiology and biotechnology , cancer , chemistry , immunology , suppressor , biochemistry , in vitro , genetics , enzyme

Regulatory myeloid immune cells, such as myeloid-derived suppressor cells (MDSCs), populate inflamed or cancerous tissue and block immune cell effector functions. The lack of mechanistic insight into MDSC suppressive activity and a marker for their identification has hampered attempts to overcome T cell inhibition and unleash anti-cancer immunity. Here, we report that human MDSCs were characterized by strongly reduced metabolism and conferred this compromised metabolic state to CD8 + T cells, thereby paralyzing their effector functions. We identified accumulation of the dicarbonyl radical methylglyoxal, generated by semicarbazide-sensitive amine oxidase, to cause the metabolic phenotype of MDSCs and MDSC-mediated paralysis of CD8 + T cells. In a murine cancer model, neutralization of dicarbonyl activity overcame MDSC-mediated T cell suppression and, together with checkpoint inhibition, improved the efficacy of cancer immune therapy. Our results identify the dicarbonyl methylglyoxal as a marker metabolite for MDSCs that mediates T cell paralysis and can serve as a target to improve cancer immune therapy.

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