Identification of natural RORγ ligands that regulate the development of lymphoid cells

Identification of natural RORγ ligands that regulate the development of lymphoid cells

Mice deficient in the nuclear hormone receptor RORγt have defective development of thymocytes, lymphoid organs, Th17 cells, and type 3 innate lymphoid cells. RORγt binds to oxysterols derived from cholesterol catabolism, but it is not clear whether these are its natural ligands. Here, we show that s...

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Veröffentlicht in:Cell Metabolism 2015-02, Vol.21 (2), p.286-297
Hauptverfasser: Santori, Fabio R, Huang, Pengxiang, van de Pavert, Serge A, Douglass, Eugene F, Leaver, David J, Haubrich, Brad A, Keber, Rok, Lorbek, Gregor, Konijn, Tanja, Rosales, Brittany N, Rozman, Damjana, Horvat, Simon, Rahier, Alain, Mebius, Reina E, Rastinejad, Fraydoon, Nes, W. David, Littman, Dan R
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container_end_page 297
container_issue 2
container_start_page 286
container_title Cell Metabolism
container_volume 21
creator Santori, Fabio R
Huang, Pengxiang
van de Pavert, Serge A
Douglass, Eugene F
Leaver, David J
Haubrich, Brad A
Keber, Rok
Lorbek, Gregor
Konijn, Tanja
Rosales, Brittany N
Rozman, Damjana
Horvat, Simon
Rahier, Alain
Mebius, Reina E
Rastinejad, Fraydoon
Nes, W. David
Littman, Dan R
description Mice deficient in the nuclear hormone receptor RORγt have defective development of thymocytes, lymphoid organs, Th17 cells, and type 3 innate lymphoid cells. RORγt binds to oxysterols derived from cholesterol catabolism, but it is not clear whether these are its natural ligands. Here, we show that sterol lipids are necessary and sufficient to drive RORγt-dependent transcription. We combined overexpression, RNAi, and genetic deletion of metabolic enzymes to study RORγ-dependent transcription. Our results are consistent with the RORγt ligand(s) being a cholesterol biosynthetic intermediate (CBI) downstream of lanosterol and upstream of zymosterol. Analysis of lipids bound to RORγ identified molecules with molecular weights consistent with CBIs. Furthermore, CBIs stabilized the RORγ ligand-binding domain and induced coactivator recruitment. Genetic deletion of metabolic enzymes upstream of the RORγt-ligand(s) affected the development of lymph nodes and Th17 cells. Our data suggest that CBIs play a role in lymphocyte development potentially through regulation of RORγt.
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title Identification of natural RORγ ligands that regulate the development of lymphoid cells
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