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Unless otherwise stated all data on this page refer to the human proteins. Gene information is provided for human (Hs), mouse (Mm) and rat (Rn).
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Liver X and farnesoid X receptors (LXR and FXR, nomenclature as agreed by the NC-IUPHAR Subcommittee on Nuclear Hormone Receptors [1,7]) are members of a steroid analogue-activated nuclear receptor subfamily, which form heterodimers with members of the retinoid X receptor family. Endogenous ligands for LXRs include hydroxycholesterols (OHC), while FXRs appear to be activated by bile acids. In humans and primates, NR1H5P is a pseudogene. However, in other mammals, it encodes a functional nuclear hormone receptor that appears to be involved in cholesterol biosynthesis [8].
Farnesoid X receptor / NR1H4
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Farnesoid X receptor-β / NR1H5
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Liver X receptor-α / NR1H3
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Liver X receptor-β / NR1H2
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* Key recommended reading is highlighted with an asterisk
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1. Alexander SPH, Cidlowski JA, Kelly E, Mathie A, Peters JA, Veale EL, Armstrong JF, Faccenda E, Harding SD, Pawson AJ et al.. (2019) THE CONCISE GUIDE TO PHARMACOLOGY 2019/20: Nuclear hormone receptors. Br J Pharmacol, 176 Suppl 1: S229-S246. [PMID:31710718]
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Subcommittee members:
Donald P. McDonnell
Rachid Safi |
Database page citation (select format):
Concise Guide to PHARMACOLOGY citation:
Alexander SP, Cidlowski JA, Kelly E, Mathie A, Peters JA, Veale EL et al. (2021) THE CONCISE GUIDE TO PHARMACOLOGY 2021/22: Nuclear hormone receptors. Br J Pharmacol. 178 Suppl 1:S246-S263.
This work is licensed under a Creative Commons Attribution-ShareAlike 4.0 International License
T0901317 [11] and GW3965 [2] are synthetic agonists acting at both LXRα and LXRβ with less than 10-fold selectivity.