Disulfide-Trapping Identifies a New, Effective Chemical Probe for Activating the Nuclear Receptor Human LRH-1 (NR5A2)

Cortez, Felipe de Jesus; Suzawa, Miyuki; Irvy, Sam; Bruning, John M.; Sablin, Elena P.; Jacobson, Matthew P.; Fletterick, Robert J.; Ingraham, Holly A.; England, Pamela M.

doi:10.1371/journal.pone.0159316

Cited by 11 publications

(12 citation statements)

References 21 publications

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“…To ascertain if ligand binding is necessary for hLRH-1-mediated rescue, we next attempted to salvage organoid viability with the well-characterized ligand-binding-defective variant of hLRH-1 (PM; Fig. 3a ) 26 , 27 . Bulky hydrophobic residues were modeled in the binding pocket to impede ligand uptake without effecting protein integrity, as previously demonstrated in cultured cell lines 26 .…”

Section: Resultsmentioning

confidence: 99%

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LRH-1 mitigates intestinal inflammatory disease by maintaining epithelial homeostasis and cell survival

et al. 2018

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Epithelial dysfunction and crypt destruction are defining features of inflammatory bowel disease (IBD). However, current IBD therapies targeting epithelial dysfunction are lacking. The nuclear receptor LRH-1 (NR5A2) is expressed in intestinal epithelium and thought to contribute to epithelial renewal. Here we show that LRH-1 maintains intestinal epithelial health and protects against inflammatory damage. Knocking out LRH-1 in murine intestinal organoids reduces Notch signaling, increases crypt cell death, distorts the cellular composition of the epithelium, and weakens the epithelial barrier. Human LRH-1 (hLRH-1) rescues epithelial integrity and when overexpressed, mitigates inflammatory damage in murine and human intestinal organoids, including those derived from IBD patients. Finally, hLRH-1 greatly reduces disease severity in T-cell-mediated murine colitis. Together with the failure of a ligand-incompetent hLRH-1 mutant to protect against TNFα-damage, these findings provide compelling evidence that hLRH-1 mediates epithelial homeostasis and is an attractive target for intestinal disease.

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Section: Resultsmentioning

confidence: 99%

“…Indeed, the human PM variant is stably expressed in intestinal organoids (Fig. 3c , right), and despite the fact that the hPM retains modest transcriptional activity 26 , 27 , it failed to rescue TNFα-induced cell death in Lrh1 IEC-KO intestinal organoids (Fig. 3f , light blue bar).…”

Section: Resultsmentioning

confidence: 99%

LRH-1 mitigates intestinal inflammatory disease by maintaining epithelial homeostasis and cell survival

et al. 2018

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“…Computational modeling suggested a structure of the small molecule complex with NR5A2 and cellular assays were used to find an analog with no sulfur atom. This analog is termed PME8 and is a good activator, with A dissociation constant of 5 μM …”

Section: Part 1 Exploratory Chemistry Matched To Expansive Biologymentioning

confidence: 99%

“…This analog is termed PME8 and is a good activator, with A dissociation constant of 5 μM. 10 This technical approach could be used with protein complexes of NR5A2 such as with DAX1 peptide or β-catenin and suggest that with further development this chemical probes that are specific antagonists.…”

Section: Part 1 Exploratory Chemistry Matched To Expansive Biologymentioning

confidence: 99%

NR5A2 discovering compounds that block tumor growth in PDAC

Fletterick¹

2017

Journal of Surgical Oncology

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Pancreatic Cancers depend on driver molecules, oncogene proteins such as RAS. NR5A2 protein is a transcription factor and either activates or inhibits transcription through actions at hundreds of enhancers. It has unusual properties with effects appearing in multiple signaling networks. NR5A2 is a pluripotency reprogramming factor in the class nuclear receptor. Its controlling hormone is PIP3. Experiments suggest NR5A2 activation drives PDAC and inhibitors blunt cancer cell proliferation.

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“…Towards this end, several laboratories have madesignificant advances in developing potent LRH-1 modulators. [13][14][15] Despite these advances, rational design has been difficult, in partbecause of the large, highly hydrophobic LRH-1 ligand binding pocket. Due to this lipophilicity and a scarcity of sites for anchoring polar interactions, even highly similar compounds can bind unpredictably, 15,16 further complicating systematic agonist development.…”

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confidence: 99%

Development of a new class of liver receptor homolog-1 (LRH-1) agonists by photoredox conjugate addition

Cornelison

Cato

Johnson

et al. 2020

Preprint

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Article history:Received Revised Accepted Available online LRH-1 is a nuclear receptor that regulates lipid metabolism and homeostasis, making it an attractive target for the treatment of diabetes and non-alcoholic fatty liver disease. Building on recent structural information about ligand binding from our labs, we have designed a series of new LRH-1 agonists that further engage LRH-1 through added polar interactions. While the current synthetic approach to this scaffold has, in large part, allowed for decoration of the agonist core, significant variation of the bridgehead substituent is mechanistically precluded. We have developed a new synthetic approach to overcome this limitation, identified that bridgehead substitution is necessary for LRH-1 activation, and described an alternative class of bridgehead substituents for effective LRH-1 agonist development. We determined the crystal structure of LRH-1 bound to a bridgehead-modified compound, revealing a promising opportunity to target novel regions of the ligand-binding pocket to alter LRH-1 target gene expression..

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Disulfide-Trapping Identifies a New, Effective Chemical Probe for Activating the Nuclear Receptor Human LRH-1 (NR5A2)

Cited by 11 publications

References 21 publications

LRH-1 mitigates intestinal inflammatory disease by maintaining epithelial homeostasis and cell survival

LRH-1 mitigates intestinal inflammatory disease by maintaining epithelial homeostasis and cell survival

NR5A2 discovering compounds that block tumor growth in PDAC

Development of a new class of liver receptor homolog-1 (LRH-1) agonists by photoredox conjugate addition

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