A Genomic DNA Reporter Screen Identifies Squalene Synthase Inhibitors That Act Cooperatively with Statins to Upregulate the Low-Density Lipoprotein Receptor

Kerr, Alastair G; Lcs., Tam; Hale, Ashley; Cioroch, Milena; Douglas, Gillian; Agkatsev, S; Hibbitt, Olivia; Mason, John; Holt‐Martyn, James P.; Bataille, Carole J. R.; Wynne, Graham M.; Channon, Keith M.; Russell, Angela J.; Wade‐Martins, Richard

doi:10.1124/jpet.116.239574

Cited by 5 publications

(5 citation statements)

References 36 publications

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“…The organic layer was dried over anhydrous Na 2 SO 4 , filtered and evaporated under vacuum, providing the desired compound 31 as a white solid in 92% yield. mp = 103-105 °C (coherent with literature 26 ). R f (cyclohexane/EtOAc 1:1 + 3% TEA) = 0.2.…”

Section: (E)-4-(2-(nn-dimethylamino)ethyloxy)stilbene (31)supporting

confidence: 87%

“…As in our previous investigation on onium-alkyloxy-stilbene based compounds, the pharmacological characterization of this new series of stilbenol ammoniumalkyl ethers, formally derived from the lead 1 by modification of the cationic head (4)(5)(6)(7)(8)(9)(10)(11)(12)(13)(14)(15)(16)(17) or rigidification of the O-N linker (18)(19)(20)(21)(22)(23)(24)(25)(26)(27), started from the evaluation of the α7-nAChR binding affinity by α-Bgtx displacement. This is indicative of competition for the same ACh orthosteric binding sites of this receptor and, in the development of our investigation, a useful guiding criterion in selecting candidates for functional study at both α7and α9α10-nAChR.…”

Section: Discussionmentioning

confidence: 99%

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From 2-Triethylammonium Ethyl Ether of 4-Stilbenol (MG624) to Selective Small-Molecule Antagonists of Human α9α10 Nicotinic Receptor by Modifications at the Ammonium Ethyl Residue

et al. 2022

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Nicotinic acetylcholine receptors containing α9 subunits (α9*-nAChRs) are potential druggable targets arousing great interest within the nicotinic receptor family with a special focus on a pain treatment alternative to opioids. Non-peptidic small molecules selectively acting as antagonists at this receptor subtype, especially without any effect on the closely related α7-nAChR, still remain an unattained goal, the achievement of which would provide invaluable tools to validate such an approach. Here, through relatively few directed modifications of the cationic head and the ethylene linker, we have converted the 2-triethylammonium ethyl ether of 4-stilbenol (MG624), a well-known antagonist for both α7 and α9* receptors, into a set of selective antagonists of human α9*-nAChR.Among these, the compound with cyclohexyldimetylammonium head (7) stands out for having no agonist or antagonist effect at α7-nAChR along with very low binding affinity at both α7 and α3β4 nicotinic receptor subtypes. Applied alone at high supra-micromolar concentrations, 7 and the other selective α9* antagonists behaved as partial agonists at α9*-nAChRs with a very short duration of the response, most likely due to very rapid block of the open channel, as revealed by the occurrence of rebound current once the application is stopped and the channel is disengaged. The small (nearly null in the case of 7) post-application residual activity of ACh control stimulation seems to be related to the slow recovery of the rebound current.

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Section: (E)-4-(2-(nn-dimethylamino)ethyloxy)stilbene (31)supporting

confidence: 87%

Section: Discussionmentioning

confidence: 99%

From 2-Triethylammonium Ethyl Ether of 4-Stilbenol (MG624) to Selective Small-Molecule Antagonists of Human α9α10 Nicotinic Receptor by Modifications at the Ammonium Ethyl Residue

et al. 2022

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“…This includes FDFT1 which encodes squalene synthase (SQS), a protein downstream HMGCR on the cholesterol biosynthesis pathway 30 . The therapeutic potential of SQS-inhibition has been explored in preclinical studies demonstrating cooperation between SQS-inhibitors and statins in achieving increased LDL-cholesterol clearance 35 . Despite our findings supporting the efficacy of FDFT1 , there was also evidence of putative adverse side-effects.…”

Section: Discussionmentioning

confidence: 99%

A factorial Mendelian randomization study to systematically prioritize genetic targets for the treatment of cardiovascular disease

Leyden

Gaunt

Richardson

2020

Preprint

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Importance New drugs which provide benefit alongside statin mono-therapy are warranted to reduce risk of cardiovascular disease. Objective To systematically evaluate the genetically predicted effects of 8,851 genes and cardiovascular disease risk factors using data from the UK Biobank and subsequently prioritize their potential to reduce cardiovascular disease in addition to statin therapy. Design, Setting, and Participants A factorial Mendelian randomization study using individual level data from the UK Biobank study. This population-based cohort includes a total of 502,602 individuals aged between 40 and 96 years old at baseline who were recruited between 2006 to 2010. Exposures Genetic variants robustly associated with the expression of target genes in whole blood (based on P<5x10-08) were used to construct gene scores using findings from the eQTLGen consortium (n=31,684). Main Outcomes and Measures Genetically predicted effects for each of the 8,851 genes were firstly evaluated with 5 measured outcomes from the UK Biobank in turn (body mass index, diastolic blood pressure, systolic blood pressure, low-density lipoproteins and triglycerides). Effects surviving multiple comparisons from this initial analysis were subsequently analyzed using factorial Mendelian randomization to evaluate evidence of an additive beneficial effect on cardiovascular disease risk compared to a HMGCR genetic score acting as a proxy for statin inhibition. Finally, a phenome-wide analysis was undertaken to evaluate predicted effects between prioritized targets and 570 outcomes in the UK Biobank to highlight potential adverse side-effects. Results 377 genetically predicted effects on cardiovascular disease risk factors were identified by Mendelian randomization (based on P<1.13x10-6). Of the 68 druggable genes, 20 candidate genes were predicted to lower cardiovascular disease risk in combination with statin treatment (P<7.35x10-4). Genes such as FDFT1 were predicted to have added benefit with statin therapy (OR=0.93; 95% CI, 0.91-0.95; P=2.21x10-10) but are unlikely to make safe targets due to their predicted effects on adverse side effects. In contrast, PRKCE provided evidence of a putative added benefit in combination with statins (OR=0.94; CI, 0.91-0.96; P=1.72x10-9) with no predicted adverse effects. Conclusions and Relevance Through the application of a systematic factorial Mendelian randomization analysis, we have prioritized (and deprioritized) potential drug targets predicted to reduce cardiovascular disease risk in addition to statin therapy.

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“…Here, the anti-DENV-2 effect of bLF was attenuated by the addition of rLDLR. The LDLR are responsible for regulating the extracellular cholesterol concentration; cholesterol-lowering drugs such as statin increase LDLR expression, thereby reducing the serum cholesterol level [ 32 ]. Thus, a comprehensive study on the role of LDLR in DENV-2 infection and a risk assessment study to determine the effect of serum cholesterol level and dengue infection may be required to investigate the impact of cholesterol–lowering drugs on DENV infection.…”

Section: Discussionmentioning

confidence: 99%

Bovine Lactoferrin Inhibits Dengue Virus Infectivity by Interacting with Heparan Sulfate, Low-Density Lipoprotein Receptor, and DC-SIGN

Chen

Fan

Lin

et al. 2017

IJMS

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Bovine lactoferrin (bLF) presents in milk and has been shown to inhibit several viral infections. Effective drugs are unavailable for the treatment of dengue virus (DENV) infection. In this study, we evaluated the antiviral effect of bLF against DENV infection in vivo and in vitro. Bovine LF significantly inhibited the infection of the four serotypes of DENV in Vero cells. In the time-of-drug addition test, DENV-2 infection was remarkably inhibited when bLF was added during or prior to the occurrence of virus attachment. We also revealed that bovine LF blocks binding between DENV-2 and the cellular membrane by interacting with heparan sulfate (HS), dendritic cell-specific intercellular adhesion molecule 3-grabbing non-integrin (DC-SIGN), and low-density lipoprotein receptors (LDLR). In addition, bLF inhibits DENV-2 infection and decreases morbidity in a suckling mouse challenge model. This study supports the finding that bLF may inhibit DENV infection by binding to the potential DENV receptors.

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A Genomic DNA Reporter Screen Identifies Squalene Synthase Inhibitors That Act Cooperatively with Statins to Upregulate the Low-Density Lipoprotein Receptor

Cited by 5 publications

References 36 publications

From 2-Triethylammonium Ethyl Ether of 4-Stilbenol (MG624) to Selective Small-Molecule Antagonists of Human α9α10 Nicotinic Receptor by Modifications at the Ammonium Ethyl Residue

From 2-Triethylammonium Ethyl Ether of 4-Stilbenol (MG624) to Selective Small-Molecule Antagonists of Human α9α10 Nicotinic Receptor by Modifications at the Ammonium Ethyl Residue

A factorial Mendelian randomization study to systematically prioritize genetic targets for the treatment of cardiovascular disease

Bovine Lactoferrin Inhibits Dengue Virus Infectivity by Interacting with Heparan Sulfate, Low-Density Lipoprotein Receptor, and DC-SIGN

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