Methyl fluorosulfonyldifluoroacetate (MFSDA): An Underutilised Reagent for Trifluoromethylation

Clarke, Sarah L.; McGlacken, Gerard P.

doi:10.1002/chem.201602511

Cited by 53 publications

(25 citation statements)

References 109 publications

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“…Methyl 2,2-difluoro-2-(fluorosulfonyl) acetate (MFSDA) was used as the reagent for the trifluoromethylation of pyridone 14 to give novel pyridone 8 3031. Before returning to in depth biological studies, the prepared pyridone 8 was deemed not toxic in the two cell lines tested: Hek293a-GHS-R1a and mHypoE-N38 using the resazurin toxicity assay (for details, see SI, Figure S1).…”

Section: Resultsmentioning

confidence: 99%

A Novel Non-Peptidic Agonist of the Ghrelin Receptor with Orexigenic Activity In vivo

Pastor-Cavada

Pardo

Kandil

et al. 2016

Sci Rep

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Loss of appetite in the medically ill and ageing populations is a major health problem and a significant symptom in cachexia syndromes, which is the loss of muscle and fat mass. Ghrelin is a gut-derived hormone which can stimulate appetite. Herein we describe a novel, simple, non-peptidic, 2-pyridone which acts as a selective agonist for the ghrelin receptor (GHS-R1a). The small 2-pyridone demonstrated clear agonistic activity in both transfected human cells and mouse hypothalamic cells with endogenous GHS-R1a receptor expression. In vivo tests with the hit compound showed significant increased food intake following peripheral administration, which highlights the potent orexigenic effect of this novel GHS-R1a receptor ligand.

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Section: Resultsmentioning

confidence: 99%

A Novel Non-Peptidic Agonist of the Ghrelin Receptor with Orexigenic Activity In vivo

Pastor-Cavada

Pardo

Kandil

et al. 2016

Sci Rep

Self Cite

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“…Other compounds such as the polyphenol naringin, the gamma-secretase inhibitor “semagacestat,” and biosynthetic intermediates of teaghrelins and emoghrelin have also shown a potential as GHS-R1a agonists [ 29 , 30 , 31 ]. Recently, we also demonstrated a novel, non-peptidic, 2-pyridone bears a crucial trifluoromethyl group [ 32 , 33 ] at the 3-position, which demonstrated a selective GHS-R1a agonist potential in vitro and promised modulation of food intake in vivo [ 22 ]. However, further studies are warranted to identify novel selective GHS-R1a-targeting small molecule agonists with increased potency and selectivity as well as improved pharmacokinetics and bioavailability.…”

Section: Introductionmentioning

confidence: 99%

Quinolones Modulate Ghrelin Receptor Signaling: Potential for a Novel Small Molecule Scaffold in the Treatment of Cachexia

Torres‐Fuentes

Pastor-Cavada

Cano

et al. 2018

IJMS

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Cachexia is a metabolic wasting disorder characterized by progressive weight loss, muscle atrophy, fatigue, weakness, and appetite loss. Cachexia is associated with almost all major chronic illnesses including cancer, heart failure, obstructive pulmonary disease, and kidney disease and significantly impedes treatment outcome and therapy tolerance, reducing physical function and increasing mortality. Current cachexia treatments are limited and new pharmacological strategies are needed. Agonists for the growth hormone secretagogue (GHS-R1a), or ghrelin receptor, prospectively regulate the central regulation of appetite and growth hormone secretion, and therefore have tremendous potential as cachexia therapeutics. Non-peptide GHS-R1a agonists are of particular interest, especially given the high gastrointestinal degradation of peptide-based structures, including that of the endogenous ligand, ghrelin, which has a half-life of only 30 min. However, few compounds have been reported in the literature as non-peptide GHS-R1a agonists. In this paper, we investigate the in vitro potential of quinolone compounds to modulate the GHS-R1a in both transfected human cells and mouse hypothalamic cells. These chemically synthesized compounds demonstrate a promising potential as GHS-R1a agonists, shown by an increased intracellular calcium influx. Further studies are now warranted to substantiate and exploit the potential of these novel quinolone-based compounds as orexigenic therapeutics in conditions of cachexia and other metabolic and eating disorders.

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“…To explore this, we have carried out aD FT-based conformational Scheme3.Putative mechanism for the trifluoromethylationo f18. [17][18][19][20][21] Scheme4.Synthesis of iodomuscimol 5.a)33% HBrinAcOH,608C, 17 h, 19 %. bond approximately perpendicular to the aromatic ring, very similar to the X-ray structuref or 3 (see Computational Details in the Supporting Information).…”

Section: Gaba Receptor Agonist Assaysmentioning

confidence: 99%

The Synthesis and Evaluation of Fluoro‐, Trifluoromethyl‐, and Iodomuscimols as GABA Agonists

Manan

Cordes

Slawin

et al. 2017

Chemistry A European J

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Halogenated analogues of the neurotoxic alkaloid muscimol were prepared with fluorine, iodine or trifluoromethyl at the 4 position of the isoxazole ring system. These compounds were investigated as agonists for GABA receptors. Only the C-4 fluorine-containing analogue proved to be an active compound in these assays. The fluoro analogue was less active than muscimol, however it showed differential activity between synaptic (α β γ ) and extrasynaptic (α β γ) GABA receptors, having a similar potency to the neurotransmitter GABA for the extrasynaptic (α β γ) receptor.

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Methyl fluorosulfonyldifluoroacetate (MFSDA): An Underutilised Reagent for Trifluoromethylation

Cited by 53 publications

References 109 publications

A Novel Non-Peptidic Agonist of the Ghrelin Receptor with Orexigenic Activity In vivo

A Novel Non-Peptidic Agonist of the Ghrelin Receptor with Orexigenic Activity In vivo

Quinolones Modulate Ghrelin Receptor Signaling: Potential for a Novel Small Molecule Scaffold in the Treatment of Cachexia

The Synthesis and Evaluation of Fluoro‐, Trifluoromethyl‐, and Iodomuscimols as GABA Agonists

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