Flow synthesis of a versatile fructosamine mimic and quenching studies of a fructose transport probe

Plutschack, Matthew B.; McQuade, D. Tyler; Valenti, Giulio; Seeberger, Peter H.

doi:10.3762/bjoc.9.238

Cited by 8 publications

(5 citation statements)

References 31 publications

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“…Plutschack et al [57] applied the TD in a flow-based approach to contract a six-membered ring to a five-membered ring (Scheme 19). This was achieved using an acidic resin in which the educt, glucosamine hydrochloride, was passed over.…”

Section: Scheme 16mentioning

confidence: 99%

“…Comparing these results with the previously used batch production, a ~ 64-fold increase in the throughput rate and a decrease in reaction time from 3 days to 1 day was observed. This modification of the TD helps to shift the paradigm of synthesis away from the one-pot-approaches to dynamic flow-approaches, which are not only easier to control, but can also lead to shorter reaction time due to higher throughput [57].…”

Section: Scheme 16mentioning

confidence: 99%

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The synthetic versatility of the Tiffeneau–Demjanov chemistry in homologation tactics

et al. 2019

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The Tiffeneau–Demjanov rearrangement can be regarded as an interesting alternative to the more common semi-pinacol transposition. It is usually employed for ring extension but, under specific conditions, it can also be used for ring contraction. Compared to other techniques, such as the Demjanov rearrangement or homologations with diazo compounds, the Tiffeneau–Demjanov pathway presents attractive features including high yielding and selective processes. Ring enlargements follow very strict and simple rules, such as the movement of the less substituted carbon and retention of the configuration. The rearrangement process is mainly affected by steric factors, due to presence of neighbouring groups, rather than electronic ones. The ring contraction may be achieved positioning the amine within the ring, thus achieving a high level of control. Unfortunately, applications of the reaction in modern homologation chemistry are rare; therefore, the aim of the review is re-proposing to the synthetic community the versatility of this venerable reaction and thus, spurring its employment for tackling challenging homologations processes. Graphic abstract

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Section: Scheme 16mentioning

confidence: 99%

Section: Scheme 16mentioning

confidence: 99%

The synthetic versatility of the Tiffeneau–Demjanov chemistry in homologation tactics

et al. 2019

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“…The next generation of radiotracer probes was derived from 2,5‐anhydro‐ d ‐mannitol, on the basis of its high affinity towards Glut 5. 1‐[ 18 F]fluoro‐1‐deoxy‐2,5‐anhydro‐ d ‐mannitol ( 13 , Scheme ) was tested for PET imaging of breast tumor in rabbits by Sun and co‐workers . The results showed that the probe is taken up more avidly by the tumor than by normal cells but is rapidly excreted.…”

Section: Biochemical and Biomedical Glut Agentsmentioning

confidence: 99%

“…[23][24][25]28] Scheme5.Glucose-and fructose-based PET imagingprobes. [30,34,36,[39][40][41] ChemBioChem 2017, 18,1774 -1788 www.chembiochem.org Fructose-transport-targeting probesa ttracted attention due to the apparent connectionb etween the expression of fructose transporterG lut 5a nd cancerd evelopment, progression, and metastasis. [5] Designedb yM aeda and co-workers, [38] 1-[ 18 F]fluoro-1-deoxy-d-fructose (1-FDF, 11,S cheme 5) was the first fructose derivativetested as at racer for targeting Glut 5i n cancers.S ynthesized in two steps from 2,3,4,5-di-O-isopropylidene-1-O-(trifluoromethanesulfonyl)-d-fructose, 1-[ 18 F]fluoro-1deoxy-d-fructose was tested in mouse and rat tumor xenografts and showed rapid clearance through kidney and liver.…”

Section: Gluts and Diagnostic Probesmentioning

confidence: 99%

Molecular Tools for Facilitative Carbohydrate Transporters (Gluts)

Tanasova

Fedie

2017

ChemBioChem

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Facilitative carbohydrate transporters-Gluts-have received wide attention over decades due to their essential role in nutrient uptake and links with various metabolic disorders, including diabetes, obesity, and cancer. Endeavors directed towards understanding the mechanisms of Glut-mediated nutrient uptake have resulted in a multidisciplinary research field spanning protein chemistry, chemical biology, organic synthesis, crystallography, and biomolecular modeling. Gluts became attractive targets for cancer research and medicinal chemistry, leading to the development of new approaches to cancer diagnostics and providing avenues for cancer-targeting therapeutics. In this review, the current state of knowledge of the molecular interactions behind Glut-mediated sugar uptake, Glut-targeting probes, therapeutics, and inhibitors are discussed.

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“…GLUT4 has been found to have links with insulin resistance and diabetes and has been a potential therapeutic target [26]. [18][19][20], because GLUT transporters being antiporter take up and excrete carbohydrates, but not their phosphorylated analogs [21]. As a result, sugar transport is loosely coupled to phosphorylation, so that a high rate of sugar accumulation is maintained without requiring a reduction in the intracellular sugar concentration.…”

Section: Gluts: Classification and Expressionmentioning

confidence: 99%

Fluorescent Probe Development for Fructose Specific Transporters in Cancer

Fedie¹

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Flow synthesis of a versatile fructosamine mimic and quenching studies of a fructose transport probe

Cited by 8 publications

References 31 publications

The synthetic versatility of the Tiffeneau–Demjanov chemistry in homologation tactics

The synthetic versatility of the Tiffeneau–Demjanov chemistry in homologation tactics

Molecular Tools for Facilitative Carbohydrate Transporters (Gluts)

Fluorescent Probe Development for Fructose Specific Transporters in Cancer

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