Your search keyword '"Conner, Elizabeth S."' showing total 5 results

1. Remote Hydroxylation through Radical Translocation and Polar Crossover.

Author

Hollister KA, Conner ES, Spell ML, Deveaux K, Maneval L, Beal MW, and Ragains JR

Subjects

Alcohols chemical synthesis, Carbon chemistry, Catalysis, Fluoxetine chemical synthesis, Hydrogen chemistry, Hydroxylation, Iridium chemistry, Oxidation-Reduction, Sulfonamides chemistry, Sulfonic Acids chemistry, Hydrocarbons chemistry, Oxygen chemistry, Water chemistry

Abstract

Mild conditions are reported for the hydroxylation of aliphatic C-H bonds through radical translocation, oxidation to carbocation, and nucleophilic trapping with H2O. This remote functionalization employs fac-[Ir(ppy)3] together with Tz(o) sulfonate esters and sulfonamides to facilitate the site-selective replacement of relatively inert C-H bonds with the more synthetically useful C-OH group. The hydroxylation of a range of substrates and the methoxylation of two substrates through 1,6- and 1,7-hydrogen-atom transfer are demonstrated. In addition, a synthesis of the antidepressant fluoxetine using remote hydroxylation as a key step is presented., (© 2015 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2015

2. Visible-light-promoted selenofunctionalization of alkenes.

Author

Conner ES, Crocker KE, Fernando RG, Fronczek FR, Stanley GG, and Ragains JR

Abstract

A visible-light-promoted method for the selenofunctionalization (and tellurofunctionalization) of alkenes has been developed. This method obviates the prepreparation of moisture-sensitive chalcogen electrophiles. The experimental setup is simple, and superior yields are obtained in the case of selenofunctionalization (up to 99%) while moderate to good yields are obtained in the case of tellurofunctionalization (53-75%). A variety of intra- and intermolecular processes and a short synthesis of the Amaryllidaceae alkaloid (±)-γ-lycorane are demonstrated with this method.

Published

2013

3. Ascaroside activity in Caenorhabditis elegans is highly dependent on chemical structure.

Author

Hollister KA, Conner ES, Zhang X, Spell M, Bernard GM, Patel P, de Carvalho AC, Butcher RA, and Ragains JR

Subjects

Animals, Caenorhabditis elegans growth & development, Glycolipids chemical synthesis, Glycolipids pharmacology, Larva drug effects, Larva physiology, Pheromones chemical synthesis, Pheromones pharmacology, Structure-Activity Relationship, Caenorhabditis elegans metabolism, Glycolipids chemistry, Pheromones chemistry

Abstract

The nematode Caenorhabditis elegans secretes ascarosides, structurally diverse derivatives of the 3,6-dideoxysugar ascarylose, and uses them in chemical communication. At high population densities, specific ascarosides, which are together known as the dauer pheromone, trigger entry into the stress-resistant dauer larval stage. In order to study the structure-activity relationships for the ascarosides, we synthesized a panel of ascarosides and tested them for dauer-inducing activity. This panel includes a number of natural ascarosides that were detected in crude pheromone extract, but as yet have no assigned function, as well as many unnatural ascaroside derivatives. Most of these ascarosides, some of which have significant structural similarity to the natural dauer pheromone components, have very little dauer-inducing activity. Our results provide a primer to ascaroside structure-activity relationships and suggest that slight modifications to ascaroside structure dramatically influence binding to the relevant G protein-coupled receptors that control dauer formation., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

4. A novel ascaroside controls the parasitic life cycle of the entomopathogenic nematode Heterorhabditis bacteriophora.

Author

Noguez JH, Conner ES, Zhou Y, Ciche TA, Ragains JR, and Butcher RA

Subjects

Animals, Caenorhabditis elegans growth & development, Caenorhabditis elegans physiology, Glycolipids chemistry, Life Cycle Stages, Nematoda chemistry, Nematoda growth & development, Pheromones chemistry, Glycolipids metabolism, Host-Parasite Interactions, Insecta parasitology, Nematoda physiology, Pheromones metabolism

Abstract

Entomopathogenic nematodes survive in the soil as stress-resistant infective juveniles that seek out and infect insect hosts. Upon sensing internal host cues, the infective juveniles regurgitate bacterial pathogens from their gut that ultimately kill the host. Inside the host, the nematode develops into a reproductive adult and multiplies until unknown cues trigger the accumulation of infective juveniles. Here, we show that the entomopathogenic nematode Heterorhabditis bacteriophora uses a small-molecule pheromone to control infective juvenile development. The pheromone is structurally related to the dauer pheromone ascarosides that the free-living nematode Caenorhabditis elegans uses to control its development. However, none of the C. elegans ascarosides are effective in H. bacteriophora, suggesting that there is a high degree of species specificity. Our report is the first to show that ascarosides are important regulators of development in a parasitic nematode species. An understanding of chemical signaling in parasitic nematodes may enable the development of chemical tools to control these species.

Published

2012

5. Synthesis and biochemical evaluation of thiochromanone thiosemicarbazone analogues as inhibitors of cathepsin L.

Author

Song J, Jones LM, Kumar GD, Conner ES, Bayeh L, Chavarria GE, Charlton-Sevcik AK, Chen SE, Chaplin DJ, Trawick ML, and Pinney KG

Abstract

A series of 36 thiosemicarbazone analogues containing the thiochromanone molecular scaffold functionalized primarily at the C-6 position were prepared by chemical synthesis and evaluated as inhibitors of cathepsins L and B. The most promising inhibitors from this group are selective for cathepsin L and demonstrate IC50 values in the low nanomolar range. In nearly all cases, the thiochromanone sulfide analogues show superior inhibition of cathepsin L as compared to their corresponding thiochromanone sulfone derivatives. Without exception, the compounds evaluated were inactive (IC50 > 10000 nM) against cathepsin B. The most potent inhibitor (IC50 = 46 nM) of cathepsin L proved to be the 6,7-difluoro analogue 4. This small library of compounds significantly expands the structure-activity relationship known for small molecule, nonpeptidic inhibitors of cathepsin L.

Published

2012