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Featured researches published by John Mulcahy.


Journal of the American Chemical Society | 2008

A Stereoselective Synthesis of (+)-Gonyautoxin 3

John Mulcahy; J. Du Bois

An asymmetric synthesis of the paralytic shellfish poison (PSP), (+)-gonyautoxin 3, is described. A unique, Rh-catalyzed amination reaction provides rapid access to the heteratom-rich, tricyclic core of the toxin, which is common to more than 30 related natural products. The completed route should facilitate the preparation of other naturally occurring PSPs and designed analogues thereof.


Journal of the American Chemical Society | 2014

Visualizing Dermal Permeation of Sodium Channel Modulators by Mass Spectrometric Imaging

Livia S. Eberlin; John Mulcahy; Alexander Tzabazis; Jialing Zhang; Huwei Liu; Matthew M. Logan; Heather J. Roberts; Gordon K. Lee; David C. Yeomans; Justin Du Bois; Richard N. Zare

Determining permeability of a given compound through human skin is a principal challenge owing to the highly complex nature of dermal tissue. We describe the application of an ambient mass spectrometry imaging method for visualizing skin penetration of sodium channel modulators, including novel synthetic analogs of natural neurotoxic alkaloids, topically applied ex vivo to human skin. Our simple and label-free approach enables successful mapping of the transverse and lateral diffusion of small molecules having different physicochemical properties without the need for extensive sample preparation.


Journal of the American Chemical Society | 2016

Synthesis of the Paralytic Shellfish Poisons (+)-Gonyautoxin 2, (+)-Gonyautoxin 3, and (+)-11,11-Dihydroxysaxitoxin

John Mulcahy; James R. Walker; Jeffrey E. Merit; Alan Whitehead; J. Du Bois

The paralytic shellfish poisons are a collection of guanidine-containing natural products that are biosynthesized by prokaryote and eukaryote marine organisms. These compounds bind and inhibit isoforms of the mammalian voltage-gated Na(+) ion channel at concentrations ranging from 10(-11) to 10(-5) M. Here, we describe the de novo synthesis of three paralytic shellfish poisons, gonyautoxin 2, gonyautoxin 3, and 11,11-dihydroxysaxitoxin. Key steps include a diastereoselective Pictet-Spengler reaction and an intramolecular amination of an N-guanidyl pyrrole by a sulfonyl guanidine. The IC50s of GTX 2, GTX 3, and 11,11-dhSTX have been measured against rat NaV1.4, and are found to be 22 nM, 15 nM, and 2.2 μM, respectively.


Organic Letters | 2006

Expanding the Substrate Scope for C−H Amination Reactions: Oxidative Cyclization of Urea and Guanidine Derivatives

Mihyong Kim; John Mulcahy; and Christine G. Espino; J. Du Bois


Archive | 2010

Methods and compositions for studying, imaging, and treating pain

Justin Dubois; John Mulcahy; Brian Andresen; David C. Yeomans; Sandip Biswal


Archive | 2018

SAXITOXIN DERIVATIVES, METHODS AND COMPOSITIONS FOR STUDYING, IMAGING, AND TREATING PAIN

Justin Du Bois; John Mulcahy; Brian Andresen; David C. Yeomans; Sandip Biswal


Archive | 2017

METHODS FOR STUDYING, IMAGING AND TREATING PAIN, AND COMPOSITIONS FOR STUDYING, IMAGING AND TREATING PAIN

Justin Dubois; John Mulcahy; Brian Andresen; Yeomans David C; Sandip Biswal


Archive | 2015

PAIN STUDY, IMAGING AND THERAPEUTIC METHOD, AND COMPOSITION FOR PAIN STUDY, IMAGING AND THERAPY

Justin Dubois; John Mulcahy; Brian Andresen; Yeomans David C; Sandip Biswal


Archive | 2015

10',11'-modified saxitoxins for the treatment of pain

Hassan Pajouhesh; George Miljanich; John Mulcahy; Bois Justin Du; Matthew Axtman; James T. Walker; Jeffrey E. Merit


Archive | 2015

10',11'-modified saxitoxins useful for the treatment of pain

Hassan Pajouhesh; George Miljanich; John Mulcahy; Justin Du Bois; Matthew Axtman; James T. Walker; Jeffrey E. Merit

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