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Dive into the research topics where Eric Brian Sjogren is active.

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Featured researches published by Eric Brian Sjogren.


Molecular Cancer Therapeutics | 2014

Antitumor Activity of the Glutaminase Inhibitor CB-839 in Triple-Negative Breast Cancer

Matthew I. Gross; Susan Demo; Jennifer B. Dennison; Lijing Chen; Tania Chernov-Rogan; Bindu Goyal; Julie Janes; Guy J. Laidig; Evan R. Lewis; Jim Li; Andrew L. Mackinnon; Francesco Parlati; Mirna Rodriguez; Peter Shwonek; Eric Brian Sjogren; Timothy Friend Stanton; Taotao Wang; Jinfu Yang; Frances Zhao; Mark K. Bennett

Glutamine serves as an important source of energy and building blocks for many tumor cells. The first step in glutamine utilization is its conversion to glutamate by the mitochondrial enzyme glutaminase. CB-839 is a potent, selective, and orally bioavailable inhibitor of both splice variants of glutaminase (KGA and GAC). CB-839 had antiproliferative activity in a triple-negative breast cancer (TNBC) cell line, HCC-1806, that was associated with a marked decrease in glutamine consumption, glutamate production, oxygen consumption, and the steady-state levels of glutathione and several tricarboxylic acid cycle intermediates. In contrast, no antiproliferative activity was observed in an estrogen receptor–positive cell line, T47D, and only modest effects on glutamine consumption and downstream metabolites were observed. Across a panel of breast cancer cell lines, GAC protein expression and glutaminase activity were elevated in the majority of TNBC cell lines relative to receptor positive cells. Furthermore, the TNBC subtype displayed the greatest sensitivity to CB-839 treatment and this sensitivity was correlated with (i) dependence on extracellular glutamine for growth, (ii) intracellular glutamate and glutamine levels, and (iii) GAC (but not KGA) expression, a potential biomarker for sensitivity. CB-839 displayed significant antitumor activity in two xenograft models: as a single agent in a patient-derived TNBC model and in a basal like HER2+ cell line model, JIMT-1, both as a single agent and in combination with paclitaxel. Together, these data provide a strong rationale for the clinical investigation of CB-839 as a targeted therapeutic in patients with TNBC and other glutamine-dependent tumors. Mol Cancer Ther; 13(4); 890–901. ©2014 AACR.


Archive | 2012

Heterocyclic inhibitors of glutaminase

Jim Li; Lijing Chen; Bindu Goyal; Guy J. Laidig; Timothy Friend Stanton; Eric Brian Sjogren


Archive | 2013

HETEROCYCLIC GLUTAMINASE INHIBITORS

Jim Li; Lijing Chen; Bindu Goyal; Guy J. Laidig; Timothy Friend Stanton; Eric Brian Sjogren


Archive | 2013

Treatment of cancer with heterocyclic inhibitors of glutaminase

Mark K. Bennett; Matthew I. Gross; Susan D. Bromley; Jim Li; Lijing Chen; Bindu Goyal; Guy J. Laidig; Timothy Friend Stanton; Eric Brian Sjogren


Archive | 2015

Combination therapy with glutaminase inhibitors

Francesco Parlati; Mirna Rodriguez; Matthew I. Gross; Terri L. Davis; Jim Li; Lijing Chen; Bindu Goyal; Guy J. Laidig; Timothy Friend Stanton; Eric Brian Sjogren


Archive | 2014

Treatment of viral infections with inhibitors of glutaminase

Susan D. Bromley; Mark K. Bennett; Matthew I. Gross; Jim Li; Lijing Chen; Bindu Goyal; Guy J. Laidig; Timothy Friend Stanton; Eric Brian Sjogren


Archive | 2017

tratamento de câncer com inibidores heterocíclicos da glutaminase

Bindu Goyal; Eric Brian Sjogren; Guy J. Laidig; Jim Li; Lijing Chen; Mark K. Bennett; Matthew I. Gross; Susan D. Bromley; Timothy Friend Stanton


Archive | 2017

inibidores heterocíclicos de glutaminase

Bindu Goyal; Eric Brian Sjogren; Guy J. Laidig; Jim Li; Lijing Chen; Timothy Friend Stanton


Archive | 2017

inibidores de glutaminase heterocíclica

Bindu Goyal; Eric Brian Sjogren; Guy J. Laidig; Jim Li; Lijing Chen; Timothy Friend Stanton


Archive | 2014

INHIBIDORES HETEROCICLICOS DE GLUTAMINASA

Jim Li; Lijing Chen; Timothy Friend Stanton; Bindu Goyal; Guy J. Laidig; Eric Brian Sjogren

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Guy J. Laidig

University of California

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Mark K. Bennett

California Institute of Technology

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Jennifer B. Dennison

University of Texas MD Anderson Cancer Center

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