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2 research outputs found

Increased Glucose Availability Sensitizes Pancreatic Cancer to Chemotherapy

Author: Abbas Ata
Bederman Ilya
Brody Jonathan R.
Brunengraber Henri
Chelstowska Sylwia
Feczko John
Goudarzi Maryam
Graor Hallie J.
Hajihassani Omid
Hue Jonathan J.
Kresak Adam
Loftus Alexander W.
Lyssiotis Costas A.
Rathore Moeez
Salvino Joseph M.
Tatsuoka Curtis
Titomihelakis George
Vaziri-Gohar Ali
Wang Gi-Ming
Wang Rui
Willard Belinda
Willis Joseph E.
Winter Jordan M.
Zarei Mahsa
Zarei Mehrdad
Zhang Li
Zhang Renliang
Publication venue: Jefferson Digital Commons
Publication date: 28/06/2023
Field of study

Pancreatic Ductal Adenocarcinoma (PDAC) is highly resistant to chemotherapy. Effective alternative therapies have yet to emerge, as chemotherapy remains the best available systemic treatment. However, the discovery of safe and available adjuncts to enhance chemotherapeutic efficacy can still improve survival outcomes. We show that a hyperglycemic state substantially enhances the efficacy of conventional single- and multi-agent chemotherapy regimens against PDAC. Molecular analyses of tumors exposed to high glucose levels reveal that the expression of GCLC (glutamate-cysteine ligase catalytic subunit), a key component of glutathione biosynthesis, is diminished, which in turn augments oxidative anti-tumor damage by chemotherapy. Inhibition of GCLC phenocopies the suppressive effect of forced hyperglycemia in mouse models of PDAC, while rescuing this pathway mitigates anti-tumor effects observed with chemotherapy and high glucose

Jefferson Digital Commons

Limited nutrient availability in the tumor microenvironment renders pancreatic tumors sensitive to allosteric IDH1 inhibitors

Author: Abbas Ata
Andren Anthony
Bederman Ilya
Bowers Jessica
Brody Jonathan R.
Brunengraber Henri
Cassel Joel
Chen Vanessa
Dukleska Katerina
Erokwu Bernadette
Flask Chris A.
Getts Robert
Graor Hallie J.
Hajihassani Omid
Hue Jonathan J.
Karim Saadia A.
Katayama Erryk S.
Khokhar Imran
Lyssiotis Costas A.
Mohammed Farheen S.
Morton Jennifer P.
Prendergast Erin
Romani Andrea M.P.
Rothermel Luke D.
Salvino Joseph M.
Srikanth Yellamelli V.V.
Tatsuoka Curtis
Vaziri-Gohar Ali
Wang Rui
Winter Jordan M.
Wu Chunying
Zarei Mahsa
Zarei Mehrdad
Zhang Li
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2022
Field of study

Nutrient-deprived conditions in the tumor microenvironment (TME) restrain cancer cell viability due to increased free radicals and reduced energy production. In pancreatic cancer cells a cytosolic metabolic enzyme, wild-type isocitrate dehydrogenase 1 (wtIDH1), enables adaptation to these conditions. Under nutrient starvation, wtIDH1 oxidizes isocitrate to generate α-ketoglutarate (αKG) for anaplerosis and NADPH to support antioxidant defense. In this study, we show that allosteric inhibitors of mutant IDH1 (mIDH1) are potent wtIDH1 inhibitors under conditions present in the TME. We demonstrate that low magnesium levels facilitate allosteric inhibition of wtIDH1, which is lethal to cancer cells when nutrients are limited. Furthermore, the Food & Drug Administration (FDA)-approved mIDH1 inhibitor ivosidenib (AG-120) dramatically inhibited tumor growth in preclinical models of pancreatic cancer, highlighting this approach as a potential therapeutic strategy against wild-type IDH1 cancers

PubMed Central

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