Upregulation of the Glutaminase II Pathway Contributes to Glutamate Production upon Glutaminase 1 Inhibition in Pancreatic Cancer

Sunag Udupa; Stephanie Nguyen; Giang Hoang; Tu Nguyen; Addison Quinones; Khoa Pham; Ryoichi Asaka; Kiet Nguyen; Cissy Zhang; Amira Elgogary; Jin G. Jung; Qingguo Xu; Jie Fu; Ajit G. Thomas; Takashi Tsukamoto; Justin Hanes; Barbara S. Slusher; Arthur J.L. Cooper; Anne Le

doi:10.1002/pmic.201800451

Upregulation of the Glutaminase II Pathway Contributes to Glutamate Production upon Glutaminase 1 Inhibition in Pancreatic Cancer

Sunag Udupa
, Stephanie Nguyen
, Giang Hoang
, Tu Nguyen
, Addison Quinones
, Khoa Pham
, Ryoichi Asaka
, Kiet Nguyen
, Cissy Zhang
, Amira Elgogary
, Jin G. Jung
, Qingguo Xu
, Jie Fu
, Ajit G. Thomas
, Takashi Tsukamoto
, Justin Hanes
, Barbara S. Slusher
, Arthur J.L. Cooper
, Anne Le

Department of Pathology and Laboratory Medicine

Research output: Contribution to journal › Article › peer-review

56 Scopus citations

Abstract

The targeting of glutamine metabolism specifically via pharmacological inhibition of glutaminase 1 (GLS1) has been translated into clinical trials as a novel therapy for several cancers. The results, though encouraging, show room for improvement in terms of tumor reduction. In this study, the glutaminase II pathway is found to be upregulated for glutamate production upon GLS1 inhibition in pancreatic tumors. Moreover, genetic suppression of glutamine transaminase K (GTK), a key enzyme of the glutaminase II pathway, leads to the complete inhibition of pancreatic tumorigenesis in vivo unveiling GTK as a new metabolic target for cancer therapy. These results suggest that current trials using GLS1 inhibition as a therapeutic approach targeting glutamine metabolism in cancer should take into account the upregulation of other metabolic pathways that can lead to glutamate production; one such pathway is the glutaminase II pathway via GTK.

Original language	English (US)
Article number	1800451
Journal	Proteomics
Volume	19
Issue number	21-22
DOIs	https://doi.org/10.1002/pmic.201800451
State	Published - Nov 1 2019

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

All Science Journal Classification (ASJC) codes

Biochemistry
Molecular Biology

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10.1002/pmic.201800451

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Udupa, S., Nguyen, S., Hoang, G., Nguyen, T., Quinones, A., Pham, K., Asaka, R., Nguyen, K., Zhang, C., Elgogary, A., Jung, J. G., Xu, Q., Fu, J., Thomas, A. G., Tsukamoto, T., Hanes, J., Slusher, B. S., Cooper, A. J. L., & Le, A. (2019). Upregulation of the Glutaminase II Pathway Contributes to Glutamate Production upon Glutaminase 1 Inhibition in Pancreatic Cancer. Proteomics, 19(21-22), Article 1800451. https://doi.org/10.1002/pmic.201800451

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title = "Upregulation of the Glutaminase II Pathway Contributes to Glutamate Production upon Glutaminase 1 Inhibition in Pancreatic Cancer",

abstract = "The targeting of glutamine metabolism specifically via pharmacological inhibition of glutaminase 1 (GLS1) has been translated into clinical trials as a novel therapy for several cancers. The results, though encouraging, show room for improvement in terms of tumor reduction. In this study, the glutaminase II pathway is found to be upregulated for glutamate production upon GLS1 inhibition in pancreatic tumors. Moreover, genetic suppression of glutamine transaminase K (GTK), a key enzyme of the glutaminase II pathway, leads to the complete inhibition of pancreatic tumorigenesis in vivo unveiling GTK as a new metabolic target for cancer therapy. These results suggest that current trials using GLS1 inhibition as a therapeutic approach targeting glutamine metabolism in cancer should take into account the upregulation of other metabolic pathways that can lead to glutamate production; one such pathway is the glutaminase II pathway via GTK.",

author = "Sunag Udupa and Stephanie Nguyen and Giang Hoang and Tu Nguyen and Addison Quinones and Khoa Pham and Ryoichi Asaka and Kiet Nguyen and Cissy Zhang and Amira Elgogary and Jung, \{Jin G.\} and Qingguo Xu and Jie Fu and Thomas, \{Ajit G.\} and Takashi Tsukamoto and Justin Hanes and Slusher, \{Barbara S.\} and Cooper, \{Arthur J.L.\} and Anne Le",

note = "Publisher Copyright: {\textcopyright} 2019 Johns Hopkins University School of Medicine. Proteomics published by WILEY-VCH Verlag GmbH \& Co. KGaA, Weinheim",

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doi = "10.1002/pmic.201800451",

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Udupa, S, Nguyen, S, Hoang, G, Nguyen, T, Quinones, A, Pham, K, Asaka, R, Nguyen, K, Zhang, C, Elgogary, A, Jung, JG, Xu, Q, Fu, J, Thomas, AG, Tsukamoto, T, Hanes, J, Slusher, BS, Cooper, AJL & Le, A 2019, 'Upregulation of the Glutaminase II Pathway Contributes to Glutamate Production upon Glutaminase 1 Inhibition in Pancreatic Cancer', Proteomics, vol. 19, no. 21-22, 1800451. https://doi.org/10.1002/pmic.201800451

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AU - Udupa, Sunag

AU - Nguyen, Stephanie

AU - Hoang, Giang

AU - Nguyen, Tu

AU - Quinones, Addison

AU - Pham, Khoa

AU - Asaka, Ryoichi

AU - Nguyen, Kiet

AU - Zhang, Cissy

AU - Elgogary, Amira

AU - Jung, Jin G.

AU - Xu, Qingguo

AU - Fu, Jie

AU - Thomas, Ajit G.

AU - Tsukamoto, Takashi

AU - Hanes, Justin

AU - Slusher, Barbara S.

AU - Cooper, Arthur J.L.

AU - Le, Anne

PY - 2019/11/1

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N2 - The targeting of glutamine metabolism specifically via pharmacological inhibition of glutaminase 1 (GLS1) has been translated into clinical trials as a novel therapy for several cancers. The results, though encouraging, show room for improvement in terms of tumor reduction. In this study, the glutaminase II pathway is found to be upregulated for glutamate production upon GLS1 inhibition in pancreatic tumors. Moreover, genetic suppression of glutamine transaminase K (GTK), a key enzyme of the glutaminase II pathway, leads to the complete inhibition of pancreatic tumorigenesis in vivo unveiling GTK as a new metabolic target for cancer therapy. These results suggest that current trials using GLS1 inhibition as a therapeutic approach targeting glutamine metabolism in cancer should take into account the upregulation of other metabolic pathways that can lead to glutamate production; one such pathway is the glutaminase II pathway via GTK.

AB - The targeting of glutamine metabolism specifically via pharmacological inhibition of glutaminase 1 (GLS1) has been translated into clinical trials as a novel therapy for several cancers. The results, though encouraging, show room for improvement in terms of tumor reduction. In this study, the glutaminase II pathway is found to be upregulated for glutamate production upon GLS1 inhibition in pancreatic tumors. Moreover, genetic suppression of glutamine transaminase K (GTK), a key enzyme of the glutaminase II pathway, leads to the complete inhibition of pancreatic tumorigenesis in vivo unveiling GTK as a new metabolic target for cancer therapy. These results suggest that current trials using GLS1 inhibition as a therapeutic approach targeting glutamine metabolism in cancer should take into account the upregulation of other metabolic pathways that can lead to glutamate production; one such pathway is the glutaminase II pathway via GTK.

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Upregulation of the Glutaminase II Pathway Contributes to Glutamate Production upon Glutaminase 1 Inhibition in Pancreatic Cancer

Abstract

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