Compensatory Metabolic Networks in Pancreatic Cancers Upon Perturbation of Glutamine Metabolism

Overview

Journal Nat Commun

Specialty Biology

Date 2017 Jul 4

PMID 28671190

Citations 169

Authors

Douglas E Biancur

Joao A Paulo

Beata Malachowska

Maria Quiles Del Rey

Cristovao M Sousa

Xiaoxu Wang

Albert S W Sohn

Gerald C Chu

Steven P Gygi

J Wade Harper

Wojciech Fendler

Joseph D Mancias

Alec C Kimmelman

Affiliations

Soon will be listed here.

Abstract

Pancreatic ductal adenocarcinoma is a notoriously difficult-to-treat cancer and patients are in need of novel therapies. We have shown previously that these tumours have altered metabolic requirements, making them highly reliant on a number of adaptations including a non-canonical glutamine (Gln) metabolic pathway and that inhibition of downstream components of Gln metabolism leads to a decrease in tumour growth. Here we test whether recently developed inhibitors of glutaminase (GLS), which mediates an early step in Gln metabolism, represent a viable therapeutic strategy. We show that despite marked early effects on in vitro proliferation caused by GLS inhibition, pancreatic cancer cells have adaptive metabolic networks that sustain proliferation in vitro and in vivo. We use an integrated metabolomic and proteomic platform to understand this adaptive response and thereby design rational combinatorial approaches. We demonstrate that pancreatic cancer metabolism is adaptive and that targeting Gln metabolism in combination with these adaptive responses may yield clinical benefits for patients.

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