TY - JOUR
T1 - Targeting glutaminolysis in chondrosarcoma in context of the IDH1/2 mutation
AU - Peterse, Elisabeth F.P.
AU - Niessen, Bertine
AU - Addie, Ruben D.
AU - De Jong, Yvonne
AU - Cleven, Arjen H.G.
AU - Kruisselbrink, Alwine B.
AU - Van Den Akker, Brendy E.W.M.
AU - Molenaar, Remco J.
AU - Cleton-Jansen, Anne Marie
AU - Bovée, Judith V.M.G.
N1 - Funding Information: The authors thank Dr. Joel A. Block (Rush University, Chicago, USA) for providing JJ012, Prof. Antonio Llombart-Bosch (Valencia University, Spain) for CH2879 and CH3573, Dr. M. Namba (Okayama University Medical School, Japan) for OUMS27, and Dr. Naoko Kudo (Niigata University Graduate School of Medical and Dental Sciences, Japan) for NDCS1. In addition, the authors thank Gaia Alberti, Hans Baelde, Pauline Wijers-Koster and Inge Briaire-de Bruijn for technical assistance, Jolieke G. van Oosterwijk for construction of the tissue microarray, and Willem Corver for help with the Seahorse experiments. This study was funded by the Leiden University Medical Center. Publisher Copyright: © 2018 Cancer Research UK.
PY - 2018/4/1
Y1 - 2018/4/1
N2 - Introduction: Chondrosarcoma is a malignant cartilage-forming bone tumour in which mutations in IDH1 and IDH2 frequently occur. Previous studies suggest an increased dependency on glutaminolysis in IDH1/2 mutant cells, which resulted in clinical trials with the drugs CB-839, metformin and chloroquine. In this study, the preclinical rationale for using these drugs as a treatment for chondrosarcoma was evaluated. Methods: Expression of glutaminase was determined in 120 cartilage tumours by immunohistochemistry. Ten chondrosarcoma cell lines were treated with the metabolic compounds CB-849, metformin, phenformin (lipophilic analogue of metformin) and chloroquine. Results: A difference in glutaminase expression levels between the different tumour grades (p = 0.001, one-way ANOVA) was identified, with the highest expression observed in high-grade chondrosarcomas. Treatment with CB-839, metformin, phenformin or chloroquine revealed that chondrosarcoma cell lines are sensitive to glutaminolysis inhibition. Metformin and phenformin decreased mTOR activity in chondrosarcoma cells, and metformin decreased LC3B-II levels, which is counteracted by chloroquine. Conclusion: Targeting glutaminolysis with CB-839, metformin, phenformin or chloroquine is a potential therapeutic strategy for a subset of high-grade chondrosarcomas, irrespective of the presence or absence of an IDH1/2 mutation.
AB - Introduction: Chondrosarcoma is a malignant cartilage-forming bone tumour in which mutations in IDH1 and IDH2 frequently occur. Previous studies suggest an increased dependency on glutaminolysis in IDH1/2 mutant cells, which resulted in clinical trials with the drugs CB-839, metformin and chloroquine. In this study, the preclinical rationale for using these drugs as a treatment for chondrosarcoma was evaluated. Methods: Expression of glutaminase was determined in 120 cartilage tumours by immunohistochemistry. Ten chondrosarcoma cell lines were treated with the metabolic compounds CB-849, metformin, phenformin (lipophilic analogue of metformin) and chloroquine. Results: A difference in glutaminase expression levels between the different tumour grades (p = 0.001, one-way ANOVA) was identified, with the highest expression observed in high-grade chondrosarcomas. Treatment with CB-839, metformin, phenformin or chloroquine revealed that chondrosarcoma cell lines are sensitive to glutaminolysis inhibition. Metformin and phenformin decreased mTOR activity in chondrosarcoma cells, and metformin decreased LC3B-II levels, which is counteracted by chloroquine. Conclusion: Targeting glutaminolysis with CB-839, metformin, phenformin or chloroquine is a potential therapeutic strategy for a subset of high-grade chondrosarcomas, irrespective of the presence or absence of an IDH1/2 mutation.
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UR - https://www.ncbi.nlm.nih.gov/pubmed/29576625
U2 - https://doi.org/10.1038/s41416-018-0050-9
DO - https://doi.org/10.1038/s41416-018-0050-9
M3 - Article
C2 - 29576625
SN - 0007-0920
VL - 118
SP - 1074
EP - 1083
JO - British journal of cancer
JF - British journal of cancer
IS - 8
ER -