The landscape of cancer cell line metabolism

Li, Haoxin; Ning, Shaoyang; Ghandi, Mahmoud; Kryukov, Gregory V.; Gopal, Shuba; Deik, Amy; Souza, Amanda; Pierce, Kerry A.; Keskula, Paula; Hernandez, Desiree; Ann, Julie; Shkoza, Dojna; Apfel, Verena; Zou, Yilong; Vázquez, Francisca; Barretina, Jordi; Pagliarini, Raymond; Galli, Giorgio; Root, David E.; Hahn, William C.; Tsherniak, Aviad; Giannakis, Marios; Schreiber, Stuart L.; Clish, Clary B.; Garraway, Levi A.; Sellers, William R.

doi:10.1038/s41591-019-0404-8

Cited by 409 publications

(431 citation statements)

References 30 publications

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“…ASNase could break down both asparagine and glutamine, even though its glutaminase activity was not required for ASNS‐negative cancer cells (Chan et al , ). Moreover, ASNase was found effective in treating solid tumors with intrinsic loss of ASNS (Li et al , ). We observed that in cell culture conditions, both asparagine and glutamine were robustly depleted by ASNase (Fig G).…”

Section: Discussionmentioning

confidence: 99%

SLC 1A3 contributes to L‐asparaginase resistance in solid tumors

et al. 2019

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L‐asparaginase (ASNase) serves as an effective drug for adolescent acute lymphoblastic leukemia. However, many clinical trials indicated severe ASNase toxicity in patients with solid tumors, with resistant mechanisms not well understood. Here, we took a functional genetic approach and identified SLC1A3 as a novel contributor to ASNase resistance in cancer cells. In combination with ASNase, SLC1A3 inhibition caused cell cycle arrest or apoptosis, and myriads of metabolic vulnerabilities in tricarboxylic acid (TCA) cycle, urea cycle, nucleotides biosynthesis, energy production, redox homeostasis, and lipid biosynthesis. SLC1A3 is an aspartate and glutamate transporter, mainly expressed in brain tissues, but high expression levels were also observed in some tumor types. Here, we demonstrate that ASNase stimulates aspartate and glutamate consumptions, and their refilling through SLC1A3 promotes cancer cell proliferation. Lastly, in vivo experiments indicated that SLC1A3 expression promoted tumor development and metastasis while negating the suppressive effects of ASNase by fueling aspartate, glutamate, and glutamine metabolisms despite of asparagine shortage. Altogether, our findings identify a novel role for SLC1A3 in ASNase resistance and suggest that restrictive aspartate and glutamate uptake might improve ASNase efficacy with solid tumors.

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Section: Discussionmentioning

confidence: 99%

SLC 1A3 contributes to L‐asparaginase resistance in solid tumors

et al. 2019

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“…As such, the global lipid landscape of cancer cell lines greatly differs from noncancerous cells . Indeed, recent evidence also shows that substantial lipid diversity exists within distinct types of cancer cells …”

Section: Lipid Metabolism and Leukaemiamentioning

confidence: 99%

“…91 Indeed, recent evidence also shows that substantial lipid diversity exists within distinct types of cancer cells. 92 Sphingolipid synthesis is a tightly regulated process that is thought to be self-regulated. Importantly, enzymes involved in sphingolipid metabolism have been identified as targets for the Runx family of genes with glucosylceramide and ganglioside synthesis being upregulated and S1P catabolism downregulated upon Runx activation.…”

Section: Lipid Metabolism and Leukaemiamentioning

confidence: 99%

Fat for fuel: lipid metabolism in haematopoiesis

et al. 2019

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The importance of metabolic regulation in the immune system has launched back into the limelight in recent years. Various metabolic pathways have been examined in the context of their contribution to maintaining immune cell homeostasis and function. Moreover, this regulation is also important in the immune cell precursors, where metabolism controls their maintenance and cell fate. This review will discuss lipid metabolism in the context of haematopoiesis, that is blood cell development. We specifically focus on nonoxidative lipid metabolism which encapsulates the synthesis and degradation of the major lipid classes such as phospholipids, sphingolipids and sterols. We will also discuss how these metabolic processes are affected by haematological malignancies such as leukaemia and lymphoma, which are known to have altered metabolism, and how these different pathways contribute to the pathology.

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“…The inherent plasticity of cellular metabolism and the high degree of metabolic heterogeneity in TNBCs pose great challenges for metabolism targeting therapy 21 . Recent work suggests that heterogeneous metabolic dependencies within cancer cells underline the differential therapeutic vulnerabilities 22 . Therefore, in order for GLUT1 inhibition to be a successful strategy for TNBC therapy, the precise contexts in which this metabolic pathway is essential needs to be identified.…”

Section: Introductionmentioning

confidence: 99%

GLUT1 inhibition blocks growth of RB1-positive Triple Negative Breast Cancer

Ba-Alawi

Deblois

et al. 2019

Preprint

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Triple negative breast cancer (TNBC) is a deadly form of breast cancer due to the development of resistance to chemotherapy affecting over 30% of patients. New therapeutics and companion biomarkers are urgently needed. Recognizing the elevated expression of glucose transporter 1 (GLUT1, encoded by SLC2A1) and associated metabolic dependencies in TNBC, we investigated the vulnerability of TNBC cell lines and patient-derived samples to GLUT1 inhibition. We report that genetic or pharmacological inhibition of GLUT1 with BAY-876 impairs the growth of a subset of TNBC cells displaying high glycolytic and lower oxidative phosphorylation (OXPHOS) rates. Pathway enrichment analysis of gene expression data implicates E2F Targets pathway activity as a surrogate of OXPHOS activity. Furthermore, the protein levels of retinoblastoma tumor suppressor (RB1) are strongly correlated with the degree of sensitivity to GLUT1 inhibition in TNBC, where RB1-negative cells are insensitive to GLUT1 inhibition. Collectively, our results highlight a strong and targetable RB1-GLUT1 metabolic axis in TNBC and warrant clinical evaluation of GLUT1 inhibition in TNBC patients stratified according to RB1 protein expression levels.

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The landscape of cancer cell line metabolism

Cited by 409 publications

References 30 publications

SLC 1A3 contributes to L‐asparaginase resistance in solid tumors

SLC 1A3 contributes to L‐asparaginase resistance in solid tumors

Fat for fuel: lipid metabolism in haematopoiesis

GLUT1 inhibition blocks growth of RB1-positive Triple Negative Breast Cancer

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