Glutaminase inhibitor CB-839 synergizes with carfilzomib in resistant multiple myeloma cells

Thompson, Ravyn M.; Dytfeld, Dominik; Reyes, Leticia; Robinson, Reeder M.; Curtiss, Brittany M.; Manevich, Yefim; Jakubowiak, Andrzej; Komarnicki, Mieczysław; Przybyłowicz-Chalecka, Anna; Szczepaniak, Tomasz; Mitra, Amit; Ness, Brian G. Van; Łuczak, Magdalena; Dolloff, Nathan G.

doi:10.18632/oncotarget.16262

Cited by 99 publications

(96 citation statements)

References 51 publications

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“…Interestingly, we found that upregulation of LIG3 is associated to bortezomib resistance and that LIG3 downregulation is highly toxic and partially restore drug sensitivity in bortezomib-resistant cells. These findings could be consistent with recent evidence which showed that bortezomib resistance in malignant plasmacells is associated to high dependency on increased mitochondrial activity and that mitochondrial activity modulation decreases bortezomib resistance [57][58][59].…”

Section: Discussionsupporting

confidence: 93%

miR-22 suppresses DNA ligase III addiction in multiple myeloma

et al. 2018

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Multiple myeloma (MM) is a hematologic malignancy characterized by high genomic instability. Here we provide evidence that hyper-activation of DNA ligase III (LIG3) is crucial for genomic instability and survival of MM cells. LIG3 mRNA expression in MM patients correlates with shorter survival and even increases with more advanced stage of disease. Knockdown of LIG3 impairs MM cells viability in vitro and in vivo, suggesting that neoplastic plasmacells are dependent on LIG3-driven repair. To investigate the mechanisms involved in LIG3 expression, we investigated the post-transcriptional regulation. We identified miR-22-3p as effective negative regulator of LIG3 in MM. Enforced expression of miR-22 in MM cells downregulated LIG3 protein, which in turn increased DNA damage inhibiting in vitro and in vivo cell growth. Taken together, our findings demonstrate that myeloma cells are addicted to LIG3, which can be effectively inhibited by miR-22, promoting a novel axis of genome stability regulation.

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Section: Discussionsupporting

confidence: 93%

miR-22 suppresses DNA ligase III addiction in multiple myeloma

et al. 2018

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“…The data highlight increased antioxidant capacity, higher redox homeostasis and NAD + levels as the key metabolic changes in PI-resistance and are consistent with findings from earlier models including our own proteomic data. [5][6][7][8][9][10][11][12][13] We functionally validated the increased capacity of PIresistant cells to buffer the formation of reactive oxygen species (ROS), demonstrating 2-to 4-fold lower ROS levels in these cells than in PI-sensitive cells, confirming a significantly higher antioxidant capacity (Figure 2A). Consistent with this, PI-resistant cells are more resistant than PI-sensitive cells to H2O2-induced cytotoxicity (Online Supplementary Figure S4, Online Supplementary Table S2).…”

mentioning

confidence: 82%

A metabolic switch in proteasome inhibitor-resistant multiple myeloma ensures higher mitochondrial metabolism, protein folding and sphingomyelin synthesis

Besse

Mendez-Lopez

et al. 2019

Haematologica

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“…From a therapeutic perspective, mitochondrial metabolism is an attractive target for treatment regimes, but is not without significant risk of toxicity. Agents which target the mitochondria are potently anti-proliferative, and several small molecules are in clinical trials which inhibit mitochondrial metabolic pathways [14,15,23]. The present study points to a potential complication with this kind of therapeutic strategy however; in that targeting mitochondrial metabolism (e.g.…”

Section: Discussionmentioning

confidence: 77%

“…fluorouracil) have been used clinically for decades [13]. Therapies which target amino acid synthesis are emerging in clinical development, and are showing promise [14][15][16].…”

Section: Introductionmentioning

confidence: 99%

CHCHD4 regulates tumour proliferation and EMT-related phenotypes, through respiratory chain-mediated metabolism

et al. 2019

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Background Mitochondrial oxidative phosphorylation (OXPHOS) via the respiratory chain is required for the maintenance of tumour cell proliferation and regulation of epithelial to mesenchymal transition (EMT)-related phenotypes through mechanisms that are not fully understood. The essential mitochondrial import protein coiled-coil helix coiled-coil helix domain-containing protein 4 (CHCHD4) controls respiratory chain complex activity and oxygen consumption, and regulates the growth of tumours in vivo. In this study, we interrogate the importance of CHCHD4-regulated mitochondrial metabolism for tumour cell proliferation and EMT-related phenotypes, and elucidate key pathways involved. Results Using in silico analyses of 967 tumour cell lines, and tumours from different cancer patient cohorts, we show that CHCHD4 expression positively correlates with OXPHOS and proliferative pathways including the mTORC1 signalling pathway. We show that CHCHD4 expression significantly correlates with the doubling time of a range of tumour cell lines, and that CHCHD4-mediated tumour cell growth and mTORC1 signalling is coupled to respiratory chain complex I (CI) activity. Using global metabolomics analysis, we show that CHCHD4 regulates amino acid metabolism, and that CHCHD4-mediated tumour cell growth is dependent on glutamine. We show that CHCHD4-mediated tumour cell growth is linked to CI-regulated mTORC1 signalling and amino acid metabolism. Finally, we show that CHCHD4 expression in tumours is inversely correlated with EMT-related gene expression, and that increased CHCHD4 expression in tumour cells modulates EMT-related phenotypes. Conclusions CHCHD4 drives tumour cell growth and activates mTORC1 signalling through its control of respiratory chain mediated metabolism and complex I biology, and also regulates EMT-related phenotypes of tumour cells. Electronic supplementary material The online version of this article (10.1186/s40170-019-0200-4) contains supplementary material, which is available to authorized users.

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Glutaminase inhibitor CB-839 synergizes with carfilzomib in resistant multiple myeloma cells

Cited by 99 publications

References 51 publications

miR-22 suppresses DNA ligase III addiction in multiple myeloma

miR-22 suppresses DNA ligase III addiction in multiple myeloma

A metabolic switch in proteasome inhibitor-resistant multiple myeloma ensures higher mitochondrial metabolism, protein folding and sphingomyelin synthesis

CHCHD4 regulates tumour proliferation and EMT-related phenotypes, through respiratory chain-mediated metabolism

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