Dichloroacetate affects proliferation but not survival of human colorectal cancer cells

Delaney, Leanne M.; Ho, Nelson; Morrison, Jodi; Farias, Nathan; Mosser, Dick D.; Coomber, Brenda L.

doi:10.1007/s10495-014-1046-4

Cited by 22 publications

(15 citation statements)

References 52 publications

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“…Our previous study demonstrated that dichloroacetate effectively induced a dose-dependent proliferation arrest of in vitro cultures of glioblastoma cells but had no significant effect on noncancerous cells (15). This result is in line with most of the studies that investigated the efficacy of dichloroacetate demonstrating that a therapeutic window exists although suprapharmacologic level of dichloroacetate (5-50 mmol/L) is necessary to halt the growth of cancer cells in vitro (9,32,33,35). In the current study, we further analyzed the cell-cycle distribution after dichloroacetate treatment showing that dichloroacetate induced G 2 -M arrest and decreased the cell proportion in S-phase.…”

Section: Discussionsupporting

confidence: 75%

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Sensitization of Glioblastoma Cells to Irradiation by Modulating the Glucose Metabolism

Shen

Hau

Joshi

et al. 2015

Molecular Cancer Therapeutics

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Because radiotherapy significantly increases median survival in patients with glioblastoma, the modulation of radiation resistance is of significant interest. High glycolytic states of tumor cells are known to correlate strongly with radioresistance; thus, the concept of metabolic targeting needs to be investigated in combination with radiotherapy. Metabolically, the elevated glycolysis in glioblastoma cells was observed postradiotherapy together with upregulated hypoxia-inducible factor (HIF)-1a and its target pyruvate dehydrogenase kinase 1 (PDK1). Dichloroacetate, a PDK inhibitor currently being used to treat lactic acidosis, can modify tumor metabolism by activating mitochondrial activity to force glycolytic tumor cells into oxidative phosphorylation. Dichloroacetate alone demonstrated modest antitumor effects in both in vitro and in vivo models of glioblastoma and has the ability to reverse the radiotherapy-induced glycolytic shift when given in combination. In vitro, an enhanced inhibition of clonogenicity of a panel of glioblastoma cells was observed when dichloroacetate was combined with radiotherapy. Further mechanistic investigation revealed that dichloroacetate sensitized glioblastoma cells to radiotherapy by inducing the cell-cycle arrest at the G 2 -M phase, reducing mitochondrial reserve capacity, and increasing the oxidative stress as well as DNA damage in glioblastoma cells together with radiotherapy. In vivo, the combinatorial treatment of dichloroacetate and radiotherapy improved the survival of orthotopic glioblastoma-bearing mice. In conclusion, this study provides the proof of concept that dichloroacetate can effectively sensitize glioblastoma cells to radiotherapy by modulating the metabolic state of tumor cells. These findings warrant further evaluation of the combination of dichloroacetate and radiotherapy in clinical trials.

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Section: Discussionsupporting

confidence: 75%

“…It has been demonstrated with moderate antitumor activity (31)(32)(33) and to induce apoptosis in tumors of patients with glioblastoma by restoring the mitochondrial activity (34). Several studies have also used it as a radiosensitizer in lung (11), colorectal (13), and prostate cancer cells (12) in vitro.…”

Section: Discussionmentioning

confidence: 99%

Sensitization of Glioblastoma Cells to Irradiation by Modulating the Glucose Metabolism

Shen

Hau

Joshi

et al. 2015

Molecular Cancer Therapeutics

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“…4A) showed that increased proteins involved in structural constituent of ribosome, structural molecule activity, ATPase activity were changed significantly, while the decreased proteins participated in nucleic acid binding, heterocyclic compound binding, and other bindings were severely affected. The results were consistent with the notion that DCA can lead to the inhibition of cell proliferation and cause cell death24. In cellular compartment (Fig.…”

Section: Resultssupporting

confidence: 91%

Crosstalk among proteome, acetylome and succinylome in colon cancer HCT116 cell treated with sodium dichloroacetate

Zhu

Hou

Zhao

et al. 2016

Sci Rep

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Protein lysine acetylation and succinylation play important regulatory roles in cells, both of which or each other has a close relationship. Dichloroacetate (DCA), a well-known pyruvate dehydrogenase kinase (PDK) inhibitor, has the potential to be used as anti-cancer drugs for several tumors including colorectal cancer. However, little is known about the potential mechanism of DCA-based cancer therapy by protein posttranslational modifications (PTM) including global proteome, acetylome and succinylome. Here the combinations with stable isotope labeling (SILAC), antibody affinity enrichment and high resolution LC-MS/MS analysis were performed in human colon cancer HCT116 cells. The quantifiable proteome was annotated using bioinformatics. In total, 4,518 proteins, 1,436 acetylation sites, and 671 succinylation sites were quantified, respectively to DCA treatment. Among the quantified acetylated sites, 158 were with increased level (quantification ratio >1.5) and 145 with decreased level (quantification ratio <0.67). Meanwhile, 179 up-regulated and 114 down-regulated succinylated sites were identified. The bioinformatics analyses initially showed acetylation and succinylation were involved in a wide range of cellular functions upon DCA-based anti-cancer effects. Notably, protein-protein interaction network analyses demonstrated widespread interactions modulated by protein acetylation and succinylation. Taken together, this study may shed a light on understanding the mechanism of DCA-based cancer treatment.

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“…In the colorectal cancer cell line HCT116, DCA has been shown to affect cell proliferation without affecting survival or inducing apoptosis [65]. In other cancer cell lines, the effects were more varied [66].…”

Section: Catching Cancer In the Metabolic Crab Pot: Attempts Failurementioning

confidence: 99%

Pyruvate and Metabolic Flexibility: Illuminating a Path Toward Selective Cancer Therapies

Olson

Schell

Rutter

2016

Trends in Biochemical Sciences

106

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Dysregulated metabolism is an emerging hallmark of cancer and there is abundant interest in developing therapies to selectively target these aberrant metabolic phenotypes. Sitting at the decision point between mitochondrial carbohydrate oxidation and aerobic glycolysis (i.e., the “Warburg Effect”), the synthesis and consumption of pyruvate is tightly controlled and is often differentially regulated in cancer cells. This review examines recent efforts toward understanding and targeting mitochondrial pyruvate metabolism, and addresses some of the successes, pitfalls and significant challenges of metabolic therapy to date.

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Dichloroacetate affects proliferation but not survival of human colorectal cancer cells

Cited by 22 publications

References 52 publications

Sensitization of Glioblastoma Cells to Irradiation by Modulating the Glucose Metabolism

Sensitization of Glioblastoma Cells to Irradiation by Modulating the Glucose Metabolism

Crosstalk among proteome, acetylome and succinylome in colon cancer HCT116 cell treated with sodium dichloroacetate

Pyruvate and Metabolic Flexibility: Illuminating a Path Toward Selective Cancer Therapies

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