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Targeting the tumor metabolism by oxamate potentiates the impact of chemotherapeutics in colorectal cancer cells

Yıl 2021, Cilt: 5 Sayı: 3, 205 - 212, 20.09.2021
https://doi.org/10.30621/jbachs.988996

Öz

Background/Aim: Cancer cells promote lactate formation via pyruvate rather than oxidative phosphorylation by programming their metabolism to maintain proliferation under the Warburg effect. It has shown that the altered metabolic phenotype with activation of lactate dehydrogenase-A in the cancer cell may affect survival, chemotherapy resistance, and metastasis. In this direction, studies are focusing on reprogramming cancer metabolism and increase the effectiveness of chemotherapy. In this study, the main aim was to target the Warburg phenotype via the inhibition of lactate dehydrogenase with the combination of sodium oxamate and current colorectal cancer treatment options such as 5-fluorouracil and irinotecan.
Methods: The effect of chemotherapeutics on the cellular behaviour was evaluated by real-time cytotoxicity and migration analysis systems, and metabolic phenotype was assessed by measuring lactate, lactate dehydrogenase expression, and reactive oxygen species levels.
Results: According to the results, the viability and migration of colorectal cancer cells were significantly decreased with the combination of chemotherapeutics and sodium oxamate which decreases lactate levels.
Conclusion: As a result, the combination of sodium oxamate with the chemotherapeutics hinders the cancer cell viability and migration by changing metabolic phenotype with decreased lactate.

Proje Numarası

This project was supported by Dokuz Eylul University-Scientific Research Projects, 2018.KB.SAG.072.

Kaynakça

  • Persidis A. Cancer multidrug resistance. Nat Biotechnol 1999; 17(1); 94-5.
  • Crawford S. Is it time for a new paradigm for systemic cancer treatment? Lessons from a century of cancer chemotherapy. Front Pharmacol. 2013; 4: 68.
  • Galluzzi L, Kepp O, Vander Heiden MG, et al. Metabolic targets for cancer therapy. Nat Rev Drug Discov 2013; 12(11): 829-46.
  • Schwartz L, Supuran CT, Alfarouk KO. The Warburg Effect and the Hallmarks of Cancer. Anticancer Agents Med Chem 2017; 17(2); 164-70.
  • Vander Heiden MG, Cantley LC, Thompson CB. Understanding the Warburg effect: the metabolic requirements of cell proliferation. Science 2009; 324(5930): 1029-33.
  • Doherty JR, Cleveland JL. Targeting lactate metabolism for cancer therapeutics. J Clin Invest 2013; 123(9): 3685-92.
  • Ward PS, Thompson CB. Metabolic reprogramming: a cancer hallmark even warburg did not anticipate. Cancer Cell 2012; 21(3): 297-308.
  • Zhao Z, Han F, Yang S, et al. Oxamate-mediated inhibition of lactate dehydrogenase induces protective autophagy in gastric cancer cells: involvement of the Akt-mTOR signaling pathway. Cancer Lett 2015; 358(1): 17-26.
  • Seliger C, Leukel P, Moeckel S, et al. Lactate-modulated induction of THBS-1 activates transforming growth factor (TGF)-beta2 and migration of glioma cells in vitro. PLoS One 2013; 8(11): e78935.
  • Liu X, Yang Z, Chen Z, et al. Effects of the suppression of lactate dehydrogenase A on the growth and invasion of human gastric cancer cells. Oncol Rep 2015; 33(1): 157-62.
  • Zhai X, Yang Y, Wan J, et al. Inhibition of LDH-A by oxamate induces G2/M arrest, apoptosis and increases radiosensitivity in nasopharyngeal carcinoma cells. Oncol Rep 2013; 30(6): 2983-91.
  • Yang Y, Su D, Zhao L, et al. Different effects of LDH-A inhibition by oxamate in non-small cell lung cancer cells. Oncotarget 2014; 5(23): 11886-96.
  • Fiume L, Manerba M, Vettraino M, et al. Impairment of aerobic glycolysis by inhibitors of lactic dehydrogenase hinders the growth of human hepatocellular carcinoma cell lines. Pharmacology 2010; 86(3): 157-62.
  • Zhou M, Zhao Y, Ding Y, et al. Warburg effect in chemosensitivity: targeting lactate dehydrogenase-A re-sensitizes taxol-resistant cancer cells to taxol. Mol Cancer 2010; 9: 33.
  • Hutton JE, Wang X, Zimmerman LJ, et al. Oncogenic KRAS and BRAF Drive Metabolic Reprogramming in Colorectal Cancer. Mol Cell Proteomics 2016; 15(9): 2924-38.
  • Lundberg IV, Wikberg ML, Ljuslinder I, Li X, Myte R, et al. MicroRNA Expression in KRAS- and BRAF-mutated Colorectal Cancers. Anticancer Res 2018; 38(2): 677-83.
  • Sagaert X, Vanstapel A, Verbeek S. Tumor Heterogeneity in Colorectal Cancer: What Do We Know So Far? Pathobiology 2018; 85(1-2): 72-84
  • Arseneault R, Chien A, Newington JT, et al. Attenuation of LDHA expression in cancer cells leads to redox-dependent alterations in cytoskeletal structure and cell migration. Cancer Lett 2013; 338(2): 255-66.
  • Jiang F, Ma S, Xue Y, et al. LDH-A promotes malignant progression via activation of epithelial-to-mesenchymal transition and conferring stemness in muscle-invasive bladder cancer. Biochem Biophys Res Commun 2016; 469(4): 985-92.
Yıl 2021, Cilt: 5 Sayı: 3, 205 - 212, 20.09.2021
https://doi.org/10.30621/jbachs.988996

Öz

Proje Numarası

This project was supported by Dokuz Eylul University-Scientific Research Projects, 2018.KB.SAG.072.

Kaynakça

  • Persidis A. Cancer multidrug resistance. Nat Biotechnol 1999; 17(1); 94-5.
  • Crawford S. Is it time for a new paradigm for systemic cancer treatment? Lessons from a century of cancer chemotherapy. Front Pharmacol. 2013; 4: 68.
  • Galluzzi L, Kepp O, Vander Heiden MG, et al. Metabolic targets for cancer therapy. Nat Rev Drug Discov 2013; 12(11): 829-46.
  • Schwartz L, Supuran CT, Alfarouk KO. The Warburg Effect and the Hallmarks of Cancer. Anticancer Agents Med Chem 2017; 17(2); 164-70.
  • Vander Heiden MG, Cantley LC, Thompson CB. Understanding the Warburg effect: the metabolic requirements of cell proliferation. Science 2009; 324(5930): 1029-33.
  • Doherty JR, Cleveland JL. Targeting lactate metabolism for cancer therapeutics. J Clin Invest 2013; 123(9): 3685-92.
  • Ward PS, Thompson CB. Metabolic reprogramming: a cancer hallmark even warburg did not anticipate. Cancer Cell 2012; 21(3): 297-308.
  • Zhao Z, Han F, Yang S, et al. Oxamate-mediated inhibition of lactate dehydrogenase induces protective autophagy in gastric cancer cells: involvement of the Akt-mTOR signaling pathway. Cancer Lett 2015; 358(1): 17-26.
  • Seliger C, Leukel P, Moeckel S, et al. Lactate-modulated induction of THBS-1 activates transforming growth factor (TGF)-beta2 and migration of glioma cells in vitro. PLoS One 2013; 8(11): e78935.
  • Liu X, Yang Z, Chen Z, et al. Effects of the suppression of lactate dehydrogenase A on the growth and invasion of human gastric cancer cells. Oncol Rep 2015; 33(1): 157-62.
  • Zhai X, Yang Y, Wan J, et al. Inhibition of LDH-A by oxamate induces G2/M arrest, apoptosis and increases radiosensitivity in nasopharyngeal carcinoma cells. Oncol Rep 2013; 30(6): 2983-91.
  • Yang Y, Su D, Zhao L, et al. Different effects of LDH-A inhibition by oxamate in non-small cell lung cancer cells. Oncotarget 2014; 5(23): 11886-96.
  • Fiume L, Manerba M, Vettraino M, et al. Impairment of aerobic glycolysis by inhibitors of lactic dehydrogenase hinders the growth of human hepatocellular carcinoma cell lines. Pharmacology 2010; 86(3): 157-62.
  • Zhou M, Zhao Y, Ding Y, et al. Warburg effect in chemosensitivity: targeting lactate dehydrogenase-A re-sensitizes taxol-resistant cancer cells to taxol. Mol Cancer 2010; 9: 33.
  • Hutton JE, Wang X, Zimmerman LJ, et al. Oncogenic KRAS and BRAF Drive Metabolic Reprogramming in Colorectal Cancer. Mol Cell Proteomics 2016; 15(9): 2924-38.
  • Lundberg IV, Wikberg ML, Ljuslinder I, Li X, Myte R, et al. MicroRNA Expression in KRAS- and BRAF-mutated Colorectal Cancers. Anticancer Res 2018; 38(2): 677-83.
  • Sagaert X, Vanstapel A, Verbeek S. Tumor Heterogeneity in Colorectal Cancer: What Do We Know So Far? Pathobiology 2018; 85(1-2): 72-84
  • Arseneault R, Chien A, Newington JT, et al. Attenuation of LDHA expression in cancer cells leads to redox-dependent alterations in cytoskeletal structure and cell migration. Cancer Lett 2013; 338(2): 255-66.
  • Jiang F, Ma S, Xue Y, et al. LDH-A promotes malignant progression via activation of epithelial-to-mesenchymal transition and conferring stemness in muscle-invasive bladder cancer. Biochem Biophys Res Commun 2016; 469(4): 985-92.
Toplam 19 adet kaynakça vardır.

Ayrıntılar

Birincil Dil İngilizce
Konular Sağlık Kurumları Yönetimi
Bölüm Research Article
Yazarlar

Gizem Çalıbaşı Koçal 0000-0002-3201-4752

Çağrı Çakıcı 0000-0002-8662-5284

Feriha Toksöz Bu kişi benim 0000-0002-6262-173X

Şeniz İnanç Sürer 0000-0002-4985-9022

Tolga Sever 0000-0002-0135-0243

Yasemin Başbınar 0000-0001-9439-2217

Türkan Yiğitbaşı 0000-0002-0675-1839

Proje Numarası This project was supported by Dokuz Eylul University-Scientific Research Projects, 2018.KB.SAG.072.
Yayımlanma Tarihi 20 Eylül 2021
Gönderilme Tarihi 31 Ağustos 2021
Yayımlandığı Sayı Yıl 2021 Cilt: 5 Sayı: 3

Kaynak Göster

APA Çalıbaşı Koçal, G., Çakıcı, Ç., Toksöz, F., İnanç Sürer, Ş., vd. (2021). Targeting the tumor metabolism by oxamate potentiates the impact of chemotherapeutics in colorectal cancer cells. Journal of Basic and Clinical Health Sciences, 5(3), 205-212. https://doi.org/10.30621/jbachs.988996
AMA Çalıbaşı Koçal G, Çakıcı Ç, Toksöz F, İnanç Sürer Ş, Sever T, Başbınar Y, Yiğitbaşı T. Targeting the tumor metabolism by oxamate potentiates the impact of chemotherapeutics in colorectal cancer cells. JBACHS. Eylül 2021;5(3):205-212. doi:10.30621/jbachs.988996
Chicago Çalıbaşı Koçal, Gizem, Çağrı Çakıcı, Feriha Toksöz, Şeniz İnanç Sürer, Tolga Sever, Yasemin Başbınar, ve Türkan Yiğitbaşı. “Targeting the Tumor Metabolism by Oxamate Potentiates the Impact of Chemotherapeutics in Colorectal Cancer Cells”. Journal of Basic and Clinical Health Sciences 5, sy. 3 (Eylül 2021): 205-12. https://doi.org/10.30621/jbachs.988996.
EndNote Çalıbaşı Koçal G, Çakıcı Ç, Toksöz F, İnanç Sürer Ş, Sever T, Başbınar Y, Yiğitbaşı T (01 Eylül 2021) Targeting the tumor metabolism by oxamate potentiates the impact of chemotherapeutics in colorectal cancer cells. Journal of Basic and Clinical Health Sciences 5 3 205–212.
IEEE G. Çalıbaşı Koçal, Ç. Çakıcı, F. Toksöz, Ş. İnanç Sürer, T. Sever, Y. Başbınar, ve T. Yiğitbaşı, “Targeting the tumor metabolism by oxamate potentiates the impact of chemotherapeutics in colorectal cancer cells”, JBACHS, c. 5, sy. 3, ss. 205–212, 2021, doi: 10.30621/jbachs.988996.
ISNAD Çalıbaşı Koçal, Gizem vd. “Targeting the Tumor Metabolism by Oxamate Potentiates the Impact of Chemotherapeutics in Colorectal Cancer Cells”. Journal of Basic and Clinical Health Sciences 5/3 (Eylül 2021), 205-212. https://doi.org/10.30621/jbachs.988996.
JAMA Çalıbaşı Koçal G, Çakıcı Ç, Toksöz F, İnanç Sürer Ş, Sever T, Başbınar Y, Yiğitbaşı T. Targeting the tumor metabolism by oxamate potentiates the impact of chemotherapeutics in colorectal cancer cells. JBACHS. 2021;5:205–212.
MLA Çalıbaşı Koçal, Gizem vd. “Targeting the Tumor Metabolism by Oxamate Potentiates the Impact of Chemotherapeutics in Colorectal Cancer Cells”. Journal of Basic and Clinical Health Sciences, c. 5, sy. 3, 2021, ss. 205-12, doi:10.30621/jbachs.988996.
Vancouver Çalıbaşı Koçal G, Çakıcı Ç, Toksöz F, İnanç Sürer Ş, Sever T, Başbınar Y, Yiğitbaşı T. Targeting the tumor metabolism by oxamate potentiates the impact of chemotherapeutics in colorectal cancer cells. JBACHS. 2021;5(3):205-12.