Mechanisms of MTH1 inhibition-induced DNA strand breaks: The slippery slope from the oxidized nucleotide pool to genotoxic damage

Rai, Priyamvada; Sobol, Robert W.

doi:10.1016/j.dnarep.2019.03.001

Cited by 26 publications

(23 citation statements)

References 119 publications

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“…MTH1 preserves genomic integrity by preventing the incorporation of mutagenic purines into nuclear and/or mitochondrial DNA [63]. Depletion or inhibition of MTH1 also results in DNA strand breaks [64]. Additionally, MTH1 helps to protect telomeres, the essential structures at the end of chromosomes, from their oxidation and shortening and prevents the induction of genomic instability [65].…”

Section: The Repair Of Oxidative Dna Damagementioning

confidence: 99%

Oxidative Damage in Sporadic Colorectal Cancer: Molecular Mapping of Base Excision Repair Glycosylases in Colorectal Cancer Patients

Vodička

Urbanová

Makovický

et al. 2020

IJMS

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Oxidative stress with subsequent premutagenic oxidative DNA damage has been implicated in colorectal carcinogenesis. The repair of oxidative DNA damage is initiated by lesion-specific DNA glycosylases (hOGG1, NTH1, MUTYH). The direct evidence of the role of oxidative DNA damage and its repair is proven by hereditary syndromes (MUTYH-associated polyposis, NTHL1-associated tumor syndrome), where germline mutations cause loss-of-function in glycosylases of base excision repair, thus enabling the accumulation of oxidative DNA damage and leading to the adenoma-colorectal cancer transition. Unrepaired oxidative DNA damage often results in G:C>T:A mutations in tumor suppressor genes and proto-oncogenes and widespread occurrence of chromosomal copy-neutral loss of heterozygosity. However, the situation is more complicated in complex and heterogeneous disease, such as sporadic colorectal cancer. Here we summarized our current knowledge of the role of oxidative DNA damage and its repair on the onset, prognosis and treatment of sporadic colorectal cancer. Molecular and histological tumor heterogeneity was considered. Our study has also suggested an additional important source of oxidative DNA damage due to intestinal dysbiosis. The roles of base excision repair glycosylases (hOGG1, MUTYH) in tumor and adjacent mucosa tissues of colorectal cancer patients, particularly in the interplay with other factors (especially microenvironment), deserve further attention. Base excision repair characteristics determined in colorectal cancer tissues reflect, rather, a disease prognosis. Finally, we discuss the role of DNA repair in the treatment of colon cancer, since acquired or inherited defects in DNA repair pathways can be effectively used in therapy.

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Section: The Repair Of Oxidative Dna Damagementioning

confidence: 99%

Oxidative Damage in Sporadic Colorectal Cancer: Molecular Mapping of Base Excision Repair Glycosylases in Colorectal Cancer Patients

Vodička

Urbanová

Makovický

et al. 2020

IJMS

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“…The expression level of NUDT1 is higher than the adjacent normal tissues in the oncogenic KRAS-driven cancers such as pancreatic and lung cancer [19]. The main protein production of NUDT1 is MTH1 protein, which expressed in cytoplasm and could hydrolyze the 8-oxo-dGTP into 8-oxo-dGMP or pyrophosphate [12,20]. Therefore, the gene mutation caused by 8-oxo-dGTP was inhibited by overexpressed NUDT1 and the cancer cell apoptosis could not be activated [21].…”

Section: Discussionmentioning

confidence: 99%

NUDT1-Knockdown Inhibits Proliferation, Invasion and Migration of CAL27

Shan

2020

Preprint

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Background: The high level of reactive oxygen species (ROS) in cancer could oxidize guanine into 8-oxoG resulting in A: T changed into G: C or G: C into A: T. Nudix hydrolase 1 (NUDT1) overexpressed in many kind of cancers could hydrolyze the 8-oxo-dGTP into 8-oxo-dGMP or pyrophosphate to prevent the DNA damage or gene mutation. However, the role and function of NUDT1 in oral squamous cell carcinoma (OSCC) has not been investigated.Methods: Firstly, the bioinformatics methods were used to predict the biological process, cellular component and molecular function of NUDT1 and to confirm the mRNA and protein expression level of NUDT1 in OSCC. Furthermore, the MTT assay, Flow Cytometry, Transwell (Invasion), Scratch Test and Transwell (Migration) were used to test the effect of NUDT1 inhibitor on the proliferation, cell apoptosis, invasion and migration of CAL27. In addition, western blot was used to exam the expression level of NUDT1 and cleaved caspase-3 in different groups. Finally, the laser scanning microscope (LSM) was used to test the invadopodia formation level in different groups.Results: The bioinformatics analysis suggested that both mRNA and protein of NUDT1 overexpressed in head and neck squamous cell carcinoma (HNSCC) and OSCC. Furthermore, the biological process of NUDT1 mainly enriched in response to oxidative stress, aging, response to cadmium ion and male gonad development in OSCC. the cellular component of NUDT1 mainly enriched in extracellular exosome, cytoplasm, plasma membrane and nucleus in OSCC. The molecular function of NUDT1 mainly enriched in protein binding in OSCC. Finally, the biological experiments confirmed that NUDT1-knockdown could inhibit the proliferation, invasion, migration and promote cell apoptosis of CAL27.Conclusion: The overexpressed NUDT1 is positively associated with the progression of OSCC which has much potential to be new target in targeted therapy of OSCC.

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“…It is mostly present in cytosol and, in lesser amounts, in mitochondria and in nuclei. Higher expression levels of the enzyme were found in thymus, testis, embryo, proliferating blood lymphocytes [193], and in cancer cells when compared with normal ones [194]. Its enzymatic activity, together with its cellular distribution and the overexpression in cancers, lead to hypothesise for MTH1 a possible role in the sanitization of nucleotide pools both for nuclear and mitochondrial DNA/RNA replication and transcription processes, preventing the misincorporation of oxidised nucleotides into nucleic acids (Figure 6, Panel 1).…”

Section: Human Mutt Homologmentioning

confidence: 99%

“…A small increase in ROS levels promotes proliferation and cancer cell survival [196,197], whereas large amounts of ROS inhibit proliferation [198] and promote senescence [199,200] and apoptosis in several cancer models [200,201,202,203]. While it is widely accepted that MTH1 is dispensable in healthy cells [194], the role of the enzyme in removing oxidised dNTP in cancer cells, thus promoting their survival, and the consequent possibility to use this enzyme as a chemotherapeutic target, is controversial. These discordances, arising probably from the use in the different reports of different experimental conditions (inhibitors, siRNA, shRNA, or CRISPR technique) and models (cell cultures, xenograft, etc.…”

Section: Human Mutt Homologmentioning

confidence: 99%

Purine-Metabolising Enzymes and Apoptosis in Cancer

Camici¹,

Garcia‐Gil

Pesi³

et al. 2019

Cancers

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The enzymes of both de novo and salvage pathways for purine nucleotide synthesis are regulated to meet the demand of nucleic acid precursors during proliferation. Among them, the salvage pathway enzymes seem to play the key role in replenishing the purine pool in dividing and tumour cells that require a greater amount of nucleotides. An imbalance in the purine pools is fundamental not only for preventing cell proliferation, but also, in many cases, to promote apoptosis. It is known that tumour cells harbour several mutations that might lead to defective apoptosis-inducing pathways, and this is probably at the basis of the initial expansion of the population of neoplastic cells. Therefore, knowledge of the molecular mechanisms that lead to apoptosis of tumoural cells is key to predicting the possible success of a drug treatment and planning more effective and focused therapies. In this review, we describe how the modulation of enzymes involved in purine metabolism in tumour cells may affect the apoptotic programme. The enzymes discussed are: ectosolic and cytosolic 5′-nucleotidases, purine nucleoside phosphorylase, adenosine deaminase, hypoxanthine-guanine phosphoribosyltransferase, and inosine-5′-monophosphate dehydrogenase, as well as recently described enzymes particularly expressed in tumour cells, such as deoxynucleoside triphosphate triphosphohydrolase and 7,8-dihydro-8-oxoguanine triphosphatase.

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Mechanisms of MTH1 inhibition-induced DNA strand breaks: The slippery slope from the oxidized nucleotide pool to genotoxic damage

Cited by 26 publications

References 119 publications

Oxidative Damage in Sporadic Colorectal Cancer: Molecular Mapping of Base Excision Repair Glycosylases in Colorectal Cancer Patients

Oxidative Damage in Sporadic Colorectal Cancer: Molecular Mapping of Base Excision Repair Glycosylases in Colorectal Cancer Patients

NUDT1-Knockdown Inhibits Proliferation, Invasion and Migration of CAL27

Purine-Metabolising Enzymes and Apoptosis in Cancer

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