Mitochondrial Common Deletion, a Potential Biomarker for Cancer Occurrence, Is Selected against in Cancer Background: A Meta-Analysis of 38 Studies

Nie, Hezhongrong; Shu, Hong-Ying; Vartak, Rasika; Milstein, Amanda Claire; Mo, Yalin; Hu, Xiaoqin; Fang, Hezhi; Shen, Lijun; Ding, Zhinan; Lü, Jianxin; Bai, Yidong

doi:10.1371/journal.pone.0067953

Cited by 38 publications

(24 citation statements)

References 61 publications

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“…Multiple reports have associated the occurrence of this mtDNA common deletion with a wide range of cancer types including breast cancer (Lu et al, 2009; Nie et al, 2013). Investigations involving cell lines further implicated the common deletion in apoptosis and tumorigenesis (Lee et al, 2007; Wang and Lu, 2009).…”

Section: Discussionmentioning

confidence: 99%

“…In addition, increasing evidence suggests that mitochondrial function is severely impaired in various cancers including breast cancer (Deus et al, 2014; Neuzil and Moreno-Sanchez, 2013) due to genetic defects in the OXPHOS system (Chandra and Singh, 2011). Consequently, mtDNA mutations have been recognized as an important aspect of breast cancer occurrence and development (Nie et al, 2013; Shen et al, 2010; Shen et al, 2011; Yu et al, 2009). …”

Section: Introductionmentioning

confidence: 99%

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Mitochondrial common deletion is elevated in blood of breast cancer patients mediated by oxidative stress

Nie

Chen

et al. 2016

Mitochondrion

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The 4,977 bp common deletion is one of the most frequently observed mitochondrial DNA (mtDNA) mutations in human tissues and has been implicated in various human cancer types. It is generally believed that continuous generation of intracellular reactive oxygen species (ROS) during oxidative phosphorylation (OXPHOS) is a major underlying mechanism for generation of such mtDNA deletions while antioxidant systems, including Manganese superoxide dismutase (MnSOD), mitigating the deleterious effects of ROS. However, the clinical significance of this common deletion remains to be explored. A comprehensive investigation on occurrence and accumulation of the common deletion and mtDNA copy number was carried out in breast carcinoma (BC) patients, benign breast disease (BBD) patients and age-matched healthy donors in our study. Meanwhile, the representative oxidative (ROS production, mtDNA and lipid oxidative damage) and anti-oxidative features (MnSOD expression level and variation) in blood samples from these groups were also analyzed. We found that the mtDNA common deletion is much more likely to be detected in BC patients at relatively high levels while the mtDNA content is lower. This alteration has been associated with a higher MnSOD level and higher oxidative damages in both BC and BBD patients. Our results indicate that the mtDNA common deletion in blood may serve a biomarker for the breast cancer.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Mitochondrial common deletion is elevated in blood of breast cancer patients mediated by oxidative stress

Nie

Chen

et al. 2016

Mitochondrion

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“…In studies on other cancers [25,27], ∼5 kb deletion was found to be consistently lowered in cancer tissues; this deletion was detected in 24 % of the breast tumors, 52 % of the colorectal tumors, 79 % of the gastric tumors, and 40 % of the head and neck tumors as compared with 77, 83, 100, and 90 % of the adjacent respective non-tumor tissues [36]. In a meta-analysis on different cancers, ∼5 kb deletion was found to be less in cancer tissues compared to adjacent or matched normal tissues [37]. In another study on oral cancer and precancer tissues, not only this specific deletion was found to be lower in cancer tissues; a trend was observed in this lowering from controls to precancers to cancerous tissues [26].…”

Section: Discussionmentioning

confidence: 99%

D-loop somatic mutations and ∼5 kb “common” deletion in mitochondrial DNA: important molecular markers to distinguish oral precancer and cancer

et al. 2014

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Apart from genomic DNA, mutations at mitochondrial DNA (mtDNA) have been hypothesized to play vital roles in cancer development. In this study, ∼5 kb deletion and D-loop mutations in mtDNA and alteration in mtDNA content were investigated in buccal smears from 104 healthy controls and 74 leukoplakia and 117 cancer tissue samples using Taqman-based quantitative assay and re-sequencing. The ∼5 kb deletion in mtDNA was significantly less (9.8 and 10.5 folds, P < 0.0001) in cancer tissues compared to control and leukoplakia tissues, respectively. On the other hand, somatic mutations in D-loop, investigated in 54 controls, 50 leukoplakias and 56 cancer patients, were found to be significantly more in cancer tissues, but not in leukoplakia tissues, compared to control (Z-score = 5.4). MtDNA contents were observed to be significantly more in leukoplakia (2.1 folds, P = 0.004) and cancer (1.6 folds, P = 0.03) tissues compared to control tissues. So, D-loop somatic mutations and ∼5 kb deletion patterns could be used as distinguishing markers between precancer and cancer tissues. This observation further suggests that somatic mutations in D-loop may facilitate carcinogenesis and cancer cells with less ∼5 kb deletion, i.e., intact mtDNA, may become resistant to apoptosis.

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“…There is considerable evidence suggesting that mitochondria may serve as potential contributors to carcinogenesis even though the exact mechanism of how mitochondria involved is still debatable and is not welldocumented. Thus, mtDNA is now being targeted organelle by an increasing number of laboratories in order to investigate its potential role as biomarker for tumorigenesis in various types of tissues [86,87].…”

Section: Mitochondrial Dna Mutations In Cancermentioning

confidence: 99%

Understanding Mitochondrial DNA in Brain Tumorigenesis

Yusoff¹,

Ahmad²,

Idris³

et al. 2015

Molecular Considerations and Evolving Surgical Management Issues in the Treatment of Patients With a Brain Tumor

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Mitochondrial Common Deletion, a Potential Biomarker for Cancer Occurrence, Is Selected against in Cancer Background: A Meta-Analysis of 38 Studies

Cited by 38 publications

References 61 publications

Mitochondrial common deletion is elevated in blood of breast cancer patients mediated by oxidative stress

Mitochondrial common deletion is elevated in blood of breast cancer patients mediated by oxidative stress

D-loop somatic mutations and ∼5 kb “common” deletion in mitochondrial DNA: important molecular markers to distinguish oral precancer and cancer

Understanding Mitochondrial DNA in Brain Tumorigenesis

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