Quantitative analysis of mitochondrial DNA 4977-bp deletion in sporadic breast cancer and benign breast diseases

Ye, Chuanzhong; Shu, Xiao‐Ou; Wen, Wanqing; Pierce, Larry A.; Courtney, Regina; Gao, Yu‐Tang; Wang, Zheng; Cai, Qiuyin

doi:10.1007/s10549-007-9613-9

Cited by 47 publications

(41 citation statements)

References 33 publications

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“…In case of human oocytes it has been confirmed that age exhibits the only significant correlation with the presence of the 4977 bp deletion, while other parameters like smoking or early follicular phase FSH did not reveal any correlation (Chan et al, 2005). In recent years, a number of carefully conducted studies reported, that the level of the 4977 bp deletion is not increased in different tumour tissues (Dani et al, 2004;Dai et al, 2006;Ye et al, 2007) and in conditions associated with chronic inflammation like ulcerative colitis (Fukushima and Fiocchi, 2004). Though our data display a great variability even in individuals of the same age group, the large pool of data may help to discriminate between physiological ageing and pathological conditions associated with accelerated ageing.…”

Section: Discussionmentioning

confidence: 97%

The 4977bp deletion of mitochondrial DNA in human skeletal muscle, heart and different areas of the brain: A useful biomarker or more?

Meißner

Bruse

Mohamed

et al. 2008

Experimental Gerontology

143

119

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It has been suggested that deletions of mitochondrial DNA (mtDNA) are important players with regard to the ageing process. Since the early 1990s, the 4977 bp deletion has been studied in various tissues, especially in postmitotic tissues with high energy demand. Unfortunately, some of these studies included less than 10 subjects, so the aim of our study was to quantify reliable the deletion amount in nine different regions of human brain, heart and skeletal muscle in a cohort of 92 individuals. The basal ganglia contain the highest deletion amounts with values up to 2.93% and differences in deletion levels between early adolescence and older ages were up to three orders of magnitude. Values in frontal lobe were on average an order of magnitude lower, but lowest in cerebellar tissue where the amount was on average only 5 x 10 -3 of the basal ganglia. The deletion started to accumulate in iliopsoas muscle early in the fourth decade of life with values between 0.00019% and 0.0035% and was highest in a 102 year-old woman with 0.14%. In comparison to skeletal muscle, the overall abundance in heart muscle of the left ventricle was only one third. The best linear logarithmic correlation between amount of the deletion and age was found in substanta nigra with r=0.87 (p<0.0005) followed by anterior wall of the left ventricle (r=0.82; p<0.0005). With regard to mitochondrial DNA damage, we propose to use the 4977 bp deletion as an ideal biomarker to discriminate between physiological ageing and accelerated ageing. The biological meaning of mitochondrial deletions in the process of ageing is under discussion, but there is experimental evidence that large-scale deletions impair the oxidative phosphorylation in single cells and sensitize these cells to undergo apoptosis.

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Section: Discussionmentioning

confidence: 97%

The 4977bp deletion of mitochondrial DNA in human skeletal muscle, heart and different areas of the brain: A useful biomarker or more?

Meißner

Bruse

Mohamed

et al. 2008

Experimental Gerontology

143

119

View full text Add to dashboard Cite

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“…However, the pathogenesis of mtDNA decrease in cancers remains unclear. It was hypothesised that mitochondrial respiratory dysfunction and damage of mtDNA, such as mutation, deletion or depletion, in carcinogenesis may course the quantitative alterations (Ye et al 2008). Those alterations of mtDNA could correlate with increased risk (Mosquera-Miguel et al 2008;Bai et al 2007) and increased invasiveness of cancer (Simonnet et al 2002).…”

Section: Discussionmentioning

confidence: 99%

Mitochondrial DNA content in paired normal and cancerous breast tissue samples from patients with breast cancer

Fan

Radpour

Haghighi

et al. 2009

J Cancer Res Clin Oncol

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Introduction We develop a multiplex quantitative realtime PCR for synchronized analysis of mitochondrial DNA (mtDNA) and nuclear DNA (nDNA) to investigate relative mtDNA abundance in paired normal and cancerous breast tissues. Materials and methodsThe amounts of nDNA and mtDNA in 102 tissue samples were quantiWed for both glyceraldehype-3-phosphodehydrogenase (GAPDH) gene and mtDNA encoded ATPase (MTATP) 8 gene. The average threshold cycle (Ct) number values of the nDNA and mtDNA were used to calculate relative mtDNA content in breast tissues. Results The median delta Ct ( Ct) and the median mtDNA content for normal and cancerous breast tissues were 6.73 and 2.54, as well as 106.50 and 5.80 (P = 0.000, respectively). The mtDNA content was decreased in 82% of cancerous breast tissues compared with the normal ones. The changes were associated with hormone receptor status. Conclusion Our Wnding suggests that decreased mtDNA content in breast cancer may have diagnostic and prognostic value for the disease.

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“…The common mtDNA 4,977-bp deletion has been shown to accumulate with age, primarily in postmitotic tissues (13) and cancers (20)(21)(22)(23)(24). The different accumulation rate could result from genetic factors (such as tissue type), energy demand, intracellular oxidative stress levels, environmental insults, or cancer progression.…”

Section: Discussionmentioning

confidence: 99%

“…In addition, it is increased by environmental insults, such as UV irradiation (15)(16)(17), cigarette smoking (18,19) and betel quid chewing (20). Moreover, the mtDNA 4,977-bp deletion is also frequently detected in various types of cancer tissues (20)(21)(22)(23)(24). Due to its good correlation with oxidative damage levels in somatic tissues, we hypothesized that the mtDNA deletion would be more frequently detected in breast tissues of the patients with NQO1 609 C/T or T/T genotype than those with C/C genotype.…”

Section: Introductionmentioning

confidence: 99%

Association between mitochondrial DNA 4,977 bp deletion and NAD(P)H:quinone oxidoreductase 1 C609T polymorphism in human breast tissues

et al. 2009

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Abstract. The NAD(P)H:quinone oxidoreductase 1 (NQO1) enzyme is implicated in protection against oxidative stress and carcinogenesis. NQO1 C609T genetic polymorphism was reported to be associated with an increased risk for cancers, including breast cancer. However, there is still lack of evidence whether higher oxidative stress occurs in breast tissues of patients with NQO1 609 C/T and/or T/T genotypes. Mitochondrial DNA (MtDNA) 4,977-bp deletion, the most common mutation of mtDNA, was frequently detected in post-mitotic tissues of aged subjects and associated with oxidative damage. In this study, we detected the mtDNA 4,977-bp deletion in 60 breast cancers and corresponding non-cancerous breast tissues. The incidence of the common 4,977-bp deletion in non-cancerous breast tissues (48.3%) was higher than that in breast cancer (5.0%). Moreover, 63.4% of the breast cancer patients with NQO1 C/T or T/T genotypes had the deletion in their non-cancerous breast tissues. The mtDNA deletion was more frequently detected in breast tissue of NQO1 C/T carriers (65.2%) and T/T carriers (61.1%) as compared with the NQO1 C/C carriers (15.8%, P=0.003). Similar results were observed in the <50 years old (y/o) group (P=0.06) and the ≥50 y/o group (P=0.005). Our findings suggest that mtDNA 4,977-bp deletion associated with NQO1 deficiency is involved in carcinogenesis and progression of breast cancer.

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Quantitative analysis of mitochondrial DNA 4977-bp deletion in sporadic breast cancer and benign breast diseases

Cited by 47 publications

References 33 publications

The 4977bp deletion of mitochondrial DNA in human skeletal muscle, heart and different areas of the brain: A useful biomarker or more?

The 4977bp deletion of mitochondrial DNA in human skeletal muscle, heart and different areas of the brain: A useful biomarker or more?

Mitochondrial DNA content in paired normal and cancerous breast tissue samples from patients with breast cancer

Association between mitochondrial DNA 4,977 bp deletion and NAD(P)H:quinone oxidoreductase 1 C609T polymorphism in human breast tissues

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