Estrogen suppresses brain mitochondrial oxidative stress in female and male rats

Razmara, Ali; Duckles, Sue Piper; Krause, Diana N.; Procaccio, Vincent

doi:10.1016/j.brainres.2007.08.036

Cited by 179 publications

(102 citation statements)

References 70 publications

(96 reference statements)

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“…β-E2 is also effective in several neural injury and toxicity models. In animal models of AD, β-E2 reduces Aβ pathology and improves cognition [15], although the effectiveness of β-E2 is reduced in the presence of APOE4 [16]. This latter observation is consistent with a role for APOE in modulating the biological effects of estrogen-based therapy.…”

supporting

confidence: 67%

Possible APOE Genotype and Sex Dependent Effects of 17-α- estradiol on Alzheimers Disease Pathology

Manaye¹

2013

J Alzheimers Dis Parkinsonism

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Alzheimer's disease (AD) remains the most prevalent cause of elderly dementia, posing an increasingly important health problem as the population ages [1]. AD is a neurodegenerative disorder defined by the presence of extracellular deposits of β-amyloid (Aβ), intraneuronal accumulations of neurofibrillary tangles containing hyperphosporylated tau protein, and the progressive loss of synapses and neurons that correlate with atrophy of brain regions [2]. Specific areas of the brain that show particularly severe neuronal loss include the entorhinal cortex, pyramidal neurons in the CA1 subregion of the hippocampus, and the noradrenergic neurons of the locus coeruleus [3][4][5]. The neuronal populations within these areas mediate attention, learning, memory and other neural processes associated with higher cognitive function. The specific mechanism(s) that underlie neuronal loss are not clearly understood, and there are no approved methods to slow this neurodegeneration.Of the risk factors identified that facilitate AD progression, the strongest are aging, the inheritance of the ε4 allele of the Apolipoprotein E (APOE) gene, and sex -women have a higher incidence of AD than men [6]. The APOE gene encodes a 34 kDa protein that is the major protein component of CNS lipoproteins, involved in lipid transport and redistribution [7]. Even though there is no clear understanding of the role of APOE in AD pathology, the role of APOE4 isoform has been shown to affect synaptic structure, Aβ clearance and transport across blood brain barrier as well as energy metabolism [8]. In mice, APOE4 decrease dendritic spine density and neuronal complexity in various cortical brain regions [9]. In addition, APOE4 mice show impaired learning and memory in the Barnes maze tests [10]. These effects were observed in absence of significant Aβ accumulation suggesting Aβ independent mechanisms contributing to functional impairments in APOE4 carriers.There is a stronger association of APOE with AD in women than men that correlates well with greater hippocampal atrophy, plaque pathology and cognitive decline [11]. The gradual loss of sex steroid hormones in women may contribute to age associated cognitive decline [12]. A neuroprotective role of natural and synthetic estrogens in the mammalian brain has been established during the past decade. In particular, 17-β-estradiol (β-E2), has commonly been known to play a pivotal role in female reproductive physiology, enhances synaptic plasticity, neurite growth, hippocampal neurogliosis and long-term potentiation [13,14]. β-E2 is also effective in several neural injury and toxicity models. In animal models of AD, β-E2 reduces Aβ pathology and improves cognition [15], although the effectiveness of β-E2 is reduced in the presence of APOE4 [16]. This latter observation is consistent with a role for APOE in modulating the biological effects of estrogen-based therapy.Early estrogen replacement therapy prior to menopause has been shown to reduce the AD risk in postmenopausal women [17]. However the effects of β-...

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supporting

confidence: 67%

Possible APOE Genotype and Sex Dependent Effects of 17-α- estradiol on Alzheimers Disease Pathology

Manaye¹

2013

J Alzheimers Dis Parkinsonism

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“…It has been reported that in aged rats, female brain is less prone to oxidative damage than male brain [33]. Furthermore, estrogen treatment enhanced MnSOD activity whereas it had no effect on enzyme protein in brain mitochondria of female rats [35]. This study suggests that the expression and activity of MnSOD may not be well-correlated, and some factors may independently influence MnSOD activity.…”

Section: Discussionmentioning

confidence: 64%

“…Accordingly, the previous studies carried out in rats have reported that females had lower oxidative stress and mitochondrial dysfunction than the males [29][30][31]. However, these reports concerning the gender differences in mitochondrial oxidant status have either dealt with the 4-6 months old animals [32][33], or applied some interventions such as ovariectomy and estrogen replacement therapy [30,32,34,35].…”

Section: Discussionmentioning

confidence: 99%

Age-related changes in the activity and expression of manganese superoxide dismutase, and mitochondrial oxidant generation in female and male rats

Ademoğlu

Özcan²,

Tanrıkulu-Küçük³

et al. 2013

Turk J Bioch

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Objective: The aim of this study was to examine the age-and gender-related differences in peroxide production, manganese superoxide dismutase (MnSOD) activity and expression in liver mitochondria of Wistar rats at 12 and 24 months of age. Methods: The chemiluminometric method for peroxide production, fluorometric method for malondialdehyde (MDA) levels, cumene hydroperoxide assay for glutathione peroxidase (GPx), the nitroblue tetrazolium assay for MnSOD activity, and Western-blotting for MnSOD expression were used. Results: Mitochondrial peroxides are increased significantly in both genders as aging proceeded, and females exhibited more profound increment than the males. Mitochondrial SOD and GPx activities remained unaltered between 12 and 24 months of age, with no difference between two genders. The gender-and age-related differences were observed in MnSOD expression (p<0.01). The SOD activity per expressed enzyme protein was significantly decreased in 24-month-old animals of both genders (p<0.01). Female rats had a significantly lower ratio than their male counterparts (p<0.05). In females, the expression was not associated with the activity of MnSOD, while a positive correlation existed between these parameters in males (r=0.573, p=0.001). Enzyme expression was found to be significantly higher in female rats as compared to their male counterparts. Liver mitochondria are less prone to oxidative damage in female rats compared to males as observed at 12 and 24 months of age Conclusions: An involvement of factors other than estrogen seems to be relevant for the difference in the MnSOD activity and expression pattern between two genders. Key Words: oxidative stress, aging, gender differences, MnSOD, rat liver Conflict of interest: The authors declare that there is no conflict of interest. ÖZETAmaç: Çalışmamızda, 12 ve 24 aylık Wistar cinsi sıçanların karaciğer mitokondrilerinde yaş ve cinsiyet ile ilişkili olarak peroksit üretimi, mangan süperoksit dismutaz (MnSOD) aktivitesi ve ekspresyonundaki ortaya çıkan değişikliklerin incelenmesi amaçlanmıştır. Yöntemler: Peroksit üretimi kemilümünometrik, malondialdehit (MDA) düzeyi florometrik, glutatyon peroksidaz (GPx) kümen hidroperoksit, MnSOD aktivitesi nitroblue tetrazolium yöntemleri ile MnSOD ekspresyonu ise western blotting yöntemi ile ölçülmüştür. Bulgular: Her iki cinsiyette de yaş ilerledikçe SOD ve GPx aktivitelerinde anlamlı bir değişiklik oluşmadığı, mitokondriyal peroksit üretiminin ise anlamlı şekilde arttığı ve bu artışın dişi sıçanlarda daha belirgin olduğu saptanmıştır. MnSOD ekspresyonun da yaş ve cinsiyete bağlı olarak değişiklikler gösterdiği (p<0.01) ve eksprese edilen enzim proteini başına düşen enzim aktivitesinin 24 aylık sıçanlarda her iki cinsiyette de anlamlı olarak azalmakla birlikte (p<0.01) bu azalmanın dişi sıçanlarda erkek sıçanlara göre daha belirgin (p<0.05) olduğu görülmüştür. Erkek sıçanlarda MnSOD aktivitesi ile ekspresyonu arasında pozitif bir korelasyon (r=0.573, p=0.001) olduğu saptanmış, dişi sıçanlarda ise böyle bir il...

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“…32 SOD2 function can be modulated by estrogen and TP53, and thus it may be highly relevant for breast cancer progression and treatment. 33,34 Patients with the high activity Ala allele in SOD2 rs4880 SNP treated by cyclophosphamide had poorer breast cancer survival than patients with the low activity genotype Val/Val. 19,20 In our study, SOD2 rs4880 SNP did not significantly modify the PFS of patients treated by cyclophosphamide (n ¼ 89).…”

Section: Cancer Geneticsmentioning

confidence: 99%

Association of superoxide dismutases and NAD(P)H quinone oxidoreductases with prognosis of patients with breast carcinomas

Hubackova

Václavíková

Ehrlichová

et al. 2011

Intl Journal of Cancer

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Associations of transcript levels of oxidative stress-modifying genes SOD2, SOD3, NQO1 and NQO2 and their functional single nucleotide polymorphisms (SNPs) rs4880, rs1799895, rs2536512, rs699473, rs1800566 and rs1143684 with prognosis of breast cancer patients were studied. SNPs were assessed by allelic discrimination in a cohort of 321 breast cancer patients from the Czech Republic. Transcript levels were determined by real-time polymerase chain reaction (PCR) with absolute quantification in tumor and adjacent non-neoplastic control tissues. Both genotypes and transcript levels were then compared with available clinical data on patients. Patients carrying low activity allele Leu in NQO2 rs1143684 had a greater incidence of stage 0 or I disease (i.e., better prognosis) than patients with the Phe/Phe genotype. This association was more evident in patients without expression of progesterone receptors (p 5 0.031). Patients carrying the Thr allele in SOD3 rs2536512 SNP had a significantly greater incidence of tumors expressing estrogen receptors than patients carrying the Ala/Ala genotype (p 5 0.007). SOD3 transcript level was significantly higher in grade 1 or 2 tumors than in grade 3 tumors (p 5 0.006). Patients carrying T allele in SOD3 rs699473 SNP had significantly poorer progression-free survival (PFS) than patients carrying the CC genotype (p 5 0.038). The same applied to the subgroup of patients treated by hormonal regimens (p 5 0.021). Patients carrying the high activity Ala/Ala genotype in SOD2 (rs4880) had significantly poorer PFS than Val allele carriers in the group treated by cyclophosphamide but not hormonal regimens (p 5 0.004). Our results suggest that NQO2, SOD2 and SOD3 may significantly modify prognosis of breast cancer patients and that their significance should be further characterized.Breast cancer is the most common cancer in women. In 2008, about 1,383,523 new cases of invasive breast cancer were diagnosed worldwide. 1 The necessity of treating such a large number of patients calls for efficient tools that can be used for subgrouping patients according to estimated prognosis. A different spectrum of treatment modalities with diverse mechanisms of action and adverse effects could then be offered to various prognostic groups. Besides well-established classical prognostic factors such as tumor size, nodal status, grading and expression of hormonal receptors, numerous biological molecules are under investigation as potential prognostic biomarkers in breast carcinomas.Excess of oxidative stress, mediated by reactive oxygen species, may cause cellular deregulation leading to cell apoptosis, 2 proliferation or tumor promotion. 3 Alkylation and topoisomerase poisoning present the major mechanisms of action of cyclophosphamide and anthracyclines, respectively. Oxidative stress represents an additional cytotoxic mechanism. 4,5 One of the initial molecules of oxidative stress, superoxide anion radical, is formed by the univalent reduction of triplet-state molecular oxygen. This process is mediated by e...

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Estrogen suppresses brain mitochondrial oxidative stress in female and male rats

Cited by 179 publications

References 70 publications

Possible APOE Genotype and Sex Dependent Effects of 17-α- estradiol on Alzheimers Disease Pathology

Possible APOE Genotype and Sex Dependent Effects of 17-α- estradiol on Alzheimers Disease Pathology

Age-related changes in the activity and expression of manganese superoxide dismutase, and mitochondrial oxidant generation in female and male rats

Association of superoxide dismutases and NAD(P)H quinone oxidoreductases with prognosis of patients with breast carcinomas

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