Elevated Level of DNA Damage and Impaired Repair of Oxidative DNA Damage in Patients with Recurrent Depressive Disorder

Czarny, Piotr; Kwiatkowski, Dominik; Kacperska, Dagmara; Kawczyńska, Daria; Talarowska, Monika; Orzechowska, Agata; Bielecka-Kowalska, Anna; Szemraj, Janusz; Gałecki, Piotr; Śliwiński, Tomasz

doi:10.12659/msm.892317

Cited by 57 publications

(26 citation statements)

References 33 publications

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“…These results are consistent with those of other authors [9–14]. In the previous paper, we did not calculate DRE and, therefore, cannot compare this parameter between the present and our previous study [16]. However, the kinetics of DNA damage repair was monitored and showed that the cells from patients recovered more slowly than those of the controls, suggesting that DNA damage was less efficiently repaired in patients.…”

Section: Discussionsupporting

confidence: 91%

“…However, the urinary levels of 8-oxoG in patients with milder, non-clinical depression did not differ from the healthy controls [15]. Our previous study utilizing comet assay technique on the PBMCs of patients diagnosed with clinical depression confirmed the presence of not only oxidatively modified purines and pyrimidines but also other types of DNA damage, like DNA strand breaks [16]. Furthermore, we also noted that increased DNA damage in patients with depression might be caused not only by the disease itself but also by the impairments of oxidative DNA damage repair, since we observed that the patients’ cells repaired DNA damage induced by hydrogen peroxide (H 2 O 2 ) more slowly than the controls’ cells [17].…”

Section: Introductionmentioning

confidence: 99%

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Impact of Single Nucleotide Polymorphisms of Base Excision Repair Genes on DNA Damage and Efficiency of DNA Repair in Recurrent Depression Disorder

et al. 2016

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Elevated level of DNA damage was observed in patients with depression. Furthermore, single nucleotide polymorphisms (SNPs) of base excision repair (BER) genes may modulate the risk of this disease. Therefore, the aim of this study was to delineate the association between DNA damage, DNA repair, the presence of polymorphic variants of BER genes, and occurrence of depression. The study was conducted on peripheral blood mononuclear cells of 43 patients diagnosed with depression and 59 controls without mental disorders. Comet assay was used to assess endogenous (oxidative) DNA damage and efficiency of DNA damage repair (DRE). TaqMan probes were employed to genotype 12 SNPs of BER genes. Endogenous DNA damage was higher in the patients than in the controls, but none of the SNPs affected its levels. DRE was significantly higher in the controls and was modulated by BER SNPs, particularly by c.977C>G–hOGG1, c.972G>C–MUTYH, c.2285T>C–PARP1, c.580C>T–XRCC1, c.1196A>G–XRCC1, c.444T>G–APEX1, c.-468T>G–APEX1, or c.*50C>T–LIG3. Our study suggests that both oxidative stress and disorders in DNA damage repair mechanisms contribute to elevated levels of DNA lesions observed in depression. Lower DRE can be partly attributed to the presence of specific SNP variants.Electronic supplementary materialThe online version of this article (doi:10.1007/s12035-016-9971-6) contains supplementary material, which is available to authorized users.

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Section: Discussionsupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

Impact of Single Nucleotide Polymorphisms of Base Excision Repair Genes on DNA Damage and Efficiency of DNA Repair in Recurrent Depression Disorder

et al. 2016

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“…Second, the peripheral blood leukocytes showed significantly lower copy number of mitochondrial DNA (mtDNA) and higher oxidative damage due to higher oxidative stress in MDD patients (Chang et al 2015). Similarly, another study reported higher number of single and double stranded breaks in DNA along with oxidative damage with reduced DNA repair activity in patients with depressive disorder (Czarny et al 2015b). The same group further genotyped single nucleotide polymorphisms (SNPs) of three genes encoding glycosylases, which are essential enzymes for adequate operation of base excision repair (BER).…”

Section: Dna Damage In Mddmentioning

confidence: 88%

“…Other studies also showed an increased level of telomere shortening (Simon et al 2006) and an increased frequency of DNA damage (Andreazza et al 2007). Moreover, depression can alter the ability of a cell to repair damaged DNA (Czarny et al 2015b, Forsberg et al 2015), including a reduced plasma antioxidants, antioxidant enzyme function and total antioxidant capacity (Maes et al 2011). There is a significant decreased activity of antioxidants such as whole-blood reduced glutathione, and decreased levels of antioxidant enzymes such as glutathione peroxidase, erythrocyte SOD and serum heme oxygenase 1 in depressed patients (Rybka et al 2013).…”

Section: Dna Damage In Mddmentioning

confidence: 99%

DNA Damage in Major Psychiatric Diseases

et al. 2016

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Human cells are exposed to exogenous insults and continuous production of different metabolites. These insults and unwanted metabolic products might interfere with the stability of genomic DNA. Recently many studies demonstrated that different psychiatric disorders show substantially high level of oxidative DNA damage in the brain accompanied with morphological and functional alterations. It reveals that damaged genomic DNA may contribute to the pathophysiology of these mental illnesses. Here we review the role of oxidative damage and reduced antioxidant ability in some vastly studied psychiatric disorders and emphasize the inclusion of treatment options involving DNA repair. In addition, while most currently used antidepressants are based on the manipulation of the neurotransmitter regulation in managing different mental abnormalities, they are able to prevent or reverse neurotoxin-induced DNA damage. Therefore, it may be plausible to target on genomic DNA alterations for psychiatric therapies, which is of pivotal importance for future anti-psychiatric drug development.

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“…The target gene set focused on aberrant cellular functions associated with inflammation in the context of MDD and included genes that play a role in tryptophan metabolism, lipid metabolism, mitochondrial function, and oxidative stress response. The target genes were chosen based on pathways found to be disrupted in multiple blood and brain MDD studies (Quak et al 2014; Lalovic et al 2010; Czarny et al, 2015; Spinazzola and Zeviani, 2009; Shelton et al, 2011), and gene sets were grouped together based on the functional roles of the target gene products. Importantly, all these genes were expressed in MDD and CTR HDFs at baseline, providing additional evidence that HDFs express genes relevant to cellular dysfunction observed in neuropsychiatric disease as seen in previous studies (Garbett et al, 2015b; Manier et al, 2000; Shelton et al, 2004).…”

Section: Resultsmentioning

confidence: 99%

An altered peripheral IL6 response in major depressive disorder

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Oláh

Korade

et al. 2016

Neurobiology of Disease

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Major depressive disorder (MDD) is one of the most prevalent major psychiatric disorders with a lifetime prevalence of 17%. Recent evidence suggests MDD is not only a brain dysfunction, but a systemic disease affecting the whole body. Central and peripheral inflammatory changes seem to be a centerpiece of MDD pathology: a subset of patients show elevated blood cytokine and chemokine levels that partially normalize with symptom improvement over the course of antidepressant treatment. As this inflammatory process in MDD is poorly understood, we hypothesized that the peripheral tissues of MDD patients will respond differently to inflammatory stimuli, resulting in an aberrant transcriptional response to elevated proinflammatory cytokines. To test this, we used MDD patient- and control-derived dermal fibroblast cultures to investigate their response to an acute treatment with IL6, IL1β, TNFα, or vehicle. Following RNA isolation and subsequent cDNA synthesis, quantitative PCR was used to determine the relative expression level of several families of inflammation-responsive genes. Our results showed comparable expression of the tested genes between MDD patients and controls at baseline. In contrast, MDD patient fibroblasts had a diminished transcriptional response to IL6 in all the gene sets tested (oxidative stress response, mitochondrial function, and lipid metabolism). We also found a significant increase in baseline and IL6 stimulated transcript levels of the IL6 receptor gene. This IL6 receptor transcript increase in MDD fibroblasts was accompanied by an IL6 stimulated increase in induction of SOCS3, which dampens IL6 receptor signaling. Altogether our results demonstrate that there is an altered transcriptional response to IL6 in MDD, which may represent one of the molecular mechanisms contributing to disease pathophysiology. Ultimately we hope that these studies will lead to validation of novel MDD drug targets focused on normalizing the altered IL6 response in patients.

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Elevated Level of DNA Damage and Impaired Repair of Oxidative DNA Damage in Patients with Recurrent Depressive Disorder

Cited by 57 publications

References 33 publications

Impact of Single Nucleotide Polymorphisms of Base Excision Repair Genes on DNA Damage and Efficiency of DNA Repair in Recurrent Depression Disorder

Impact of Single Nucleotide Polymorphisms of Base Excision Repair Genes on DNA Damage and Efficiency of DNA Repair in Recurrent Depression Disorder

DNA Damage in Major Psychiatric Diseases

An altered peripheral IL6 response in major depressive disorder

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