Partner: Monika Talarowska |
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Ostatnie publikacje
1. | Czarny P.♦, Kwiatkowski D.♦, Toma M.♦, Kubiak J.♦, Sliwinska A.♦, Talarowska M.♦, Szemraj J.♦, Maes M.♦, Galecki P.♦, Sliwinski T.♦, Impact of single-nucleotide polymorphisms of base excision repair genes on DNA damage and efficiency of DNA repair in recurrent depression disorder, MOLECULAR NEUROBIOLOGY, ISSN: 0893-7648, DOI: 10.1007/s12035-016-9971-6, Vol.54, No.6, pp.4150-4159, 2017 Streszczenie: 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. Słowa kluczowe: Recurrent depression disorder, DNA damage, DNA repair, Oxidative stress, Base excision repair, Single nucleotide polymorphism Afiliacje autorów:
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2. | Czarny P.♦, Kwiatkowski D.♦, Gałecki P.♦, Talarowska M.♦, Orzechowska A.♦, Bobińska K.♦, Bielecka-Kowalska A.♦, Szemraj J.♦, Maes M.♦, Su K.P.♦, Śliwiński T.♦, Association between single nucleotide polymorphisms of MUTYH, hOGG1 and NEIL1 genes, and depression, JOURNAL OF AFFECTIVE DISORDERS, ISSN: 0165-0327, DOI: 10.1016/j.jad.2015.05.044, Vol.184, pp.90-96, 2015 Streszczenie: Background: An elevated levels oxidative modified DNA bases and a decreased efficiency of oxidative DNA damage repair were found in patients with depression disorders, including recurrent type (rDD). The glycosylases are involved in base excision repair (BER), which eliminates oxidative DNA damage. Therefore, we genotyped the single nucleotide polymorphisms (SNPs) of genes encoding three glycosylases: hOGG1, MUTYH and NEILL Słowa kluczowe: Depression, Glycosylases, BER, DNA repair, DNA damage Afiliacje autorów:
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3. | Kwiatkowski D.♦, Czarny P.♦, Gałecki P.♦, Bachurska A.♦, Talarowska M.♦, Orzechowska A.♦, Bobińska K.♦, Bielecka-Kowalska A.♦, Pietras T.♦, Szemraj J.♦, Maes M.♦, Śliwiński T.♦, Variants of Base Excision Repair Genes MUTYH, PARP1 and XRCC1 in Alzheimer's Disease Risk, NEUROPSYCHOBIOLOGY, ISSN: 0302-282X, DOI: 10.1159/000381985, Vol.71, No.3, pp.176-186, 2015 Streszczenie: Background: Many clinical studies have shown that oxidative stress pathways and the efficiency of the oxidative DNA damage base excision repair (BER) system are associated with the pathogenesis of Alzheimer's disease (AD). Reduced BER efficiency may result from polymorphisms of BER-related genes. In the present study, we examine whether single nucleotide polymorphisms (SNPs) of BER genes are associated with increased risk of AD. Methods: SNP genotyping was carried out on DNA isolated from peripheral blood mononuclear cells obtained from 120 patients with AD and 110 healthy volunteers. Samples were genotyped for the presence of BER-related SNPs, i.e.XRCC1-rs1799782, rs25487; MUTYH-rs3219489, and PARP1-rs1136410. Results: We found a positive association between AD risk and the presence of G/A genotype variant of the XRCC1 rs25487 polymorphism [odds ratio (OR) = 3.762,95% Cl: 1.793-7.8911. The presence of the A/A genotype of this polymorphism reduced the risk of AD (OR = 0.485,95% Cl: 0.271-0.870). In cases of the PARP1 gene rs1136410 polymorphism, we observed that the T/C variant increases (OR =4.159, 95% Cl: 1.978-8.745) while the T/T variant reduces risk (OR = 0.240,95% Cl: 0.114-0.556) of AD. Conclusions: We conclude that BER gene polymorphisms may play an important role in the etiology of AD. Diagnosing the presence or absence of particular genetic variants may be an important marker of AD. Further research on a larger population is needed. There is also a need to examine polymorphisms of other BER in the context of AD risk. Słowa kluczowe: Alzheimer's disease, Base excision repair, Polymorphisms Afiliacje autorów:
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4. | Czarny P.♦, Kwiatkowski D.♦, Kacperska D.♦, Kawczyńska D.♦, Talarowska M.♦, Orzechowska A.♦, Bielecka-Kowalska A.♦, Szemraj J.♦, Gałecki P.♦, Śliwiński T.♦, Elevated Level of DNA Damage and Impaired Repair of Oxidative DNA Damage in Patients with Recurrent Depressive Disorder, Medical Science Monitor, ISSN: 1643-3750, DOI: 10.12659/MSM.892317, Vol.21, pp.412-418, 2015 Streszczenie: Background: Depressive disorder (DD), including recurrent DD (rDD), is a severe psychological disease, which affects a large percentage of the world population. Although pathogenesis of the disease is not known, a growing body of evidence shows that inflammation together with oxidative stress may contribute to development of DD. Since reactive oxygen species produced during stress may damage DNA, we wanted to evaluate the extent of DNA damage and efficiency of DNA repair in patients with depression. Słowa kluczowe: Depression, DNA Damage, DNA Repair, Oxidative Stress, Reactive Oxygen Species Afiliacje autorów:
| 15p. |