Anna Skibowska-Bielińska scite author profile

Anna Skibowska-Bielińska

5Publications

47Citation Statements Received

111Citation Statements Given

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University Clinical Centre

Publications

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The estimation of selected endogenous anticoagulation system parameters in patients with subclinical Cushing's syndrome

Świątkowska−Stodulska

Kaniuka-Jakubowska²,

Wiśniewski³

et al. 2011

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Objective: An increased tendency towards thromboembolic events is observed in patients with Cushing's syndrome. There are much fewer publications available about thromboembolic complications in patients with subclinical Cushing's syndrome (SCS). Therefore, a question arises whether hemostatic disturbances appear in this particular disease phase. Aim of study: Estimation of protein C (PC), free protein S (FPS), antithrombin (AT) activity, thrombomodulin (TM) concentration and activated PC resistance (APCR) in patients with SCS. Materials and methods: We studied 35 patients with SCS. The control group consisted of 33 healthy volunteers. The activity of PC, AT, FPS, APCR and the concentration of TM was estimated in all representatives.Results: The comparison of the examined coagulation parameters between the patients with SCS and the healthy individuals revealed significantly higher mean PC activity and mean FPS activity in the SCS group. Mean TM concentration was significantly lower in patients with SCS compared with the control group. The differences in APCR and AT activity were not significant. We did not prove any statistically significant correlations between the examined coagulation parameters and hormonal parameters. We did not find any correlation between the concentration of cortisol and basic coagulation parameters such as international normalized ratio, activated partial thromboplastin time or fibrinogen in the group with SCS either. Conclusions: The patients with SCS present disturbances in endogenous anticoagulation system defined as PC, FPS activity and TM concentration. This finding suggests an impact of mild autonomic cortisol overproduction on coagulation system.

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Assessment of α1-antitrypsin and α2-macroglobulin levels in obese patients

Świątkowska−Stodulska¹,

Babińska²,

Skibowska-Bielińska³

et al. 2008

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Activity of selected coagulation factors in overt and subclinical hypercortisolism

Świątkowska−Stodulska

Skibowska-Bielińska

Wiśniewski

et al. 2015

Endocr J

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Homocysteine and alpha-1 antitrypsin concentration in patients with subclinical hypercortisolemia

Świątkowska−Stodulska

Kaniuka-Jakubowska

Wiśniewski

et al. 2012

Advances in Medical Sciences

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Hageman Factor C46T Promoter Gene Polymorphism in Patients with Hypercortisolism

Świątkowska−Stodulska

Kitowska

Skibowska-Bielińska

et al. 2014

Horm Metab Res

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Glucocorticoids are a group of hormones with a particularly significant effect on hemostasis. In hypercortisolemic patients increased concentrations of II, VIII, and von Willebrand factors were reported. Considerably fewer studies were concerned with factor XII (FXII). There are reports of decreased FXII concentrations in both venous and arterial thrombosis patients. Also, it was determined that FXII C46T promoter gene polymorphism leads to changes of its concentration. The aim of the study was to determine the C46T polymorphism of FXII promoter gene in hypercortisolemic patients. Thirty hypercortisolemic patients were enrolled in the study. Twenty-nine healthy individuals served as controls. Genomic DNA was isolated from peripheral blood leukocytes. To analyse the polymorphism, PCR products were digested by Hga I at 37°C for 23 h, subjected to 2% agarose gel, and stained with ethidium bromide. In all subjects FXII activity was determined using a clot-based method. All statistical calculations were performed using STATA 12.0 software. A p-value lower than 0.05 was considered statistically significant. Prevalence of FXII C46T polymorphism did not differ significantly between hypercortisolemic patients and controls. No correlation was found between FXII activity and its gene promoter polymorphism in the hypercortisolemic group; however, a clear trend was recorded toward higher FXII activities in 46C homozygotes, and lower in 46T homozygotes. Mean FXII activities did not differ significantly between hypercortisolemic patients and the control group. It seems that in hypercortisolemic patients no significant disorders are present concerning FXII concentrations due to the C46T polymorphism of its gene promoter.

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