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Featured researches published by Leokadia Bąk-Romaniszyn.


BMC Public Health | 2012

Predictors of long-term smoking cessation: results from the global adult tobacco survey in Poland (2009–2010)

Dorota Kaleta; Przemyslaw Korytkowski; Teresa Makowiec-Dąbrowska; Bukola Usidame; Leokadia Bąk-Romaniszyn; Adam Fronczak

BackgroundExpanding the information on determinants of smoking cessation is crucial for developing and implementing more effective tobacco control measures at the national as well as European levels. Data on smoking cessation and its social correlates among adults from middle-income countries of Central and Eastern Europe are still poorly reported in the literature. The aim of the study was to analyze the association of socio-demographic indicators with long term tobacco smoking cessation (quit smoking for at least one year prior to interview) among adults. Moreover, we evaluated motives for giving up smoking from former smokers.MethodsData on former as well as current smokers’ socio-demographic and smoking-related characteristics were derived from the Global Adult Tobacco Survey (GATS). GATS is a cross-sectional, nationally representative household survey implemented in Poland between 2009 and 2010. GATS collected data on a representative sample of 7,840 individuals including 1,206 individuals who met the criteria of long-term smoking cessation and 2,233 current smokers. Smoking cessation rate was calculated as the number of former smokers divided by the number of ever smokers. Logistic regression analyses were used to obtain odds ratios (ORs) and 95% confidence interval (CI) of the broad number of variables on successful cessation of smoking.ResultsAmong females the quit rate was 30.4% compared to 37.9% in males (p < 0.01). Former smokers declared concerns about the health hazard of smoking (60.8%) and the high price of cigarettes (11.6%) as primary reasons for smoking cessation. Older age, high education attainment, awareness of smoking health consequences was associated with long-term quitting among both genders. Also employed males had over twice the probability of giving up smoking compared with unemployed, and being religious did not contribute to successful smoking cessation.ConclusionResults indicated that smoking cessation policies focused on younger age groups are vital for curbing tobacco epidemic in Poland and should become a public health main concern. There is also the need for interventions to raise awareness on smoking health risks and quitting benefits are crucial to increase cessation potential among adult smokers. Nevertheless further effort needs to be done to prevent smoking uptake.


Przeglad Gastroenterologiczny | 2015

Small intestinal bacterial overgrowth syndrome in children

Katarzyna Siniewicz-Luzeńczyk; Agnieszka Bik-Gawin; Krzysztof Zeman; Leokadia Bąk-Romaniszyn

Introduction Small intestinal bacterial overgrowth syndrome (SIBO) is defined as an increased number of nonpathogenic bacteria over 105 organisms in 1 millilitre of small intestine content. The most common predisposing factors include, among others, gut motility disorders and chronic use of proton pump inhibitors. The results of recent studies indicate the importance of SIBO in gastrointestinal diseases. Aim To assess the prevalence of SIBO in children with abdominal pain. Material and methods One hundred children (59 girls and 41 boys) aged from 4 to 17 years (mean age: 10.47 ±3.73 years), hospitalised due to abdominal pain, were enrolled in the study. Hydrogen breath test (HBT) with lactulose was established among all patients. Expired air was analysed using a Gastrolyzer (Bedfont). Results The HBT result was positive in 63 (63%) children with abdominal pain; including 40 girls (67.8%) and 23 boys (56.1%). The test was positive in the group of 29 (46%) children aged under 10 years and in the group of 34 (54%) children aged over 10 years. Among the patients who reported for the control study 88% achieved a normalisation of HBT after treatment. Conclusions The prevalence of positive HBT results in the group of patients with abdominal pain is over 60%. Small intestinal bacterial overgrowth syndrome should be considered as one of the causes of abdominal pain in children. The SIBO in children shows a good response to treatment.


Immunobiology | 2016

Components of the lectin pathway of complement activation in paediatric patients of intensive care units.

Anna S. Świerzko; Agnieszka Szala-Poździej; David C. Kilpatrick; Michał Sobociński; Karolina Chojnacka; Anna Sokolowska; Mateusz Michalski; Karolina Mazerant; Jens C. Jensenius; Misao Matsushita; Wojciech Krajewski; Jerzy Szczapa; Leokadia Bąk-Romaniszyn; Krzysztof Zeman; Maciej Cedzynski

Infections are a major cause of childhood mortality. We investigated components of the lectin pathway of complement activation in the context of sepsis at both genetic and protein levels in neonates, infants and older children. Major components of the lectin pathway and two genes for Toll-like receptors were studied in 87 neonates with confirmed sepsis and compared with 40 babies with infections who did not develop sepsis (disease controls) and 273 infection-free neonatal controls. A second cohort comprised 47 older children with sepsis and 87 controls. Low MBL-conferring genotypes (LXA/O+O/O) were more frequent in sepsis patients than in healthy controls but no significant differences in the frequency of SNPs of other lectin pathway genes (FCN1, FCN2, FCN3, MASP1/3, MASP2) or TLR receptor genes (TLR2, TLR4) were found. One case of primary MASP-2 deficiency was found among healthy pre-terms and one neonate suffering from SIRS was heterozygous for the rare FCN1 gene mutation, +6658 G>A. Generally, sepsis was associated with low serum MBL and low ficolin-2 concentrations on admission. Among neonates, ficolin-1 and MASP-2 levels were elevated in sepsis relative to healthy, but not disease, controls. Unlike neonates, ficolin-3 and MASP-2 levels were lower in older patients than in healthy controls while no difference was found for ficolin-1. With the possible exception of MBL, inherited lectin pathway insufficiencies do not seem to predispose to sepsis, rather changes in protein concentrations reflect alterations in disease course.


Przeglad Gastroenterologiczny | 2014

Evaluation of HLA-DQ2/DQ8 genotype in patients with celiac disease hospitalised in 2012 at the Department of Paediatrics.

Dorota Szałowska-Woźniak; Leokadia Bąk-Romaniszyn; Agnieszka Cywińska-Bernas; Krzysztof Zeman

Introduction Celiac disease (CD) is a permanent intolerance to gluten that occurs in genetically predisposed individuals and leads to small intestinal mucosa damage. According to ESPGHAN guidelines from 2012, CD can be diagnosed in a patient with characteristic clinical symptoms, in whom, anti-tissue transglutaminase antibodies (> 10 times the upper limit) are found, endomysial antibodies (EMA) is confirmed and a positive genetic test is obtained. In these conditions no small-bowel biopsies are required. Aim Evaluation of the presence of HLA-DQ2 and HLA-DQ8 haplotypes in children with previously diagnosed CD, hospitalised in 2012 at the Department of Paediatrics and Immunology and/or the Gastroenterological Outpatient Clinic, and their relatives. Material and methods Blood samples of 22 subjects, including 9 children with CD diagnosed on the basis of clinical symptoms, serological investigations and small-intestine biopsy, 7 diagnosed on the basis of clinical symptoms and serological investigations, 2 with the suspicion of CD on the basis of clinical symptoms and 4 relatives of a child with CD. Methods: HLA-DQ2/DQ8 test, automatic evaluation by EUROArrayScan. Results The presence of HLA-DQ2 and/or HLA-DQ8 genotype was confirmed in 16 children with CD diagnosed on the basis of clinical symptoms and serological tests with/without intestinal biopsy, in 2 with the suspicion of CD and in 1 relative of a celiac child. Conclusions The evaluation of HLA-DQ2/DQ8 haplotype confirms the genetic predisposition to CD in subjects with the disease diagnosed previously on the basis of clinical symptoms, serological tests or intestinal biopsy. Genetic testing is particularly indicated for the diagnosis of CD in infants consuming gluten for a short time and in small amounts.


Przeglad Gastroenterologiczny | 2013

Family recognition of celiac disease

Dorota Szałowska; Leokadia Bąk-Romaniszyn

Celiac disease is a permanent intolerance to gluten that leads to small-bowel mucosal villous atrophy during autoimmune processes in genetically predisposed individuals. At present the diagnosis of celiac disease is based on characteristic clinical symptoms, the results of serological investigations (tissue transglutaminase ten times the upper limit of normal, presence of antiendomysial antibodies – EMA) and positive results of genetic examinations. The aim of this study is to present a medical history of a family in which the mother and younger son were diagnosed with celiac disease (confirmed by genotype examination). Before the genetic examination, the father and the elder son were also suspected of suffering from this disease (they were on gluten-free diets). The authors emphasize the usefulness of HLA-DQ2/DQ8 determination in first-degree relatives of celiac patients.


Immunology and Cell Biology | 2017

Lectin pathway factors in patients suffering from juvenile idiopathic arthritis

Katarzyna Kasperkiewicz; Łukasz Eppa; Anna S. Świerzko; Marcin A. Bartłomiejczyk; Zbigniew Żuber; Katarzyna Siniewicz-Luzeńczyk; Elżbieta Mężyk; Misao Matsushita; Leokadia Bąk-Romaniszyn; Krzysztof Zeman; Mikael Skurnik; Maciej Cedzynski

Both complement activation and certain infections (including those with Yersinia sp.) may contribute to the pathogenesis of juvenile idiopathic arthritis (JIA). We investigated factors specific for the lectin pathway of complement: mannose‐binding lectin (MBL), ficolins and MBL‐associated serine protease‐2 (MASP‐2), in 144 patients and 98 controls. One hundred and six patients had oligoarticular disease and 38 had polyarticular disease. In 51 patients (out of 133 tested), Yersinia‐reactive antibodies were found (JIA Ye+ group). MBL deficiency was significantly more frequent in the JIA Ye+ group than in patients without Yersinia‐reactive antibodies or in controls. Median serum ficolin‐2 level was significantly lower (and proportion of values deemed ficolin‐2 insufficient greater) in JIA patients irrespective of their Yersinia antibody status. The minority (C) allele at −64 of the FCN2 gene was less frequent among JIA patients than among control subjects. No differences were found in the frequency of FCN3 gene +1637delC or MASP2 +359 A>G mutations nor for median values of serum ficolin‐1, ficolin‐3 or MASP‐2. However, high levels of serum ficolin‐3 were under‐represented in patients, in contrast to MBL. MBL, ficolin‐1, ficolin‐2, ficolin‐3 and MASP‐2 were also readily detectable in synovial fluid samples but at a considerably lower level than in serum. Our findings suggest a possible role for the lectin pathway in the pathogenesis of JIA, perhaps secondary to a role in host defence, and indicate that investigations on the specificity of lectin pathway recognition molecules towards specific infectious agents in JIA might be fruitful.


Cancer Immunology, Immunotherapy | 2007

Mannan-binding lectin (MBL) in women with tumours of the reproductive system

A. St. Świerzko; K. Florczak; Maciej Cedzynski; J. Szemraj; D. Wydra; Leokadia Bąk-Romaniszyn; J. Emerich; Z. Sułowska


Tobacco Induced Diseases | 2016

Susceptibility to cigarette smoking among secondary and high school students from a socially disadvantaged rural area in Poland.

Kinga Polańska; Piotr Wojtysiak; Leokadia Bąk-Romaniszyn; Dorota Kaleta


Annals of Agricultural and Environmental Medicine | 2012

Changes in smoking prevalence and exposure to environmental tobacco smoke among adults in Łódź, Poland.

Adam Fronczak; Kinga Polańska; Elżbieta Dziankowska-Zaborszczyk; Leokadia Bąk-Romaniszyn; Przemyslaw Korytkowski; Andrzej Wojtyła; Dorota Kaleta


BMC Public Health | 2015

Patterns of nicotine dependence in four Eastern European countries

Dorota Kaleta; Kinga Polańska; Przemyslaw Korytkowski; Bukola Usidame; Leokadia Bąk-Romaniszyn

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Dorota Kaleta

Medical University of Łódź

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Franciszek Szatko

Medical University of Łódź

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Krzysztof Zeman

Memorial Hospital of South Bend

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Jan Krakowiak

Medical University of Łódź

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Kinga Polańska

Medical University of Łódź

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Maciej Cedzynski

Polish Academy of Sciences

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Przemyslaw Korytkowski

West Pomeranian University of Technology

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Izabela Planeta-Malecka

Memorial Hospital of South Bend

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Adam Fronczak

Medical University of Łódź

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