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Dive into the research topics where B. Ozsait is active.

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Featured researches published by B. Ozsait.


Annals of Medicine | 2009

ADAM-9, ADAM-15, and ADAM-17 are upregulated in macrophages in advanced human atherosclerotic plaques in aorta and carotid and femoral arteries—Tampere vascular study

Niku Oksala; Mari Levula; Nina Airla; Markku Pelto-Huikko; Rebekka M. Ortiz; Otso Järvinen; Juha-Pekka Salenius; B. Ozsait; Evrim Komurcu-Bayrak; Nihan Erginel-Unaltuna; Ari-Pekka J. Huovila; Leena Kytömäki; Juhani T. Soini; Mika Kähönen; Pekka J. Karhunen; Reijo Laaksonen; Terho Lehtimäki

Background and aims. The expression of disintegrin and metalloprotease ADAM-9, ADAM-15, and ADAM-17 has been associated with cell-cell, cell-platelet, and cell-matrix interactions and inflammation. They are possibly implicated in the pathophysiology of atherosclerosis. Methods and results. Whole-genome expression array and quantitative real-time polymerase chain reaction (PCR) analysis confirmed that ADAM-9, ADAM-15, and ADAM-17 are upregulated in advanced human atherosclerotic lesions in samples from carotid, aortic, and femoral territories compared to samples from internal thoracic artery (ITA) free of atherosclerotic plaques. Western analysis indicated that the majority of these ADAMs were in the catalytically active form. ADAM-9, ADAM-15, and ADAM-17-expressing cells were shown to co-localize with CD68-positive cells of monocytic origin in the atherosclerotic plaques using immunohistochemistry and double-staining immunofluorescence analysis. Co-localization was demonstrated in all vascular territories. In the carotid territory, cells expressing the ADAMs co-distributed also with smooth muscle cells and, in femoral territory, with CD31-positive endothelial cells, indicating that the ADAM expression pattern depends on vascular bed territory. Conclusions. Present findings provide strong evidence for the involvement of catalytically active ADAM-9, ADAM-15, and ADAM-17 in advanced atherosclerosis, most notably associated with cells of monocytic origin.


Atherosclerosis | 2009

Association of C-reactive protein (CRP) gene allelic variants with serum CRP levels and hypertension in Turkish adults

Evrim Komurcu-Bayrak; Nihan Erginel-Unaltuna; Altan Onat; B. Ozsait; Carita Eklund; Mikko Hurme; Nina Mononen; Reijo Laaksonen; Gülay Hergenç; Terho Lehtimäki

OBJECTIVE Serum C-reactive protein (CRP) is an independent risk factor for cardiovascular disease and metabolic syndrome (MetS). The aim of this study was to analyze the CRP gene allelic variations in the Turkish adult risk factor (TARF) study and relate them with serum CRP levels as well as MetS and its components. METHODS We analyzed CRP gene polymorphisms (-286C>T>A [rs3091244], +1444C>T [rs1130864], +1059G>C [rs1800947], and +1846G>A [rs1205]) as well as their haplotypes, in addition to measuring CRP levels (n=1138) and collecting risk factor data from 1987 adults (mean age 54.3+/-11.9 years, 51.3% women) participating in the TARF Study. MetS was defined by using the criteria of the National Cholesterol Education Program modified for pre-diabetes and in men for abdominal obesity. RESULTS After adjustment for the major cardiovascular risk factors, four CRP SNPs (-286C>T>A, +1059G>C, +1444C>T, and +1846G>A) were significantly associated with serum CRP levels in women (p<0.05), whereas the -286C>T>A and +1444C>T polymorphisms were associated with CRP levels in men (p<0.05). The haplotype analyses revealed four common CRP haplotypes. The haplotype 1 (CGCA) in women and the haplotype 3 (TGTG) in men were associated with serum CRP levels and hypertension (p<0.05). However, no haplotype association was observed for MetS or its components. CONCLUSION CRP gene allelic variation is associated with serum CRP levels as well as hypertension in Turkish adults.


Reproductive Biomedicine Online | 2003

Effect of leukaemia inhibitory factor on long-term sperm motility and survival

Erkut Attar; B. Ozsait; Sibel Bulgurcuoglu; Hasan Serdaroglu; Aydin Arici

Leukaemia inhibitory factor (LIF) is expressed at high constitutive levels in the human Fallopian tubal epithelium. In this study, the effect of human recombinant LIF on sperm motility and survival in vitro was investigated. Human spermatozoa were incubated in sperm washing medium that contained various concentrations of LIF at 37 degrees C and under 5% of CO(2) in air for up to 48 h. Sperm motion characteristics were measured using a sperm motility analyser. Sperm survival was determined by the hypo-osmotic swelling test. The effect of LIF on sperm motility was concentration-dependent and maximal effect was observed at a concentration of 5 ng/ml. Sperm motility was significantly higher after 24 h exposure to LIF compared with control (P < 0.001). Sperm survival was also prolonged in a concentration-dependent manner. LIF significantly enhanced sperm survival at higher concentrations (10 ng/ml) and the result was significant after 48 h exposure (P < 0.05). LIF increased long-term sperm motility and survival in vitro.


Biochemical and Biophysical Research Communications | 2010

Niemann–Pick type C fibroblasts have a distinct microRNA profile related to lipid metabolism and certain cellular components

B. Ozsait; Evrim Komurcu-Bayrak; Mari Levula; Nihan Erginel-Unaltuna; Mika Kähönen; Myriam Rai; Terho Lehtimäki; Reijo Laaksonen

MicroRNAs (miRNAs) are non-coding RNAs that regulate gene expression at post-transcriptional level. Dysregulation of miRNA expression may lead to severe pathophysiologies in human cells. Niemann-Pick type C (NPC) disease is a complex lipid storage disease characterized by late endosomal-lysosomal accumulation of multiple lipid molecules. Our aim was to characterize the miRNA profile in NPC fibroblasts as they may play an active role in the NPC disease associated changes in the cellular physiology. To investigate the miRNA expression, total RNAs were isolated from cultured human NPC fibroblasts and healthy fibroblasts and then, TaqMan Low-Density Array system containing 365 mature human miRNAs was used. Expression differences between the healthy and NPC cells were detected according to the relative quantification values. Target genes were predicted by using three different algorithms and classified regarding NPC related biological processes and cellular components. We found that three miRNAs, miR-196a, miR-196b and miR-296 were up-regulated (>3.5-fold increase, p<0.05) whereas 38 miRNAs were significantly down-regulated in NPC cells (>3.5-fold decrease, p<0.05). Among these non-coding RNAs, miR-98 was the most down-regulated (-33.3-fold) miRNA and miR-143, the lipid biosynthesis associated miRNA, had a 20-fold decreased expression in the NPC cells. Additionally, gene ontology analyses of the target genes suggested a distinct role for each miRNA. Our results show that NPC fibroblasts have an altered miRNA expression profile and certain miRNAs have importance in disease pathogenesis as well as the therapeutic capacity to correct lipid related pathophysiologies in the NPC cells.


Molecular Biology Reports | 2012

Isolation and analysis of genes mainly expressed in adult mouse heart using subtractive hybridization cDNA library

Evrim Komurcu-Bayrak; B. Ozsait; Nihan Erginel-Unaltuna

Subtractive hybridization cDNA library (SHL) is one of the powerful approaches for isolating differentially expressed genes. Using this technique between mouse heart and skeletal muscle (skm) tissues, we aimed to construct a cDNA-library that was specific to heart tissue and to identify the potential candidate genes that might be responsible for the development of cardiac diseases or related pathophysiological conditions. In the first step of the study, we created a cDNA-library between mouse heart and skm tissues. The homologies of the randomly selected 215 clones were analyzed and then classified by function. A total of 146 genes were analyzed for their expression profiles in the heart and skm tissues in published mouse microarray dataset. In the second step, we analyzed the expression patterns of the selected genes by Northern blot and RNA in situ hybridization (RISH). In Northern blot analyses, the expression levels of Myl3, Myl2, Mfn2, Dcn, Pdlim4, mt-Co3, mt-Co1, Atpase6 and Tsc22d1 genes were higher in heart than skm. For first time with this study, expression patterns of Pdlim4 and Tsc22d1 genes in mouse heart and skm were shown by RISH. In the last step, 43 genes in this library were identified to have relationships mostly with cardiac diseases and/or related phenotypes. This is the first study reporting differentially expressed genes in healthy mouse heart using SHL technique. This study confirms our hypothesis that tissue-specific genes are most likely to have a disease association, if they possess mutations.


The Anatolian journal of cardiology | 2008

CETP TaqIB polymorphism in Turkish adults: association with dyslipidemia and metabolic syndrome

B. Ozsait; E Komurcue-Bayrak; M. Poda; Günay Can; Gülay Hergenç; Altan Onat; Steve E. Humphries; Nihan Erginel-Unaltuna


Archive | 2008

CETP TaqIB polymorphism in Turkish adults: association with dyslipidemia and metabolic syndrome Türk yetiflkinlerinde CETP TaqIB polimorfizmi: Dislipidemi ve metabolik sendrom iliflkisi 324

B. Ozsait; Evrim Komurcu-Bayrak; Mehvefl Poda; Günay Can; Gülay Hergenç; Altan Onat; Steve E. Humphries; Nihan Erginel-Unaltuna


Atherosclerosis Supplements | 2008

CRP GENE POLYMORPHISMS ARE INVOLVED IN THE REGULATION OF PLASMA CRP CONCENTRATIONS IN TURKISH POPULATION: TURKISH ADULT RISK FACTOR STUDY

Evrim Komurcu-Bayrak; B. Ozsait; Nina Mononen; Reijo Laaksonen; Altan Onat; Gülay Hergenç; Terho Lehtimäki; Nihan Erginel-Unaltuna


Atherosclerosis Supplements | 2008

USF1 GENE IS INVOLVED IN THE REGULATION OF HUMAN LONGEVITY

B. Ozsait; Evrim Komurcu-Bayrak; M. Jylha; M. Perola; K. Kristiansson; Nina Mononen; Mikko Hurme; Reijo Laaksonen; A. Hervonen; Nihan Erginel-Unaltuna; P. Karhunen; Terho Lehtimäki


Fertility and Sterility | 2007

Effects of male age on semen quality and embryo development in assisted reproductive techniques

B. Ozsait; Sibel Bulgurcuoglu; N. Sen; G. Can; Hasan Serdaroglu; Erkut Attar

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Gülay Hergenç

Yıldız Technical University

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