Your search keyword '"Guzel EE"' showing total 4 results

1. Histological Evaluation of the Effects of Growth Factors in a Fibrin Network on Bone Regeneration.

Author

Cakir S, Gultekin BA, Karabagli M, Yilmaz TE, Cakir E, Guzel EE, Yalcin S, Mortellaro C, and Mijiritsky E

Subjects

Animals, Autografts, Biocompatible Materials pharmacology, Bone Regeneration physiology, Bone Transplantation, Calcium Phosphates therapeutic use, Male, Models, Animal, Random Allocation, Sheep, Tibia cytology, Tibia physiology, Wound Healing drug effects, Bone Regeneration drug effects, Calcium Phosphates pharmacology, Platelet-Rich Fibrin physiology

Abstract

Objective: The aim of this study was to evaluate the effect of mineralized plasmatic matrix (MPM), comprising a combination of synthetic graft and platelet concentrates, on bone regeneration., Methods: Critical size defects of 6-mm diameter were created on the tibias of 6 male sheep, with the animals subsequently assigned into 2 groups. Of the 5 bone defects generated per animal, 4 were randomly filled with MPM, beta-tricalcium phosphate graft (β-TCP), platelet-rich fibrin (PRF) + β-TCP, and autogenous graft. One defect was left empty as a control group. Animals were killed at 3 weeks (early healing group) and 6 weeks (late healing group). The specimens underwent histologic and histomorphometric analysis to evaluate new bone formation., Results: In both healing periods, new bone formation from autogenous bone was observed significantly more often than from biomaterials or the empty defect. The degree of new bone formation for MPM was significantly higher than that of the control group at all healing periods. In addition, it was significantly higher in both healing periods than that of β-TCP albeit only in the late healing period than that of the PRF + β-TCP combination. In all biomaterial groups, residual graft ratios decreased from early to late healing periods., Conclusion: The results indicated that MPM, representing growth factors in a fibrin network, increases new bone formation in surgically created defects in sheep tibia as confirmed by histologic assessment.

Published

2019

2. The investigation of effect of alpha lipoic acid against damage on neonatal rat lung to maternal tobacco smoke exposure.

Author

Guzel EE, Kaya N, Ozan G, Tektemur A, Dabak DO, and Ozan IE

Abstract

This study was carried out to determine the changes in the lungs of the rat pups exposed to tobacco smoke during pregnancy period and to investigate the protective effects of alpha lipoic acid, which is administered during pregnancy, on these changes. Spraque-Dawley female rats were divided into four groups: control, tobacco smoke (TS), tobacco smoke + alpha lipoic acid (TS + ALA) and alpha lipoic acid (ALA). The rats in control group were untreated. Rats were exposed to TS twice a day for one hour starting from eight weeks before mating and during pregnancy. 20 mg / kg of ALA was administered to rats. On 7 th and 21 st days 7 of the pups from each group were decapitated. Histological, morphometric, biochemical and quantitative real-time RT-PCR analyzes were performed. Histopathological and biochemical changes were observed in TS group. While a significant decrease was observed both in SP-A and VEGF immunoreactivities and mRNA levels, caspase-3 immunoreactivity and TUNEL positive cells were increased in TS group. It is suggested that prenatal TS exposure leads to morphological and histopathological changes on lung development by causing oxidative damage in lungs of neonatal rats and the maternal use of ALA can provide a limited protective effect on the neonatal lung development against this oxidative stress originating from TS. Although pregnant women are increasingly aware on health risks of smoking, environmental tobacco smoke exposure is still a widespread problem. For this reason, it is thought that this damage can be partially reduced by some antioxidant supplements in pregnancy.

Published

2018

3. Meningoencephalitis caused by pathogenic Sarcocystis species in a naturally infected sheep in Turkey.

Author

Alasonyalilar-Demirer A, Kahraman MM, Akkoç A, Erturkuner SP, Guzel EE, Kul O, and Ipek V

Subjects

Animals, Central Nervous System Protozoal Infections diagnosis, Central Nervous System Protozoal Infections pathology, Cerebellum parasitology, Cerebellum pathology, Cerebrum parasitology, Cerebrum pathology, Diagnosis, Differential, Heart parasitology, Myocardium pathology, Sarcocystis isolation & purification, Sarcocystis ultrastructure, Sarcocystosis diagnosis, Sarcocystosis pathology, Sheep, Sheep Diseases parasitology, Sheep Diseases pathology, Turkey, Central Nervous System Protozoal Infections veterinary, Sarcocystis pathogenicity, Sarcocystosis veterinary, Sheep Diseases diagnosis

Abstract

A 3-year-old sheep was examined after an acute onset of hind limb paralysis and ataxia. At necropsy, central nervous system, pulmonary and intestinal hyperaemia and ecchymoses in the aortic arch were observed. Main microscopic lesions were confined to the heart, cerebrum and cerebellum. There were a multifocal mild myocarditis and nonsuppurative meningoencephalitis together with protozoal cysts in the heart and the brain. Protozoal cystic structures were observed within many of the myocardial fibers as well as in the cerebrum and cerebellum. Using light microscopy it could not be morphologically determined whether these organisms were Toxoplasma (T.) gondii or Neospora (N.) caninum. Additional diagnostic methods like immunohistochemistry and polymerase chain reaction provided differentiation of Sarcocystis from T. gondii and N. caninum. Transmission electron microscopy demonstrated characteristic features of Sarcocystis sp. as previously described. This is the first confirmed diagnosis of Sarcocystis sp. in the central nervous system of a sheep from Turkey.

Published

2017

4. Distribution of inflammatory cells, adhesion molecules, intermediate filaments, and chemokine receptors in subgroups of nasal polyp patients.

Author

Onerci M, Elsurer C, Guzel EE, and Dagdeviren A

Subjects

Adult, Antigens, CD genetics, Biomarkers metabolism, Cell Adhesion Molecules genetics, Cell Adhesion Molecules immunology, Female, Gene Expression Profiling, Humans, Immunohistochemistry, Intermediate Filaments genetics, Intermediate Filaments immunology, Male, Middle Aged, Receptors, Chemokine genetics, Receptors, Chemokine immunology, Antigens, CD metabolism, Cell Adhesion Molecules metabolism, Intermediate Filaments metabolism, Nasal Polyps immunology, Receptors, Chemokine metabolism

Abstract

Background: The pathogenesis of nasal polyps (NPs) is incompletely understood. The aim of this study was to investigate the distribution of inflammatory cells, adhesion molecules, intermediate filaments, and chemokine receptors in subgroups of NP patients., Methods: In total, 35 patients were enrolled (group 1, 10 patients with Samter syndrome; group 2, 10 patients with diffuse polyposis without signs of Samter syndrome; group 3: 5 patients with solitary nasal polyps; group 4, 10 controls). Immunohistochemical staining was performed for CD105, CD106, CD62E, CD4, CD8, CXCR4, CD147, CD90, CD104, BF45, vimentin, pancytokeratin, and muscle-specific actin (MSA) in all patients' specimens., Results: Expression of CD4, CD8, and CD106 were similar between the groups. Number of patients expressing CD4 in groups 1, 2, and 3 were higher than the controls. Number of patients expressing CD8 antigen were significantly higher in all three groups than in the control group. Expression of CD147 in groups 3 and 4 was significantly higher than in groups 1 and 2. CD98 expression was higher in groups 1, 2, and 3 than in group 4. The number of patients expressing vimentin in groups 1, 2, and 3 was significantly higher than in group 4. Immunostaining for pancytokeratin was positive in all patients., Conclusion: In conclusion, inflammatory cell, adhesion molecule, intermediate filament, and chemokine receptor profiles in nasal polyps differ among different patient groups and control subjects. Additional specific immunohistochemical studies are necessary for development of more specific immunotherapies.

Published

2011