H. Arzu Ergen
Istanbul University
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Featured researches published by H. Arzu Ergen.
Experimental and Molecular Medicine | 2004
H. Arzu Ergen; Husrev Hatemi; Bedia Agachan; Hakan Camlica; Turgay Isbir
Non-insulin dependent diabetes mellitus is often associated with some complications such as nephropathy, retinopathy and neuropathy. Genes of the renin angiotensin system are potential candidate genes for diabetic complications. We investigated the relationship between angiotensin converting enzyme (ACE) gene polymorphism in type 2 diabetic patients with and without diabetic nephropathy. Seventy five patients (25 type 2 diabetic patients with nephropathy, 50 type 2 diabetic patients without nephropathy) and 37 healthy controls were studied. Gene polymorphism of ACE was determined by PCR (polymerase chain reaction) amplification using allele-spesific primers. The frequencies of ACE DD, ID and II genoypes among the patients with type 2 diabetic patients were found 48%, 42%, 10% whereas in control subjects, 27%, 60%, 13% respectively. Type 2 diabetic patients carrying DD genotype without nephropathy increased 1.77 fold than control subjects (P < 0.05). There is no significant correlation between diabetic nephropathy and ACE gene polymorphism. But we found that ACE DD genotype increased significantly in type 2 diabetic patients compared to control subjects (P < 0.05).
Archives of Medical Science | 2010
Yemliha Yildiz; Ilhan Yaylim-Eraltan; Soykan Arikan; H. Arzu Ergen; Seden Küçücük; Turgay Isbir
Introduction TNF-related apoptosis-inducing ligand (TRAIL) is a death ligand and also a member of the TNF superfamily. We aimed to investigate the possible relationship between TRAIL and breast cancer. Here, we report the results of the first association study on genetic variation in the TRAIL gene and its effect on breast cancer susceptibility and prognosis. Material and methods A C/T polymorphism at 1595 position in exon 5 of the TRAIL gene was genotyped in a Turkish breast cancer case-control population including 53 cases (mean age: 55.09 ±11.63 years) and 57 controls (mean age: 57.17 ±17.48 years) using polymerase chain reaction–restriction fragment length polymorphism (PCR-RFLP) analysis. Results There were no differences in the distribution of TRAIL genotypes and frequencies of the alleles in the breast cancer patients and controls. A heterozygous TRAIL CT polymorphism in exon 5 was present in 8.3% of tumour stage III-IV and 48.8% of stage I-II patients, and in 42.1% of controls. The reduced frequency of this genotype in patients who had advanced tumour stage was statistically significant (p = 0.017). Conclusions Our findings indicate that genetic variants of TRAIL at position 1595 in exon 5 might be associated with progression of breast cancer.
Cell Biochemistry and Function | 2007
Ilhan Yaylim-Eraltan; H. Arzu Ergen; Soykan Arikan; Erdem Okay; Oguz Ozturk; Savaş Bayrak; Turgay Isbir
Anticancer Research | 2007
H. Arzu Ergen; Fehmi Narter; Özlem Timirci; Turgay Isbir
Anticancer Research | 2010
Ilhan Yaylim-Eraltan; Soykan Arikan; Yemliha Yildiz; Canan Cacina; H. Arzu Ergen; Gulay Tuna; Uzay Görmüş; Umit Zeybek; Turgay Isbir
Journal of Surgical Research | 2005
Erdem Okay; Aynur Karadenizli; Bahar Muezzinoglu; Umit Zeybek; H. Arzu Ergen; Turgay Isbir
Anticancer Research | 2007
H. Arzu Ergen; Uzay Gormus; Fehmi Narter; Umit Zeybek; Sibel Bulgurcuoglu; Turgay Isbir
in Vivo | 2010
Kıvanç Bektaş-Kayhan; Meral Ünür; Ilhan Yaylim-Eraltan; H. Arzu Ergen; Bahar Toptaş; Gunter Hafiz; Ahmet Karadeniz; Turgay Isbir
Biochemia Medica | 2012
H. Arzu Ergen; Umit Zeybek; Ozlem Gok; Z. Eremis Karaali
Archive | 2005
C. Selim; H. Arzu Ergen; Umit Zeybek; Turgay ‹ sbir