Scopus İndeksli Yayınlar Koleksiyonu / Scopus Indexed Publications Collection
Permanent URI for this collectionhttps://hdl.handle.net/11147/7148
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Article Citation - WoS: 5Citation - Scopus: 6Sustainable Production of Aging-Resistant Bitumen: Waste Engine Oil Modification(American Society of Civil Engineers, 2021) Gökalp, İslam; Uz, Volkan EmreUsing waste engine oil (WEOIL) within bituminous binders might be one of the most energy-efficient and sustainable means of producing aging-resistant bitumen due to the antioxidative properties of WEOIL. In this paper, the use of WEOIL to obtain aging-resistant bitumen and its optimum rates for short and long terms were investigated. In this regard, a base bitumen was modified with WEOIL in certain rates ranging from 1% to 5% by weight of bitumen. Then base and oil-modified bitumen samples were subjected to aging. To define the changes in rheological properties of bitumen based on rutting, fatigue, and thermal cracking resistance, dynamic shear and bending beam rheometer tests were performed on each sample. Furthermore, an aging index (AI) analysis was performed for both the short- and long-term aging conditions to express the effect of WEOIL on aging resistance of the bitumen. According to the AI analysis, short-term-aging-resistant bitumen is obtained by adding 3.5% WEOIL to the base bitumen, while a 5.8% contribution rate is required to avoid the long-term aging effect. Moreover, the increase in rate of WEOIL content improved the low-temperature cracking resistance. Consequently, utilizing WEOIL for production of aging-resistant bitumen can provide environmental and economic benefits based on conservation of natural resources and waste recycling.Article Citation - WoS: 9Citation - Scopus: 10Characterization of Long Living Yeast Deletion Mutants That Lack Mitochondrial Metabolism Genes Dss1, Ppa2 and Afg3(Elsevier, 2019) Muid, Khandaker Ashfaqul; Kimyon, Önder; Reza, Shahadat Hasan; Karakaya, Hüseyin Çağlar; Koç, AhmetMolecular mechanisms of aging and longevity are still mostly unknown. Mitochondria play central roles in cellular metabolism and aging. In this study, we identified three deletion mutants of mitochondrial metabolism genes (ppa2 Delta, dss1 Delta, and afg3 Delta) that live longer than wild-type cells. These long-lived cells harbored significantly decreased amount of mitochondria] DNA (mtDNA) and reactive oxygen species (ROS). Compared to the serpentine nature of wild-type mitochondria, a different dynamics and distribution pattern of mitochondria were observed in the mutants. Both young and old long-lived cells produced relatively low but adequate levels of ATP for cellular activities. The status of the retrograde signaling was checked by expression of CIT2 gene and found activated in long-lived mutants. The mutant cells were also profiled for their gene expression patterns, and genes that were differentially regulated were determined. All long-lived cells comprised similar pleiotropic phenotype regarding mitochondrial dynamics and functions. Thus, this study suggests that DSS1, PPA2, and AFG3 genes modulate the lifespan by altering the mitochondrial morphology and functions.Article Citation - WoS: 12Citation - Scopus: 12Identification of Respiratory Chain Gene Mutations That Shorten Replicative Life Span in Yeast(Elsevier Ltd., 2012) Hacıoğlu, Elise; Demir, Ayşe Banu; Koç, AhmetAging is the progressive accumulation of alterations in cells that elevates the risk of death. The mitochondrial theory of aging postulates that free radicals produced by the mitochondrial respiratory system contribute to the aging process. However, the roles of individual electron transfer chain (ETC) components in cellular aging have not been elucidated. In this study, we analyzed the replicative life span of 73 yeast deletion mutants lacking the genes of the mitochondrial electron transfer chain system, and found that nine of these mutants (δ nde1, δ tcm62, δ rip1, δ cyt1, δ qrc8, δ pet117, δ cox11, δ atp11, δ fmc1) had significantly shorter life spans. These mutants had lower rates of respiration and were slightly sensitive to exogenous administration of hydrogen peroxide. However, only two of them, δ nde1 and δ fmc1, produced higher amounts of intrinsic superoxide radicals in the presence of glucose compared to that of wild type cells. Interestingly, there were no significant alterations in the mitochondrial membrane potentials of these mutants. We speculate that the shorter life spans of ETC mutants result from multiple mechanisms including the low respiration rate and low energy production rather than just a ROS-dependent path. © 2011 Elsevier Inc.