Transcriptomic alterations in the aged brain with and without dietary and dietary- mimetic manipulations

buir.advisorM. Adams, Michelle
dc.contributor.authorErbaba, Begün
dc.date.accessioned2022-01-26T06:02:06Z
dc.date.available2022-01-26T06:02:06Z
dc.date.copyright2021-12
dc.date.issued2021-12
dc.date.submitted2022-01-24
dc.descriptionCataloged from PDF version of article.en_US
dc.descriptionThesis (Ph.D.): Bilkent University, Department of Neuroscience, İhsan Doğramacı Bilkent University, 2021.en_US
dc.descriptionIncludes bibliographical references (leaves 122-146).en_US
dc.description.abstractAside from many genetic and environmental influences on the brain, aging itself is a significant risk factor for accelerated cognitive decline, making aging research crucial due to the increasing population age in our era. We aimed to discover gene expression differences in the aging zebrafish brain using three age groups in the first aim. We identified gjc2 (CX47) and alcamb (ALCAM) cell adhesion genes showing consistent downregulation with age across all experiments. ALCAM is also known to be associated with neuroinflammation, which has been implicated to be lowered using anti-aging, non-genetic nutrient interventions. In the second aim, we applied 12 weeks of two opposing nutrient interventions, caloric restriction (CR) and overfeeding (OF) in aging zebrafish, in order to be able to propose a reliable therapeutic approach for reversing age-related neurobiological changes. We measured protein and expression level differences of selected genes related to proliferation to inflammation with these diets. The results showed that sox2 gene expression was significantly upregulated following OF treatment than CR diet, and myca and tp53 mRNA levels were significantly downregulated with advanced age. Alcamb and tfdp1 expression levels were also marginally significantly lowered with CR compared to other groups. Meanwhile, we also conducted another transcriptomic approach using microarray to assess gene expression differences with CR compared to Ad-libitum (AL) feeding. Thus, lastly, in the third part, we found that CR causes changes in cell cycle regulation among several other functional regulatory pathways in zebrafish brains. We identified the tfdp1 gene, which showed downregulation with CR, as a possible CR regulator. Then, to create a CR mimic, we performed morpholino oligo (MO) injections to zebrafish embryos and adult brains to knock down tfdp1 gene expression levels. The injections were not successful in altering Tfdp1 protein levels in neither embryos and adults. However, 8ng tfdp1-MO injections in embryos significantly increased myca and tp53 expression levels, which are among the downstream targets of tfdp1. Our examinations shed light on healthy brain aging and possibly propose new drug targets.en_US
dc.description.provenanceSubmitted by Betül Özen (ozen@bilkent.edu.tr) on 2022-01-26T06:02:06Z No. of bitstreams: 1 Transcriptomic alterations in the aged brain with and without dietary and dietary-mimetic manipulations.pdf: 4321867 bytes, checksum: ad446d1191dcceecb96ed97ece110076 (MD5)en
dc.description.provenanceMade available in DSpace on 2022-01-26T06:02:06Z (GMT). No. of bitstreams: 1 Transcriptomic alterations in the aged brain with and without dietary and dietary-mimetic manipulations.pdf: 4321867 bytes, checksum: ad446d1191dcceecb96ed97ece110076 (MD5) Previous issue date: 2021-12en
dc.description.statementofresponsibilityby Begün Erbabaen_US
dc.format.extentxxii, 149 leaves : illustrations ; 30 cm.en_US
dc.identifier.itemidB160950
dc.identifier.urihttp://hdl.handle.net/11693/76780
dc.language.isoEnglishen_US
dc.rightsinfo:eu-repo/semantics/openAccessen_US
dc.subjectZebrafishen_US
dc.subjectBrainen_US
dc.subjectAgingen_US
dc.subjectCaloric restrictionen_US
dc.titleTranscriptomic alterations in the aged brain with and without dietary and dietary- mimetic manipulationsen_US
dc.title.alternativeDiyet ve diyet-mimetiği manipülasyonların gen anlatımı açısından yaşlanan beyne etkilerien_US
dc.typeThesisen_US
thesis.degree.disciplineNeuroscience
thesis.degree.grantorBilkent University
thesis.degree.levelDoctoral
thesis.degree.namePh.D. (Doctor of Philosophy)

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