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Analiza genetske variabilnosti na mestih poliadenilacijskega signala pri selekcijskih debelih in vitkih linijah miši
ID Šušteršič, Maša (Author), ID Kunej, Tanja (Mentor) More about this mentor... This link opens in a new window, ID Šimon, Martin (Comentor)

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Abstract
Poliadenilacija je proces, pri katerem pride do cepitve molekule prekurzorske mRNA (pre-mRNA), sledi pa dodajanje poliadeninskega repa (repa poli-A). Poliadenilacijski signal (signal PA) in ostali cis-elementi označujejo mesto poliadenilacije (mesto PA). Alternativna poliadenilacija (APA) je mehanizem uravnavanja (regulacije) genov po prepisovanju (transkripciji), pri katerem iz enega gena nastane več izooblik mRNA zaradi spreminjanja lokacije mest PA znotraj prepisane RNA (transkripta). Povezana je z različnimi boleznimi, tudi z debelostjo. V magistrski nalogi smo izvedli pregled genetskih različic v signalu PA v genih, ki so povezani z debelostjo. Pregled smo izvedli pri debeli in vitki selekcionirani liniji miši. Gene povezane z debelostjo (495) smo pridobili iz podatkovne zbirke IMPC in mesta PA v podatkovni zbirki PolyASite 2.0. Genetske različice so bile določene s predhodnim sekvenciranjem genoma selekcioniranih linij, ki sta nastali s križanjem sorodnih linij JU in CBA ter nesorodne linije CFLP. Po filtriranju genetskih različic s programskim orodjem RStudio smo ugotovili, da se je zaradi različic spremenilo 61 signalov PA v 56 genih. Med temi smo izpostavili gene, pri katerih se je zaradi različic: 1. izgubil/pridobil kanonični signal (AATAAA ali ATTAAA), 2. v zaporedju izgubil edini signal ali 3. ustvaril povsem nov signal, ki ga ni v referenčnem zaporedju. Ti geni so Cep250 in Tnik pri debeli liniji ter Alg8, Arhgef4, Cnot4, Csmd3, Dscc1, Gxylt2, Usp15 pri vitki liniji. V prihodnje bi bilo treba raziskati funkcionalen vpliv različic znotraj signalov PA, preveriti ali imajo različice vpliv na APA ter pregledati ohranjenosti genetskih polimorfizmov v signalu PA med različnimi linijami miši in ostalimi vrstami.

Language:Slovenian
Keywords:alternativna poliadenilacija, debelost, geni za nalaganje maščobe, poliadenilacijski signal, poliadenilacijsko mesto, različice nukleotidnega zaporedja
Work type:Master's thesis/paper
Typology:2.09 - Master's Thesis
Organization:BF - Biotechnical Faculty
Year:2024
PID:20.500.12556/RUL-164529 This link opens in a new window
COBISS.SI-ID:213419779 This link opens in a new window
Publication date in RUL:30.10.2024
Views:70
Downloads:27
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Secondary language

Language:English
Title:Analysis of genetic variability at polyadenylation signal sites in selection mouse lines for fatness and leanness
Abstract:
Polyadenylation is a process in which a precursor mRNA (pre-mRNA) is cleaved, followed by the addition of a polyadenine tail (poly-A tail). The polyadenylation site (PA site) is marked by the polyadenylation signal (PA signal) and other cis-elements. Alternative polyadenylation (APA) is a post-transcriptional regulatory mechanism that generates multiple mRNA isoforms from one gene by varying the location of polyadenylation sites within the transcript. It is linked with different diseases, including obesity. In this study, we examined genetic variants in the PA signals in obesity-related genes. The examination was performed in mouse lines selected for fatness and leanness. Obesity-related genes (495) were obtained from the IMPC database, and PA sites were obtained from the PolyASite 2.0 database. Genetic variants were available by prior sequencing of the genome of selected lines, which were created by crossing the inbred lines JU and CBA and the outbred line CFLP. After filtering of genetic variants using the RStudio software tool, we found out that 61 PA signals in 56 genes were altered due to the variants. Among these, we highlighted genes in which genetic variants caused: 1. loss/gain of canonic signal (AATAAA or ATTAAA), 2. loss of the only signal in the sequence, or 3. a creation of a completely new signal while the reference genome had no other signals. These genes include Cep250, Tnik for fat line and Alg8, Arhgef4, Cnot4, Csmd3, Dscc1, Gxylt2, Usp15 for lean line. In future research, it would be necessary to investigate the functional impact of variants within the PA signals, to check whether the variants have an impact on APA, and to examine the conservation of genetic polymorphisms in the PA signal between different lines of mice and other species.

Keywords:alternative polyadenylation, obesity, obesity-related genes, polyadenylation signal, polyadenylation site, single nucleotide polymorphism

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