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Funkcionalna opredelitev zarodnih različic neznanega kliničnega pomena z analizo mRNA pri bolnikih ogroženih z dednimi oblikami raka : doktorska disertacija
ID Šetrajčič Dragoš, Vita (Author), ID Novaković, Srdjan (Mentor) More about this mentor... This link opens in a new window

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Abstract
Genetske različice lahko povzročijo nepravilno prepoznavo spojitvenih mest med procesom izrezovanja intronov in spajanja eksonov, ki ga izvrši izrezovalno-povezovalni kompleks med formiranjem zrele mRNA. Posledica tega je spremenjena mRNA molekula, kar je lahko vzrok za nastanek genetskih sindromov. Eden od načinov, da odkrijemo različice, ki povzročijo napačno prepoznavo spojitvenih mest je, da določimo neposreden vpliv različice na molekuli mRNA nosilca različice. Za namen te doktorske naloge smo razvili in validirali nov pristop sekvenciranja cDNA za določanje alternativnih transkriptov in zarodnih okvar na molekuli mRNA nastalih med procesom izrezovanja intronov in spajanja eksonov. Z novim pristopom sekvenciranja cDNA smo odkrili nove alternativne transkripte v genih STK11, NBN in BRIP1. V genu STK11 smo odkrili 18, v genu NBN 49 in v genu BRIP1 7 novih alternativnih transkriptov. Vse odkrite alternativne transkripte smo anotirali in objavili prvi obsežen katalog alternativnih transkriptov v navedenih genih. V drugem delu raziskave smo izvedli bioinformatsko oceno vpliva različic na izrezovanje intronov in spajanje eksonov. Funkcijsko smo opredelili 32 različic neznanega kliničnega pomena (VUS) v genih povezanimi z dednimi oblikami raka. S pomočjo novega pristopa sekvenciranja cDNA smo uspešno reklasificirali 65,6 % vseh VUS-ov (46,9 % v verjetno benigno različico in 18,8 % v verjetno patogeno različico). Od 2808 preiskovancev smo pri 2 % odkrili VUS s potencialnim vplivom na izrezovanje intronov in spajanje eksonov. Od analize mRNA je imelo korist 1,4 % pacientov, pri katerih smo VUS reklasificirali. Vzročno različico smo z analizo mRNA opredelili pri 0,2 % preiskovancih.

Language:Slovenian
Keywords:genetika, mRNA, sekvenciranje naslednje generacije, sekvenciranje RNA, različice neznanega kliničnega pomena, dedne oblike raka
Work type:Doctoral dissertation
Typology:2.08 - Doctoral Dissertation
Organization:BF - Biotechnical Faculty
Year:2023
PID:20.500.12556/RUL-151816 This link opens in a new window
COBISS.SI-ID:169486339 This link opens in a new window
Publication date in RUL:21.10.2023
Views:865
Downloads:100
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Secondary language

Language:English
Title:Functional assessment of germline variants of unknown clinical significance by mRNA analysis in patients at high risk of hereditary cancers : doctoral dissertation
Abstract:
During RNA splicing, genetic variants can alter the identification of splice sites recognized by the spliceosome. Altered recognition of splice sites can cause aberrant mRNA molecule, which can be the underlying cause of genetic syndrome development. One of the approaches to detect variants that cause misrecognition of splice sites is to determine the effect of the variant directly on the patient’s mRNA molecule. In this doctoral thesis, we developed and validated a new cDNA sequencing approach to identify splicing aberrations resulting from germline variants. By using new approach, we discovered 18, 49, and 7 new alternative transcripts in the STK11, NBN, and BRIP1 genes, respectively. We annotated all the discovered alternative transcripts and published the first comprehensive catalog of annotated alternative transcripts for these genes. In the second part of the study, we performed a bioinformatics assessment of variants' impact on splicing. We functionally assessed 32 variants of unknown clinical significance (VUS) in genes associated with hereditary cancer syndromes. Using the novel cDNA sequencing approach, we successfully reclassified 65.6 % of all VUSs (46.9 % were reclassified as a likely benign variant and 18.8 % as a likely pathogenic variant). Among 2808 patients included in the study, we found that 2 % of them carried a VUS with a potential impact on splicing. We were able to successfully reclassify VUS in 1.4 % of patients through mRNA analysis. The causative variant was identified through mRNA analysis in 0.2 % of patients.

Keywords:genetics, mRNA, next generation sequencing, RNA sequencing, variants of unknown significance, hereditary cancer syndromes

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