prikaz prve stranice dokumenta Analysis of ADAR protein during productive HSV-1 Infection
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master's thesis
Analysis of ADAR protein during productive HSV-1 Infection
2022. urn:nbn:hr:193:745757
Echeta, Justina Oluchi
University of Rijeka
Faculty of Biotechnology and Drug Development

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Echeta, J. O. (2022). Analysis of ADAR protein during productive HSV-1 Infection (Master's thesis). Rijeka: University of Rijeka. Retrieved from https://urn.nsk.hr/urn:nbn:hr:193:745757

Echeta, Justina Oluchi. "Analysis of ADAR protein during productive HSV-1 Infection." Master's thesis, University of Rijeka, 2022. https://urn.nsk.hr/urn:nbn:hr:193:745757

Echeta, Justina Oluchi. "Analysis of ADAR protein during productive HSV-1 Infection." Master's thesis, University of Rijeka, 2022. https://urn.nsk.hr/urn:nbn:hr:193:745757

Echeta, J. O. (2022). 'Analysis of ADAR protein during productive HSV-1 Infection', Master's thesis, University of Rijeka, accessed 30 October 2024, https://urn.nsk.hr/urn:nbn:hr:193:745757

Echeta JO. Analysis of ADAR protein during productive HSV-1 Infection [Master's thesis]. Rijeka: University of Rijeka; 2022 [cited 2024 October 30] Available at: https://urn.nsk.hr/urn:nbn:hr:193:745757

J. O. Echeta, "Analysis of ADAR protein during productive HSV-1 Infection", Master's thesis, University of Rijeka, Rijeka, 2022. Available at: https://urn.nsk.hr/urn:nbn:hr:193:745757

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Metadata
TitleAnalysis of ADAR protein during productive HSV-1 Infection
Title (english)Analyza ADAR proteina tijekom produktivne infekcije HSV-1
AuthorJustina Oluchi Echeta
MentorIgor Jurak (mentor)
Committee memberIgor Jurak (predsjednik povjerenstva)
Committee memberJurica Novak (član povjerenstva)
Committee memberNicholas Bradshaw (član povjerenstva)
GranterUniversity of Rijeka
(Faculty of Biotechnology and Drug Development)
Rijeka
Defense date and country2022-07-27, Croatia
Scientific / art field,
discipline and subdiscipline		BIOTECHNICAL SCIENCES
Biotechnology
Abstract
ADAR proteins are enzymes involved in the editing of dsRNA transcripts by deamination in which adenosine is changed to Inosine. This alteration ultimately affects protein translation. ADAR1 has two isoforms; ADAR1p110 and ADAR1p150, ADAR2 and ADAR3 make up the mammalian ADAR family. Both isoforms of ADAR1 and ADAR2 are catalytically active while ADAR3 is not. ADARs edit both self and non-self dsRNA. Several studies have shown the role of ADAR proteins mostly in RNA viruses, however, the role of these proteins in dsDNA viruses is largely unknown. During viral infection, they can play an antiviral role by forming part of the cell’s innate immune response, a proviral role by blocking viral dsRNA from being recognized by the immune sensors, thereby facilitating viral replication in the host cell, or both roles as observed in Influenza A virus. Based on in vitro experiments, we have established cell models to analyse the role of ADAR proteins during productive HSV-1 infection. ADAR protein and mRNA levels during productive HSV-1 infection were determined, showing upregulation of ADAR during the infection. We observed an upregulation of ADAR proteins in U2OS, HeLa, HEK293T, and HFF cells infected with wild-type HSV-1 using MOIs 5 and 10, but not with MOI of 1. Interestingly, we observed ADAR cells-specific response to infection with UV inactivated HSV-1, which we cannot explain at this point. To investigate the functional relevance of ADAR1 and ADAR2 proteins for virus replication, we transfected cells with ADAR1 and ADAR2 expressing plasmids to overexpress ADAR in cells. Surprisingly, we did not observe any effect on virus DNA replication, indicating that ADAR1 and ADAR2 might not play a role in productive HSV-1 infection. However further investigation is needed to answer this question.
Abstract (croatian)
ADAR protein su enzimi uklučeni u uređivanje dsRNA transkripata deaminacijom u kojoj se adenozin mijenja u inozin. Ova promjena u konačnici može utjecati na stabilnost RNA te na translaciju proteina. Obitelj ADAR proteina čine ADAR1, koji ima dvije izoforme: ADAR1p110 i ADAR1p150, ADAR2 i ADAR3. ADAR1 i ADAR2 su katalitički aktivni dok ADAR3 nije. ADAR uređuju vlastite i brojne druge dsRNA. Nekoliko je studija pokazalo ulogu proteina ADAR većinom u RNA virusima, , međutim njihova uloga kod infekcije s dsDNA virusima slabo je istražena. Tijekom virusne infekcije, oni mogu imati antivirusnu ulogu čineći dio urođenog imunološkog odgovora stanica, ali i provirusnu ulogu, blokirajući virusnu dsRNA da je prepozna imunološki senzor, čime se olakšava replikacija virusa u stanici domaćinu, ili obje uloge kao što je primijećeno kod Influenza A virus. Na temelju in vitro eksperimenata, uspostavili smo stanične modele za analizu uloge ADAR proteina tijekom productivene HSV-1 infekcije. Određene su razine ADAR proteina i mRNA tijekom produktivne HSV-1 infekcije. Uočili smo pojačanu regulaciju ADAR u U2OS, HeLa, HEK293T i HFF stanicama zaraženim divljim tipom HSV-1 te je takva pojačana ekspresija ovisila o količini virusa kojom se inficira stanica. Zanimljivo je da smo uočili različiti ADAR odgovor na infekciju s UV inaktiviranim virusom kod različitih vrsta stanica, što u ovom trenutku ne možemo objasniti. Nadalje, kako bismo istražili funkcionalnu relevantnost ADAR1 i ADAR2 proteina za replikaciju virusa, transfecirali smo stanice s ADAR1 i ADAR2 ekspresijskim plazmidima za prekomjernu ekspresiju ADAR-a. Naime, nismo primijetili nikakav učinak na replikaciju DNA virusa, što ukazuje da ADAR1 i ADAR2 možda nemaju ulogu u produktivnoj HSV-1 infekciji. Međutim, potrebna su daljnja istraživanja kako bi se odgovorilo na ova pitanja.
Keywords
Keywords (english)
Languageenglish
URN:NBNurn:nbn:hr:193:745757
Study programmeTitle: Biotechnology for the Life Sciences
Study programme type: university
Study level: graduate
Academic / professional title: magistar/magistra biotehnoloških istraživanja (magistar/magistra biotehnoloških istraživanja)
Type of resourceText
File originBorn digital
Access conditionsOpen access
Embargo expiration date: 2024-10-24
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Created on2022-10-24 12:27:44